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United States Patent 5,738,096
Ben-Haim April 14, 1998
Cardiac electromechanics


Abstract

A method of constructing a cardiac map of a heart having a heart cycle including; bringing an invasive probe into contact with a location on a wall of the heart; determining, at at least two different phases of the heart cycle, a position of the invasive probe; and determining a local non-electrical physiological value at the location. The method is repeated for a plurality of locations in the heart. The positions are combined to form a time-dependent map of at least a portion of the heart and local relationships between changes in positions of the invasive probe and determined local non-electrical physiological values are determined. Preferably, local electrical activity at the plurality of locations is also acquired.

Inventors: Ben-Haim; Shlomo (Haifa, IL)
Assignee: Biosense, Inc. (Orangeburg, NY)
Appl. No.: 595365
Filed: February 1, 1996
Related U.S. Patent Documents
Application NumberFiling DatePatent NumberIssue Date
293859Aug., 1994
311593Sep., 19945546951
94539Jul., 19935391199

Current U.S. Class: 600/407 ; 128/899; 600/508
Field of Search: 128/660.03,899,662.06,642,695R 607/122,116,119,125

References Cited
U.S. Patent Documents
4173228 November 1979 Van Steenwyk et al.
4304239 December 1981 Perlin
4431005 February 1984 McCormick
4444195 April 1984 Gold
4499493 February 1985 Nishimura
4522212 June 1985 Gelinas et al.
4573473 March 1986 Hess
4613866 September 1986 Blood
4628937 December 1986 Hess et al.
4649924 March 1987 Taccardi
4697595 October 1987 Breyer et al.
4699147 October 1987 Chilson et al.
4777955 October 1988 Brayton et al.
4812976 March 1989 Lundy
4821731 April 1989 Martinelli et al.
4899750 February 1990 Ekwall
4921482 May 1990 Hammerslag et al.
4922912 May 1990 Watanabe
4940064 July 1990 Desai
4945305 July 1990 Blood
5000190 March 1991 Petre
5012814 May 1991 Mills et al.
5025786 June 1991 Siegel
5041973 August 1991 Lebron et al.
5042486 August 1991 Pfeiler et al.
5054492 October 1991 Scribner
5054496 October 1991 Wen et al.
5056517 October 1991 Fenici
5081993 January 1992 Kitney et al.
5104393 April 1992 Isner et al.
5154501 October 1992 Svenson et al.
5156151 October 1992 Imran
5158092 October 1992 Glace
5161536 November 1992 Vilkomerson et al.
5172699 December 1992 Svenson et al.
5195968 March 1993 Lundquist et al.
5211165 May 1993 Dumoulin et al.
5220924 June 1993 Frazin
5222501 June 1993 Ideker et al.
5246016 September 1993 Lieber et al.
5285788 February 1994 Arenson et al.
5295484 March 1994 Marcus et al.
5297549 March 1994 Beatty et al.
5311873 May 1994 Savard et al.
5335663 August 1994 Oakley et al.
5341807 August 1994 Nardella
5368564 November 1994 Savage
5368592 November 1994 Stern et al.
5373849 December 1994 Maroney et al.
5383923 January 1995 Webster et al.
5391199 February 1995 Ben-Haim
5403356 April 1995 Hill et al.
5404297 April 1995 Birk et al.
5431168 July 1995 Webster, Jr.
5433198 July 1995 De Sai
5443489 August 1995 Ben-Haim
5487391 January 1996 Panescu
5558091 September 1996 Acker
5577502 November 1996 Darrow et al.
5588432 December 1996 Crowley
5592939 January 1997 Martinelli
Foreign Patent Documents
0499491 Aug., 1992 EP

Other References

Josephson et al., Role of Catheter Mapping in the Preoperative Evaluation of Ventricular Tachycardia, The American Journal of Cardiology, vol. 40, pp. 207-220, Jan. 1982. .
Josephson et al., Comparison of Endocardial Catheter Mapping with Intraoperative Mapping of Ventricular Tachycardia, Circulation, vol. 61, No. 2, pp. 395-404, 1980. .
Josephson et al., Ventricular Activation During Ventricular Endocardial Pacing--II: Role of Pace-Mapping to Localize Origin of Ventricular Tachycardia The American Journal of Cardiology, vol. 30, 50, pp. 11-22, Jul. 1982. .
Witnowski et al., An Automated Simultaneous Transmural Cardiac Mapping System, American Journal of Physiology vol. 247, pp. H661-H668, 1984. .
Fann et al., Endocardial Activation mapping and Endocardial Pace-Mapping Using a Balloon Apparatus, American Journal of Cardiology vol. 55, pp. 1076-1083, Apr. 1, 1985. .
Hauer et al., Endocardial Catheter Mapping: Wire Skeleton Techniques for Representation of Computed Arrhythmogenic Sites Compared with Intraoperative Mapping, Circulation, vol. 74, No. 6, pp. 1346-1354, Dec. 1986. .
Pogwizd et al., Reentrant and Nonreentrant mechanisms Contribute to Arrhythmogenesis During Early Myocardial Ischemia: Results using Three-Dimensional Mapping, Circulation Research, vol. 61, No. 3, pp. 352-371, Sep. 1987. .
Huang et al., Radiofrequency Catheter Ablation of the Left and Right Ventricles: Anatomic and Electrophysiologic Observations, Pace vol. 11, pp. 449-459, Apr. 1988. .
Jackman et al., New Catheter Technique for Recording Left Free-Wall Accessory Atrioventricular Pathway Activation, Circulation vol. 78, No. 3, pp. 598-611, Sep. 1988. .
Page, Surgical Treatment of Ventricular Tachycardia: Regional Cryoablation Guided by Computerized Epicardial and Endocardial Mapping, Circulation vol. 80, (Supplement I), No. 3, pp. I-124--I-134, Sep. 1989. .
Tweddel et al., Potential Mapping Septal Tachycardia: Evaluation of a New Intraoperative Mapping Technique, Circulation vol. 80, (Supplement I), No. 3, pp. I-97--I-108, Sep. 1989. .
Shenasa et al., Cardiac Mapping, Part I: Wolff-Parkinson-White Syndrome Pace, vol. 13, pp. 223-230, Feb. 1990. .
Scheinman et al., Current Role of Catheter Ablative Procedures in patients with Cardiac Arrhythmias, Circulation vol. 83, No. 6, pp. 2146-2153, Jun. 1991. .
Buckles et al., Computer-Enhanced Mapping of Activation Sequences in the Surgical Treatment of Supraventricular Arrhythmias, Pace vol. 13, Pt. 1, pp. 1401-1407, Nov. 1990. .
Tanigawa et al., Prolonged and Fractionated Right Atrial Electrograms During Sinus Rhythm in Patients with Paroxysmal Atrial Fibrillation and Sick Sinus Node Syndrome, Journal of American College of Cardiologists vol. 17, No. 2, pp. 403-408, Feb. 1991. .
Kuchar et al., Electrocardiographic Localization of the Site of Ventricular Tachycardia in Patients with Prior Myocardial Infarction, JACC, vol. 13, No. 4, pp. 893-900, 1989. .
Holt et al., Ventricular Arrhythmias--A Guide to Their Localization, British Heart Journal, vol. 53, pp. 417, 430, 1985. .
Kaltenbrunner et al., Epicardial and Endocardial Mapping of Ventricular Tachycardia in Patients with Myocardial Infarction, Circulation vol. 83, No. 3, pp. 1058-1071, Sep. 1991. .
Masse et al., A Three-Dimensional Display for Cardiac Activation Mapping, Pace, vol. 14, Pt. 1, pp. 438-545, Apr. 1991. .
Desai et al., Orthogonal Electrode Catheter Array for Mapping of Endocardial Focal Site of Ventricular Activation, Pace vol. 14, Pt. 1, pp. 557-574, Apr. 1991. .
Pollak et al., Intraoperative Identification of a Radiofrequency Lesion Allowing Validation of Catheter Mapping of Ventricular Tachycardia with a Computerized Balloon Mapping System, Pace vol. 15, pp. 854-858, Jun. 1992. .
Chen et al., Reappraisal of Electrical Cure of Atrioventricular Nodal Reentrant Tachycardial--Lesions from a Modified Catheter Ablation Technique International Journal of Cardiology, vol. 37, pp. 51-60, 1992. .
Chen et al., Radiofrequency Catheter Ablation for Treatment of Wolff-Parkinson-White Syndrome--Short- and Long-term Follow-up International Journal of Cardiology, vol. 37 pp. 199-207, 1992. .
Scheinman, North American Society of Pacing and Electrophysiology (NASPE) Survey of Radiofrequency Catheter Ablation: Implications for Clinicians, Third Party Insurers, and Government Regulatory Agencies, Pace vol. 15, pp. 2228-2231, Dec. 1992. .
Silka et al., Phase Image Analysis of Anomalous Ventricular Activation in Pediatric Patients with Preexcitation Syndromes or Ventricular Tachycardia, American Heart Journal vol. 125, No. 2, Pt. 1, pp. 372-380, Feb. 1993. .
Josephson, Clincal Cardiac Electrophysiology: Techniques and Interpretations, 2nd Ed. pp. 566-580, 608-615, 770-783, Lea & Febiger, Malvern Pa., 1993. .
Fananapazir et al., Long-term Results of Dual-Chamber (DDD) Pacing in Obstructive Hypertrophic Cardiomyopathy: Evidence for Progressive Sumptomatic and Hemodynamic Improvement and Reduction of Left Ventricular Hypertrophy, Circulation, vol. 90, No. 6, pp. 2731-3742, Dec. 1994. .
Jeanrenaud et al., Effects of Dual-chamber Pacing in Hypertrophic Obstructive Cardiomyopathy, The Lancet, vol. 339, pp. 1318-1323. May 30, 1992. .
Langberg, J. J. et al "The Echo-Transponder Electrode Catheter: A New Method for Mapping the Left Ventricle", JACC vol. 12 No. 1 Jul. 1988: 218-223..

Primary Examiner: Jaworski; Francis
Attorney, Agent or Firm: Cowan, Liebowitz & Latman, P.C.
Parent Case Text


CROSS-REFERENCE TO RELATED APPLICATIONS

This application is a continuation-in-part of (1) U.S. patent application Ser. No. 60/009,769, filed Jan. 11, 1996, (2) PCT patent patent application No. PCT/US95/01103, filed Jan. 24, 1995, (3) U.S. patent application Ser. No. 08/293,859, filed Aug. 19, 1994, now abandoned, and (4) U.S. patent application Ser. No. 08/311,593, filed Sep. 23, 1994, now U.S. Pat. No. 5,546,951, which in turn is a divisional of U.S. patent application Ser. No. 08/094,539, filed Jul. 20, 1993, now U.S. Pat. No. 5,391,199.
Claims


I claim:

1. A method of constructing a map of the heart having a heart cycle comprising:

(a) bringing a probe into contact with a location on a wall of the heart;

(b) determining a position of the probe at the location;

(c) repeating (a) and (b) for a multiplicity of locations of the heart; and

(d) combining the determined positions of the probe to determine a structural map of at least a portion of the heart.

2. A method according to claim 1 comprising determining local pathologies in the heart based on the map.

3. A method according to claim 1 and comprising determining at least a second position of the probe at a phase of the cycle different from the phase at the position determination of (b) and wherein the map is a phase dependent geometric map.

4. A method according to claim 3, wherein the second position determination is performed at the location.

5. A method according to claim 4 comprising analyzing the map to determine underutilized portions of the heart.

6. A method according to claim 4 comprising analyzing the map to determine procedures for improving the operation of the heart.

7. A method according to claim 4 comprising, determining a local change in the geometry of the heart.

8. A method according to claim 7 comprising determining local pathologies in the heart based on the local changes in geometry.

9. A method according to claim 7, wherein the local change comprises a change in a local radius of the heart wall at the location.

10. A method according to claim 9 comprising determining an intra-cardiac pressure of the heart.

11. A method according to claim 10 comprising determining a tension of the heart at the location by applying Laplace's law to the change in the local radius and the determined pressure.

12. A method according to claim 9, further comprising determining a relative tension of the heart at the location by applying Laplace's law to the change in the local radius.

13. A method according to claim 4 comprising determining the activity of the heart at the location.

14. A method according to claim 13, wherein determining the activity comprises determining a relative motion profile of the location on the heart wall relative to neighboring locations.

15. A method according to claim 14 comprising determining local pathologies in the heart based on the relative motion profile.

16. A method according to claim 13, wherein determining the activity comprises determining a motion profile of the heart at the location.

17. A method according to claim 16 comprising determining local pathologies in the heart based on the motion profile.

18. A method according to claim 16 comprising monitoring the stability of the contact between the probe and the heart based on the motion profile.

19. A method according to claim 18, wherein monitoring comprises detecting changes in the motion profile for different heart cycles.

20. A method according to claim 18, wherein monitoring comprises detecting differences in positions of the probe at the same phase for different heart cycles.

21. A method according to claim 4 comprising binning positions according to characteristics of the heart cycle.

22. A method according to claim 21 comprising separately combining the information in each bin into a map.

23. A method according to claim 22 comprising determining differences between the maps.

24. A method according to claim 23 comprising determining local pathologies in the heart based on the determined differences between maps.

25. A method according to claim 21, wherein the characteristics comprise a heart rate.

26. A method according to claim 21, wherein the characteristics comprise a morphology of an ECG of the heart.

27. A method according to claim 1 comprising determining local information at the location at which the position of the probe is determined and wherein combining the positions comprises combining the positions and the local information to form a map incorporating the local information.

28. A method according to claim 27 comprising, analyzing the map to determine overstressed portions of the heart.

29. A method according to claim 27, wherein the local information is determined using a sensor not mounted on the probe.

30. A method according to claim 27, wherein the local information is determined using a sensor external to the body.

31. A method according to claim 27, wherein the local information is determined using a sensor on the probe.

32. A method according to claim 27, wherein the local information and the position of the probe are determined at substantially the same time.

33. A method according to claim 27, wherein the local information and the position of the probe are determined at substantially different times.

34. A method according to claim 27 comprising determining a relationship between changes in positions of the probe and determined local information at at least one location.

35. A method according to claim 34 comprising determining local pathologies in the heart based on the at least one local relationship.

36. A method according to claim 27, wherein the local information comprises a chemical concentration value.

37. A method according to claim 27, wherein the local information comprises a thickness of the heart at the location.

38. A method according to claim 37, wherein the thickness of the heart is determined using an ultrasonic transducer mounted on the probe.

39. A method according to claim 27, wherein the local information comprises a measure of a perfusion of the heart at the location.

40. A method according to claim 27, wherein the local information comprises a measure of the work performed by the heart portion at the location.

41. A method according to claim 27, wherein the local information comprises local electrical activity.

42. A method according to claim 41, wherein the electrical activity comprises a local electrogram.

43. A method according to claim 41, wherein the electrical activity comprises a local activation time.

44. A method according to claim 41, wherein the electrical activity comprises a local plateau duration of heart tissue at the location.

45. A method according to claim 27, wherein the probe is located in a coronary vein or artery.

46. A method according to claim 27, wherein the probe is located outside a blood vessel.

47. A method according to claim 1 comprising determining local information at at least two phases of the heart cycle at a location and wherein combining the positions comprises combining the positions and the local information to form a map comprising phase dependent local information.

48. A method according to claim 47 comprising analyzing changes in the determined local information.

49. A method according to claim 48 comprising determining local pathologies in the heart based on the changes in the local information.

50. A method according to claim 49, wherein the changes are a function of the heart cycle and further comprising determining the phase of the heart cycle at which the local information is determined.

51. A method according to claim 49, comprising determining local electrical activity at the location and wherein the changes are related to local electrical activity at the location.

52. A method according to claim 47 comprising analyzing the map to determine underutilized portions of the heart.

53. A method according to claim 47 comprising analyzing the map to determine procedures for improving the operation of the heart.

54. A method according to claim 47, wherein the local information comprises a thickness of the heart, and further comprising determining a reaction of the heart to an activation signal by analyzing changes in the thickness of the heart.

55. A method according to claim 47, further comprising binning local information according to characteristics of the heart cycle.

56. A method according to claim 55, wherein the characteristics comprise a heart rate.

57. A method according to claim 55, wherein the characteristics comprise a morphology of an ECG of the heart.

58. A method according to claim 1, further comprising reconstructing a surface portion of the heart.

59. A method according to claim 58 comprising determining local pathologies in the heart based on the reconstructed surface portion.

60. A method according to claim 1, wherein the positions of the probe are positions determined relative to a reference location.

61. A method according to claim 60, wherein the reference location is a predetermined portion of the heart.

62. A method according to claim 60, wherein a position of the reference location is determined using a position sensor.

63. A method according to claim 60, comprising periodically determining a position of the reference location.

64. A method according to claim 63, wherein the position of the reference location is acquired at the same phase of consecutive cardiac cycles.

65. A method according to claim 1, wherein the probe is located in a coronary vein or artery.

66. A method according to claim 1, wherein the probe is located outside a blood vessel.

67. A method of determining the structure of at least a portion of a heart having a heart cycle comprising:

(a) bringing a probe into contact with a location on a wall of the heart;

(b) determining a position in space of the probe at the location;

(c) acquiring data at the position in space;

(d) repeating (a), (b) and (c) for a multiplicity of locations of the heart to determine a multiplicity of data each associated with a determined position of the probe in space; and

(e) combining the multiplicity of the data and the determined positions of the probe in space to determine a map, containing said data, of at least a portion of the heart, said positions in space being determined solely from information other than that derived from an image of the vicinity of the probe at the locations.

68. A method according to claim 67 wherein the map is a phase dependent map of said data.

69. A method according to claim 67 wherein the data comprises local chemical concentration values and wherein the map comprises a map of said chemical concentration values.

70. A method according to claim 67 wherein said data comprises the thickness of the heart at said locations and wherein the map comprises a map of thickness of the heart.

71. A method according to claim 67 wherein the data comprises local perfusion of the heart at at least some of said locations and wherein the map comprises a perfusion map of at least a portion of the heart.

72. A method according to claim 67 wherein the data is used to determine local work performed at at least some of said locations and wherein the map comprises a map of the work performed at locations of the heart.

73. A method according to claim 67 wherein the data comprises electrical activity at at least some of the locations and wherein the map comprises a map of local electrical activity.

74. A method according to claim 67 wherein the data comprises local activation time at at least some of the locations and wherein the map comprises a map of local activation time.

75. A method according to claim 67 wherein the data is utilized to determine a local plateau duration at a plurality of locations and wherein the map comprises a map of local plateau duration.

76. A method according to claim 67 wherein the positions are determined with respect to a reference location.

77. A method according to claim 76 wherein the reference location is a location which is fixed in the moving heart.

78. A method according to claim 77 wherein the position in space of the reference location is determined using a position sensor.

79. A method of performing measurements of a heart having a heart cycle comprising:

(a) bringing a probe into contact with a location on a wall of the heart;

(b) determining a first position in space of the probe at the location for a first phase of the heart;

(c) repeating (b) at the location, for a second phase of the heart, to determine a second position of the probe in space; and

(d) calculating the movement of the heart at the location utilizing the first and second determined positions of the probe in space.

80. A method according to claim 79 wherein the positions are determined with respect to a reference location.

81. A method according to claim 80 wherein the reference location is a location which is fixed in the moving heart.

82. A method according to claim 79 and including repeating steps (a) to (d) for a multiplicity of different locations on the heart.

83. A method according to claim 82 and including mapping the determined motions of the heart at different locations to generate a map of heart wall motion for at least a portion of the heart.

84. A method according to claim 82 wherein the position in space of the probe is determined using a position sensor.

85. A method of determining the structure of at least a portion of a heart having a heart cycle comprising:

(a) bringing a probe into contact with a location on a wall of the heart;

(b) determining a position in space of the probe at the location;

(c) acquiring data at the position of the probe in space;

(d) repeating (a), (b) and (c) for a multiplicity of locations of the heart to determine a multiplicity of data each associated with a determined position of the probe in space; and

(e) combining the multiplicity of the data and the determined positions of the probe in space to determine a map of at least a portion of the heart containing said data, without utilizing, prior to or during said combining, an image of the heart other than one reconstructed from the determined positions of the probe in space.

86. A method according to claim 85 wherein the map is a phase dependent map of said data.

87. A method according to claim 85 wherein the data comprises local chemical concentration values and wherein the map comprises a map of said chemical concentration values.

88. A method according to claim 85 wherein said data comprises the thickness of the heart at said locations and wherein the map comprises a map of thickness of the heart.

89. A method according to claim 85 wherein the data comprises local perfusion of the heart at at least some of said locations and wherein the map comprises a perfusion map of at least a portion of the heart.

90. A method according to claim 85 wherein the data is used to determine local work performed at at least some of said locations and wherein the map comprises a map of the work performed at locations of the heart.

91. A method according to claim 85 wherein the data comprises electrical activity at at least some of the locations and wherein the map comprises a map of local electrical activity.

92. A method according to claim 85 wherein the data comprises local activation time at at least some of the locations and wherein the map comprises a map of local activation time.

93. A method according to claim 85 wherein the data is utilized to determine a local plateau duration at a plurality of locations wherein the map comprises a map of local plateau duration.

94. A method according to claim 85 wherein the positions are determined with respect to a reference location.

95. A method according to claim 94 wherein the reference location is a location which is fixed in the moving heart.

96. A method according to claim 95 wherein the position in space of the reference location is determined using a position sensor.

97. Apparatus for constructing a map of the heart having a heart cycle comprising:

a probe, having a distal end and adapted for contact of the distal end with a location on the inner heart wall;

means for determining the position in space of the distal end of the probe at the location; and

computing circuitry which combines a multiplicity of positions of the distal end of the probe in space determined at different locations on the heart to form a structural map of at least a portion of the heart.

98. Apparatus according to claim 97 wherein the probe has a position sensor located adjacent the distal end wherein the means for determining the position determines the position based on a determination of the position of the position sensor.

99. Apparatus according to claim 97 and including means for determining contact of the probe during said position determination.

100. Apparatus according to claim 97 wherein the means for determining the position of the distal end of the probe comprises means for determining the position of the distal end of the probe with respect to a reference location.

101. Apparatus according to claim 100 wherein the means for determining the position of the distal end of the probe with respect to a reference location comprises means for determining the position of a reference location fixed in the moving heart.

102. Apparatus according to claim 101 wherein the means for determining the position of a reference location fixed in the moving heart comprises a position sensor placed at the reference location.

103. Apparatus for performing measurements of a heart having a heart cycle, the apparatus comprising:

a probe, having a distal end and adapted for contact of the distal end with a location on the inner heart wall;

means for determining the position in space of the distal end of the probe at the location; and

computing circuitry which combines a multiplicity of positions in space of the distal end of the probe determined at different locations on the heart to form a map without utilizing an image of a region surrounding the distal end of the probe at the position.

104. Apparatus according to claim 103 wherein the probe has a position sensor located adjacent the distal end wherein the means for determining the position determines the position based on a determination of the position of the position sensor.

105. Apparatus according to claim 103 and including means for determining contact of the probe during said position determination.

106. Apparatus according to claim 103 wherein the map is a structural map of at least a portion of the heart.

107. Apparatus according to claim 103 wherein the means for determining the position of the distal end of the probe comprises means for determining the position of the distal end of the probe with respect to a reference location.

108. Apparatus according to claim 107 wherein the means for determining the position of the distal end of the probe with respect to a reference location comprises means for determining the position of a reference location fixed in the moving heart.

109. Apparatus according to claim 108 wherein the means for determining the position of a reference location fixed in the moving heart comprises a position sensor placed at the reference location.

110. Apparatus for performing measurements of a heart having a heart cycle, the apparatus comprising:

a probe, having a distal end and adapted for contact of the distal end with a location on the heart wall;

means for determining the position in space of the distal end of the probe at the location; and

computing circuitry which combines a plurality of positions of the distal end of the probe in space, determined at a particular location for a plurality of cycles of the heart.

111. Apparatus according to claim 110 wherein the plurality of positions are combined by the computing circuitry to determine the movement of the heart wall at the location.

112. Apparatus according to claim 111 wherein the computing circuitry combines a plurality of determined movements at different locations of the heart wall to form a map of heart wall movement.

113. Apparatus according to claim 110 wherein the means for determining the position of the distal end of the probe comprises means for determining the position of the distal end of the probe with respect to a reference location.

114. Apparatus according to claim 113 wherein the means for determining the position of the distal end of the probe with respect to a reference location comprises means for determining the position of a reference location fixed in the moving heart.

115. Apparatus according to claim 114 wherein the means for determining the position of a reference location fixed in the moving heart comprises a position sensor placed at the reference location.

116. Apparatus for performing measurements of a heart having a heart cycle, the apparatus comprising:

a probe, having a distal end and adapted for contact of the distal end with a location on the inner heart wall;

means for determining the position in space of the distal end at the location;

means for determining local information at the location, referenced to the position of the distal end in space; and

computing circuitry which combines the multiplicity of the data and the determined positions of the probe in space to determine a map, containing said data, of at least a portion of the heart, without utilizing, prior to or during said combining, an image of the heart other than one reconstructed from the determined positions.

117. Apparatus according to claim 116 wherein the means for determining the position of the distal end of the probe comprises means for determining the position of the distal end of the probe with respect to a reference location.

118. Apparatus according to claim 117 wherein the means for determining the position of the distal end of the probe with respect to a reference location comprises means for determining the position of a reference location fixed in the moving heart.

119. Apparatus according to claim 118 wherein the means for determining the position of a reference location fixed in the moving heart comprises a position sensor placed at the reference location.
Description


FIELD OF THE INVENTION

The present invention relates to the field of cardiac medicine and more particularly to diagnosing and treating diseased hearts based on the interaction between cardiac electro-physiological and cardiac bio-mechanical activity.

BACKGROUND OF THE INVENTION

Cardiovascular diseases accounted for approximately 43 percent of the mortality in the United States of America in 1991 (923,000 persons). However, many of these deaths are not directly caused by an acute myocardial infraction (AMI). Rather, many patients suffer a general decline in their cardiac output known as heart failure. Once the overt signs of heart failure appear, half the patients die within five years. It is estimated that between two and three million Americans suffer from heart failure and an estimated 200,000 new cases appear every year. In many cases heart failure is caused by damage accumulated in the patient's heart, such as damage caused by disease, chronic and acute ischemia and especially (.about.75%) as a result of hypertension.

A short discussion of the operation of a healthy heart is useful in order to appreciate the complexity of the functioning of the heart and the multitude of pathologies which can cause heart failure. FIG. 1A is a schematic drawing of a cross-section of a healthy heart 20. In general heart 20 comprises two independent pumps. One pump comprises a right atrium 22 and a right ventricle 24 which pump venous blood from an inferior and a superior vena cava to a pair of lungs (not shown) to be oxygenated. Another pump comprises a left atrium 26 and a left ventricle 28, which pump blood from pulmonary veins (not shown) to a plurality of body systems, including heart 20 itself. The two ventricles are separated by a ventricular septum 30 and the two atria are separated by an atrial septum 32.

Heart 20 has a four phase operational cycle in which the two pumps are activated synchronously. FIG. 1B shows a first phase, called systole. During this phase, right ventricle 24 contracts and ejects blood through a pulmonic valve 34 to the lungs. At the same time, left ventricle 28 contracts and ejects blood through an aortic valve 36 and into an aorta 38. Right atrium 22 and left atrium 26 are relaxed at this point and they begin filling with blood, however, this preliminary filling is limited by distortion of the atria which is caused by the contraction of the ventricles.

FIG. 1C shows a second phase, called rapid filling phase and indicates the start of a diastole. During this phase, right ventricle 24 relaxes and fills with blood flowing from right atrium 22 through a tricuspid valve 40, which is open during this phase. Pulmonic valve 34 is closed, so that no blood leaves right ventricle 24 during this phase. Left ventricle 28 also relaxes and is filled with blood flowing from left atrium 26 through a mitral valve 42, which is open. Aortic valve 36 is also closed to prevent blood from leaving left ventricle 26 during this phase. The filling of the two ventricles during this phase is affected by an existing venous pressure. Right atrium 22 and left atrium 26 also begin filling during this phase. However, due to relaxation of the ventricles, their pressure is lower than the pressure in the atria, so tricuspid valve 40 and mitral valve 42 stay open and blood flows from the atria into the ventricles.

FIG. 1D shows a third phase called diastatis, which indicates the middle of the diastole. During this phase, the ventricles fill very slowly. The slowdown in filling rate is due to the equalization of pressure between the venous pressure and the intra-cardiac pressure. In addition, the pressure gradient between the atria and the ventricles is also reduced.

FIG. 1E shows a fourth phase called atrial systole which indicates the end of the diastole and the start of the systole of the atria. During this phase, the atria contract and inject blood into the ventricles. Although there are no valves guarding the veins entering the atria, there are some mechanisms to prevent backflow during atrial systole. In left atrium 26, sleeves of atrial muscle extend for one or two centimeters along the pulmonary veins and tend to exert a sphincter-like effect on the veins. In right atrium 22, a crescentic valve forms a rudimentary valve called the eustachian valve which covers the inferior vena cava. In addition, there may be muscular bands which surround the vena cava veins at their entrance to right atria 22.

FIG. 1F is a graph showing the volume of left ventricle 24 as a function of the cardiac cycle. FIG. 1F clearly shows the additional volume of blood injected into the ventricles by the atria during atrial systole as well as the variance of the heart volume during a normal cardiac cycle. FIG. 1G is a graph which shows the time derivative of FIG. 1F, i.e., the left ventricle fill rate as a function of cardiac cycle. In FIG. 1G two peak fill rates are shown, one in the beginning of diastole and the other during atrial systole.

An important timing consideration in the cardiac cycle is that the atrial systole must complete before the ventricular systole begins. If there is an overlap between the atrial and ventricular systoles, the atria will have to force blood into the ventricle against a raising pressure, which reduces the volume of injected blood. In some pathological and induced cases, described below, the atrial systole is not synchronized to the ventricular systole, with the effect of a lower than optimal cardiac output.

It should be noted that even though the left and the right sides of heart 20 operate in synchronization with each other, their phases do not overlap. In general, right atrial systole starts slightly before left atrial systole and left ventricular systole starts slightly before right ventricular systole. Moreover, the injection of blood from left ventricle 26 into aorta 38 usually begins slightly after the start of injection of blood from right ventricle 24 towards the lungs and ends slightly before end of injection of blood from right ventricle 24. This is caused by pressures differences between the pulmonary and body circulatory systems.

When heart 20 contracts (during systole), the ventricle does not contract in a linear fashion, such as shortening of one dimension or in a radial fashion. Rather, the change in the shape of the ventricle is progressive along its length and involves a twisting effect which tends to squeeze out more blood. It should be appreciated that blood which remains in one place without moving, even in the heart, can clot, so it is very important to eject as much blood as possible out of the heart. FIG. 2 shows an arrangement of a plurality of muscle fibers 44 around left ventricle 28 which enables this type of contraction. When muscle fibers 44 are arranged in a spiral manner as shown in FIG. 2 and the activation of muscle fibers 44 is started from an apex 46 of left ventricle 28, left ventricle 28 is progressively reduced in volume from the bottom up. The spiral arrangement of muscle fibers 44 is important because muscle fibers typically contract no more than 50% in length. A spiral arrangement results in a greater change of left ventricular volume than is possible with, for example, a flat arrangement in which the fibers are arranged in bands around the heart. An additional benefit of the spiral arrangement is a leverage effect. In a flat arrangement, a contraction of 10% of a muscle fiber translates into a reduction of 10% of the ventricular radius. In a spiral arrangement with, for example, a spiral angle 48 of 45.degree., a 10% contraction translates into a 7.07% contraction in ventricular radius and a 7.07% reduction in ventricular length. Since the ventricular radius is typically smaller than the ventricular length, the net result is that, depending on spiral angle 48, a tradeoff is effected between a given amount of contraction and the amount of force exerted by that contraction.

Spiral angle 48 is not constant, rather, spiral angle 48 changes with the distance of a muscle fiber from the outer wall of the ventricle. The amount of force produced by a muscle fiber is a function of its contraction, thus, each layer is optimized to produce an optimal amount of force. Since the contraction of each muscle fiber is synchronous with the increase in the ventricular pressure (caused by the muscle contraction), it might be expected that the muscle fibers produce a maximum force at maximum contraction. However, physiological constraints on muscle fibers denote that maximal force is generated before maximal contraction. In addition, the force exerted by a muscle fiber begins to fall soon after maximum force is exerted. The varying spiral angle is a mechanism which makes it possible to increase the contractile force on the ventricle after maximum force is reached by a particular muscle fiber.

As described above, activation of the heart muscle is from the apex up. Thus, the muscle on the top of the ventricle could theoretically exert more force than the muscle at apex 46, which would cause a distention at apex 46. The varying spiral angle is one mechanism to avoid distention. Another mechanism is that the muscle near apex 46, which is activated first, is slightly more developed than the muscle at the top of the ventricle, which is activated last. As a result of the above described mechanisms, the force exerted by the ventricular wall is more evenly distributed over time and space.

As can be appreciated, a complicated mechanism is required to synchronize the activation of muscle fibers 44 so that an efficient four phase cycle is achieved. This synchronization mechanism is provided by an electrical conduction system within the heart which conducts an electrical activation signal from a (natural) cardiac pacemaker to muscle fibers 44.

FIG. 3 shows the main conduction pathways in heart 20. An SA node 50, located in right atrium 22, generates an activation signal for initiating contraction of muscle fibers 44. The activation signal is transmitted along a conduction pathway 54 to left atria 26 where the activation signal is locally disseminated via Bachman bundles and Crista terminals. The activation signal for contracting the left and right ventricles is conducted from SA node 50 to an AV node 52, where the activation signal is delayed. The ventricles are normally electrically insulated from the atria by non-conducting fibrous tissue, so the activation signal must travel through special conduction pathways. A left ventricle activation signal travels along a left pathway 58 to activate left ventricle 28 and a right ventricle activation signal travels along a right pathway 56 to activate right ventricle 24. The activation signal is locally disseminated in the left and right ventricles via Purkinje fibers 60. Generally, the conduction pathways convey the activation signal to apex 46 where they are locally disseminated via Purkinje fibers 60 and propagation over the rest of the heart is achieved by conduction in muscle fibers 44. In general, the activation of the heart is from the inner surface towards the outer surface. It should be noted that electrical conduction in muscle fibers 44 is generally faster along the direction of the muscle fibers. Thus, the conduction velocity of the activation signals in heart 20 is generally anisotropic.

As can be appreciated, the delay in AV node 52 results, in a healthy heart, in proper ventricular systolic sequencing. The temporal distribution of the activation signal in the ventricular muscle results in the activation of the ventricles from the apex up. In a healthy heart the activation signal propagates across left ventricle 28 in approximately 60 milliseconds. In an externally paced heart, where the activation signal is not conducted through Purkinje fibers 60 or in a diseased heart, the propagation time is typically longer, such as 150 milliseconds. Thus, disease and external pacing affect the activation profile of the heart.

Cardiac muscle cells usually exhibit a binary reaction to an activation signal; either the cell responds normally to the activation signal or it does not respond at all. FIG. 4 is a graph showing changes in the voltage of a single cardiac muscle cell in reaction to the activation signal. The reaction is generally divided into five stages. A rapid depolarization stage 62 occurs when the muscle cell receives an activation signal. During this stage, which lasts a few milliseconds, the potential of the cell becomes rapidly positive. After depolarization, the muscle fiber rapidly repolarizes during a rapid repolarization stage 64 until the cell voltage is approximately zero. During a slow repolarization stage 66, also known as the plateau, the muscle cell contracts. The duration of stage 66, the plateau duration, is directly related to the amount of work performed by the muscle cell. A relatively fast repolarization stage 68 follows, where the muscle cell repolarizes to its original potential. Stage 66 is also known as the refractory period, during which the cell cannot be activated by another activation signal. During stage 68, the cell is in a relative refractory period, during which the cell can be activated by an exceptionally strong activation signal. A steady state 70 follows in which the muscle cell is ready for another activation.

It should be appreciated that the contraction of cardiac muscle cells is delayed in time from their activation. In addition the duration of the contraction is generally equal to the duration of the plateau.

An important factor which may affect the length of the plateau is the existence of ionic currents which propagate from the most recently activated portions of the heart towards the earlier activated portions of the heart. As can be appreciated, the ionic current starts at the last activated portion of the heart and progresses back along the path of the activation. Thus, it is the later activated portions of the heart which are first affected by the ionic current. As a result, the repolarization of these cells is relatively faster than the repolarization of the first activated muscle fibers, and their contraction time is relatively shorter. As can be appreciated, in a healthy heart, where the propagation time of the activation signal is relatively short, the ionic currents are significantly smaller than in a diseased or externally paced heart.

One of the main results of the contraction of the ventricles is increased intra-ventricular pressure. In general, when the intra-cardiac pressure is higher, the outflow from the heart into the circulatory system is stronger and the efficiency of the heart is higher. A mathematical relationship termed Laplace's law can be used to model the relationship between the pressure in the ventricle and the tension in the wall of the ventricle. Laplace's law was formulated for generally spherical or cylindrical chambers with a distentible wall, however, the law can be applied to the ventricles since they are generally elongated spherical in shape. FIGS. 5A-C show three formulations for determining the tension in a portion of the ventricle wall, all of which are based of the law of Laplace. In FIG. 5A, the tension across a cross-section of the wall is shown wherein T, the tension in the wall, is equal to the product of P, the transmural pressure across the wall, r (squared), the radius of the ventricle, and .pi.. FIGS. 5B and C show formulas for calculating the tension per unit in portions of the ventricular wall, for example in FIG. 5C, for a unit cross-sectional area of muscle in a wall of thickness .delta..

As can be appreciated, if r, the radius of the ventricle, is large, a higher tension is needed to produce the same pressure change as in a ventricle with a smaller radius. This is one of the reasons that ventricular dilation usually leads to heart failure. The heart muscle is required to produce a higher tension is order to achieve the same pressure gradient. However, the heart is not capable of producing the required tension, so, the pressure gradient, and thus the cardiac efficiency, are reduced.

Unfortunately, not all people have healthy hearts and vascular systems. Some types of heart problems are caused by disease. HCM (hypertrophic cardiomyopathy) is a disease in which the left ventricle and, in particular, the ventricular septum hypertrophy, sometimes to an extent which blocks the aortic exit from the left ventricle. Other diseases, such as atrophy causing diseases reduce the amount of muscle fibers in portions of the heart.

A very common cause of damage to the heart is ischemia of the heart muscle. This condition, especially when manifesting itself as an acute myocardial infraction (heart attack), can create dead zones in the heart which do not contain active muscle. An additional, and possibly more important effect, is the non-conducting nature of these dead zones which may upset the natural activation sequence of the heart. In some cases, damaged heart tissue continues to conduct the activation signal, albeit at a variable or lower velocity, which may cause arrhythmias.

A chronic ischemic condition is usually caused by blockage of the coronary arteries, usually by arteriosclerosis, which limits the amount of oxygen which can reach portions of the heart muscle. When more work (i.e., more tension) is required of the heart muscle and an increase in oxygen supply is not available, the result is acute pain, and if the supply is cut off for an extended period, death of the starved muscle will follow.

When the output of the heart is insufficient, a common result is hypertrophy of the heart, usually of the left ventricle. Hypertrophy is a compensatory mechanism of the heart for increasing the output volume. However, in a chronic condition, hypertrophy has generally negative effects. For example, arrhythmias, congestive heart failure (CHF) and permanent changes in the morphology of the heart muscle (ventricular modeling) may result from hypertrophy.

One of the most common cardio-vascular diseases is hypertension. A main effect of hypertension is increased cardiac output demand, which causes hypertrophy since the blood must be pumped against a higher pressure. Furthermore, hypertension usually aggravates other existing cardiac problems.

The human heart has many compensatory and adaptive mechanisms, termed cardiac reserve, so that not all cardiac pathologies manifest as heart disease. Once the cardiac reserve is used up, the heart cannot keep up with the demand and heart failure may result. One measure of heart function and efficiency is the left ventricle ejection factor, which is the ratio between the amount of blood in the left ventricle during diastole and the amount of blood exiting during systole. It should be noted that a significant portion of the change in ventricular volume between systole and diastole is due to the thickening of activated muscle fibers. Another measure of heart function is the left ventricle stroke volume, which is the amount of blood which is ejected from the left ventricle each heart beat. It should be noted that once the cardiac reserve is used up it is difficult, if not impossible, for the heart to increase its output when needed, such as during exercise.

There are many ways in which non-optimal timing of the activation of the heart can result in lower cardiac output. In AF (atrial fibrillation) one or both atria does not contract in correct sequence with its associated ventricle. As a first result, the atria does not inject blood into its associated ventricle during atrial systole, so the ventricle volume is not maximized before ventricular systole, and stroke volume is slightly reduced. If the right atria is fibrillating, sequencing of the AV node is non-regular, which results in the ventricles contracting at an irregular rate, and the heart output is further reduced.

In some cases of a conduction block between the SA node and the ventricles, such as caused by a damaged AV node, the contraction of the atria is not synchronized to the contraction of the ventricles, which also results in a lower heart output.

Another type of timing deficiency results when there are large dead areas in the heart muscle which do not conduct electrical signals. The activation signal must circumvent the dead areas, which results in a longer pathway (and longer delay time) for the activation signal reaching some portions of the heart. In some cases, these portions of the heart are activated long after the rest of the heart has already contracted, which results in a reduced contribution of these portions to the total cardiac output.

Heart muscle which is stressed before it is activated, heart muscle which is weakened (such as by ischemia) and portions of the heart which have turned into scar tissue, may form aneurysms. As can be appreciated from Laplace's law, portions of the ventricle wall which do not generate enough tension to offset the tension induced by the intra-cardiac pressure must increase their local radius in response to the pressure overload. The stretched wall portion thins out and may burst, resulting in the death of the patient. The apex of the left ventricle is especially susceptible to aneurysms since it may be very thin. In addition, the total pressure in the ventricle and the flow from the ventricle are reduced as the aneurysm grows, so the heart output is also reduced. Although weak muscle should be expected to hypertrophy in response to the greater need, in some cases, such as after an AMI, hypertrophy may not occur before irreversible tissue changes are caused by the stretching.

Perfusion of the heart muscle usually occurs during diastole. However, if the diastole is very long, such as when the activation signal is propagated slowly, some portions of the heart may not be oxygenated properly, resulting in functional ischemia.

As mentioned above, one of the adaptation mechanisms of the heart is hypertrophy, in which the size of the heart increases to answer increased demand. However, hypertrophy increases the danger of arrhythmias, which in some cases reduce heart output and in others, such as VF (ventricular fibrillation) are life threatening. Arrhythmias are also caused by damaged heart tissues which generate erroneous activation signals and by blocks in the conduction system of the heart.

In some cases arrhythmias of the heart are treated using medicines, in others, by implanting a pacemaker or a defibrillator. A common pacemaker implanting procedure, for example for treating the effects of AF, includes:

(a) ablating or removing the AV node; and

(b) implanting a pacing electrode in the apex of the heart. The location of the pacing electrode may be changed (during the procedure) if the heart does not beat at a desired sequence for a given output of the pacemaker.

It is also known to pace using multiple electrodes, where the activation signal is initiated from a selected one or more of the electrodes, depending on sensed electrical values, such as sequence, activation time and depolarization state. Typically, the pacing regime is adapted to a specific arrhythmia. Sometimes, logic is included in the pacemaker which enables it to identify and respond to several types of arrhythmia.

U.S. Pat. No. 5,403,356 to Hill et al. describes a method of preventing atrial arrhythmias by adapting the pacing in the right atrium in response to a sensed atrial depolarization, which may indicate an arrhythmia.

Sometimes the pacing is performed for more than one chamber. For example, in dual chamber pacing, both left and right ventricles are separately paced. There have been attempts to use dual chamber pacing to relive aortic obstruction caused by HCM. The aortic exit from the left ventricle is located between the left and right ventricle, so that when both ventricles contract simultaneously, the aorta is squeezed from all sides. In a healthy heart, the ventricular septum does not obstruct the aorta, however, in an HCM-diseased heart, the enlarged septum obstructs the aortic exit from the left ventricle. When pacing to reduce aortic obstruction, the contractions of the left and right ventricles are stepped, so that when the left ventricle contracts, the right ventricle dilates and the aorta is less compressed.

Lameh Fananapazir, et al., in "Long-Term Results Of Dual-Chamber (DDD) Pacing In Obstructive Hypertrophic Cardiomyopathy", Circulation, Vol. 90, No. 60, pp 2731-2742, December 1994, describes the effects of pacing a HCM-diseased heart using DDD pacing at the apex of the right ventricle. One effect is that the muscle mass near the pacing location is reduced, i.e., the ventricular septum is atrophied. The atrophy is hypothesized to be caused by the changes in workload at the paced location which are due to the late activation time of ventricular segments far from the pacing location.

Margarete Hochleitner, et al., in "Long-Term Efficiency Of Physiologic Dual-Chamber Pacing In The Treatment Of End-Stage Idiopathic Dilated Cardiomyopathy", American Journal of Cardialogy, volume 70, pp 1320-1325, 1992, describes the effect of DDD pacing on hearts which are dilated as a result of idiopathic dilated cardiomyopathy. DDD pacing resulted in an improvement of cardiac function and in a reduction in hypertrophy in several patients. In addition, it is suggested that positioning the ventricular electrode of the DDD pacemaker in near the apex of the right ventricle reduced the stress at the apex of the left ventricle, by its early activation.

Xavier Jeanrenaud, et al., in "Effects Of Dual Chamber Pacing In Hypertrophic Obstructive Cardiomypathy", The Lancet, Vol. 339, pp 1318-1322, May 30, 1992, teaches that to ensure success of DDD pacing in HCM diseased hearts, an optimum AV interval (between atrial activation and ventricular activation) is required.

Several methods may be used to treat heart failure. One method is to connect assist pumps to the patient's circulatory system, which assist the heart by circulating the blood. To date, no satisfactory long-term assist pump has been developed. In some cases, a diseased heart is removed and replaced by another human heart. However, this is an expensive, complicated and dangerous operation and not many donor hearts are available. Artificial hearts suffer from the same limitations as assist pumps and, like them, are not yet practical.

Certain types of heart failure, such as those caused by conduction blocks in the AV node or by AF can be helped by the implantation of a pacemaker, as described above.

Some cases of heart failure can be helped by medicines which either strengthen the heart, correct arrhythmias or reduce the total volume of blood in the body (which reduces blood pressure). However, many cases of heart failure can only be treated by reducing the activity of the patient. Ultimately, once the cardiac reserve is used up, most cases of heart failure cannot be treated and result in death.

U.S. Pat. No. 5,391,199, the disclosure of which is incorporated herein by reference, discloses apparatus and method for mapping the electrical activity of the heart.

SUMMARY OF THE INVENTION

It is an object of some aspects of the present invention to provide methods of augmenting the compensatory mechanisms of the heart.

Another object of some aspects of the present invention is to provide methods of mapping the local physiological values and/or the shape of the heart to determine the activation profile of the heart and, preferably, to analyze the resulting maps to determine possible optimizations in the activation profile.

Yet another object of some aspects of the present invention is to control the adaptation mechanisms in the heart so that the heart output or some other parameter of the heart is optimized. Alternatively or additionally, the adaptation mechanisms of the heart are utilized to effect change in the morphology of the heart, such as by redistributing muscle mass.

Still another object of some aspects of the present invention is to control the activation sequence of the heart so that the heart output or some other physiological variable of the heart is optimized, preferably, in real-time.

When used herein, the terms "physiological variable" and "cardiac parameter" do not include electrical activity, rate, arrhythmia or sequencing of the heart. The term "local physiological value" does not include electrical activity, per se, rather it refers to a local physiological state, such as contraction of local heart muscle, perfusion or thickness. The term "location" refers to a location on or in an object, such as the heart muscle. For example, a valve or an apex of the heart. "Position" refers to a position in space, usually relative to a known portion of the heart, for example, 1.5 inches perpendicular from the apex of the heart.

An object of some aspects of the present invention is related to pacemakers which are adapted to control the adaptation mechanisms of the heart and/or to optimize heart parameters.

In a preferred embodiment of the invention, the mechanical motion of the heart muscle is mapped using a catheter having a position sensor near its distal end. The mapping includes:

(a) placing the catheter into contact with the heart wall;

(b) determining the position of the distal end of the catheter; and

(c) repeating step (b) for additional locations in the heart.

Preferably, the catheter is in contact with the heart wall through the entire cardiac cycle. It should be appreciated that contact with the heart wall can be achieved either from the inside or from the outside of the heart, such as outside contact being achieved by inserting the catheter into the coronary arteries and/or veins. Alternatively, the catheter is directly inserted into the body (not through the vascular system), such as through a lacoroscope or during surgery.

Preferably, (b) includes determining the position of the catheter at at least two instants of an entire heart cycle. More preferably, it includes determining the position with time over the cycle. Alternatively or additionally, the catheter has a plurality of distal ends, each with a position sensor and (b) includes determining the position of each one of the ends.

Preferably, the catheter does not move between sequential diastoles. This can be asserted, for example, by using an impedance sensor, by determining changes in a locally sensed electrogram, by determining that the position sensor repeats its trajectory during heart cycles or by determining that the catheter returns to the same location each diastole or other recognizable portion of the cardiac cycle.

Preferably, the mapping further includes determining the geometry and/or changes in the geometry of at least a portion of the heart as a function of time and/or phase of the cardiac cycle. For example, the existence of an aneurysm can be determined from a characteristic bulge of the aneurysm during systole. Likewise, a dilated ventricle can be determined from the determined volume. Additionally or alternatively, the mapping includes determining the local radius of a portion of the heart wall.

Preferably the catheter comprises a pressure sensor which measures the intra-cardiac pressure. Further preferably, the forces on the heart wall are calculated using the local radius and/or the determined pressure, preferably using Laplace's law.

Preferably, the catheter includes at least one electrode for determining the local electrical activity of the heart. Preferably, the local activation time and/or the activation signal is measured and incorporated in a map of the heart. Additionally or alternatively, local electrical conductivity is measured, since fibrous scar tissue does not conduct as well as viable muscle tissue.

A preferred embodiment of the invention provides a map which compares the local activation time to the movement of a segment of local heart wall. Preferably, the map compares activation time of the segment to movement of the segment relative to the movement of surrounding segments. Thus, the reaction of a muscle segment to the activation signal can be determined from the local geometrical changes.

In a preferred embodiment of the invention, the instantaneous thickness of the heart wall at the point of contact is also determined. Preferably, the thickness is measured using an ultrasonic transducer, preferably mounted on the distal portion of the catheter. Preferably, changes in the thickness of the cardiac wall are used to determine the reaction of the heart muscle to the activation signal. Typically, when the muscle contracts, the wall thickens, while if the muscle does not react and the intra-cardiac pressure rises, the wall thins.

In a preferred embodiment of the invention provides a map of the local energy expenditure of the heart. Preferably, the local energy expenditure is determined using Laplace's law, local changes in thickness and a pressure sensor, mounted on the catheter, which determines the intra-cardiac pressure.

In preferred embodiments of the invention, additional or alternative sensors are mounted on the distal end of the catheter and are used in constructing cardiac maps. For example, a Doppler ultrasonic sensor which measures perfusion may be used to determine the local perfusion as a function of time and workload. Additionally or alternatively, an ionic sensor is used to sense changes in ion concentrations.

Although the above maps are described as being time based or cardiac-phase based, in a preferred embodiment of the invention, measurements are binned based on geometrical characteristics of the heart or on ECG or electrogram characteristics. Preferably, the ECG characteristics comprise pulse rate and/or ECG morphology.

Preferably, maps constructed before a cardiac procedure are compared to maps constructed after a procedure to determine the effect of the procedure. In some instances, maps of the heart are constructed while the heart is artificially paced.

A preferred embodiment of the invention provides for changing the distribution of muscle-mass in the heart from an existing muscle-mass distribution to a desired muscle-mass distribution. This is achieved by adjusting the pacing of the heart to achieve an activation profile which affects such change. Preferably, portions of the heart which are relatively atrophied are activated so that relatively more effort is required of them than previously. Alternatively or additionally, portions of the heart which are hypertrophied are activated so that less effort is required of them than previously. Preferably, the decision how to change the activation profile of the heart is based on a map of the heart, further preferably, using a map which shows the local energy expenditure and/or the local work performed by each portion of the heart. Alternatively or additionally, a map which shows the ratio between local perfusion and local energy expenditure is used. Preferably, the activation profile of the heart is changed when the heart approaches the desired muscle mass distribution. Typically, the heart is paced using an implanted pacemaker. Preferably, a map is used to determine the optimal location for the pacing electrode(s). Additionally or alternatively, pharmaceuticals are used to affect the pacing.

One aspect of the invention relates to the optimal placement of pacemaker electrodes. A preferred method of determining electrode placement includes:

(a) pacing a heart from a first location;

(b) determining a value of a physiological variable while pacing at the first location;

(c) repeating (a) and (b) at least at a second location; and

(d) implanting the pacing electrode at a location of the first and second locations which yields an optimal value for the physiological variable or at a location with a response known to yield an optimal value in the future.

One preferred physiological variable is the stroke volume. Preferably, the physiological variable is measured using a catheter.

Yet another aspect of the invention relates to pacing a heart to reduce stress. A preferred method of pacing the heart includes:

(a) measuring a local physiological value at a plurality of locations in the heart;

(b) determining a pacing regime which will change the distribution of the value at the plurality of locations; and

(c) pacing the heart using the new pacing regime.

Preferably, the new pacing regime is determined such that the stress on certain portions of the heart will be reduced, preferably, by keeping the local physiological value within a range. Further preferably, the range is locally determined based on local conditions in the heart. One preferred local physiological value is blood perfusion. Preferably, (a)-(c) are performed substantially in real time. Further preferably, measuring the physiological value is performed substantially simultaneously at the plurality of locations.

Still another aspect of the invention relates to increasing the efficiency of a heart using adaptive pacing. A preferred method of adaptive pacing includes:

(a) determining a preferred pacing regime for a heart which is optimal with respect to a physiological variable; and

(b) pacing the heart using the preferred pacing regime.

Preferably, the preferred pacing regime is determined using a map of the heart. The map is preferably analyzed to determine which portions of the heart are under-utilized due to their activation time. The preferred pacing is preferably initiated by implanting a pacer, preferably, with a plurality of electrodes. Alternatively or additionally, the preferred pacing is initiated by changing the electrification of a plurality of previously implanted pacemaker electrodes.

In a preferred embodiment of the invention, the pacing regime is regularly changed so that each pacing regime optimizes the utilization of different portions of the heart. Additionally or alternatively, the pacing regime is regularly changed to temporally distribute workload between different portions of the heart.

Another aspect of the invention relates to pacemakers having adaptive pacing regimes. A preferred pacemaker includes:

a plurality of electrodes;

a source of electricity for electrifying the electrodes; and

a controller which changes the electrification of the electrodes in response to a plurality of measured local physiological values of a heart to achieve an optimization of a physiological variable of the heart.

The measured physiological values preferably include plateau length and/or activation time. Preferably, the measurement is performed using the pacemaker electrodes. Alternatively or additionally, measurement is performed using at least one additional sensor. One preferred physiological variable is stroke volume. Further preferably, the physiological variable is measured by the pacemaker, such as measuring intra-cardiac pressure using a solid-state pressure sensor.

Although the description of the present invention focuses on the heart, apparatus and methods described herein are also useful for mapping and affecting other organs, such as the stomach and other muscles. For example, in treating atrophied muscles using stimulation, an electro-mechanical map of the muscle is preferably acquired during a test stimulation to help in determining and optimal stimulation regime.

There is thus provided, in accordance with a preferred embodiment of the present invention, a method of constructing a map of a heart having a heart cycle comprising:

(a) bringing an probe into contact with a location on a wall of the heart;

(b) determining a position of the probe at the location;

(c) repeating (a)and(b) for a multiplicity of locations of the heart; and

(d) combining the positions to form a map of at least a portion of the heart.

In a preferred embodiment of the present invention, the method includes determining local pathologies in the heart based on the map.

In a preferred embodiment of the present invention, the method includes determining at least a second position of the probe at a phase of the cycle different from the phase at the position determination of (b) and wherein the map is a phase dependent geometric map. Preferably, the second position determination is performed at the location. Preferably, the method includes analyzing the map to determine underutilized portions of the heart. Additionally or alternatively, the method includes analyzing the map to determine procedures for improving the operation of the heart.

In a preferred embodiment of the present invention, the method includes determining local information at the location and wherein combining the positions comprises associating positions with locations and combining the locations and the local information to form a map of local information. Preferably, the method includes analyzing the map to determine overstressed portions of the heart. Preferably, the local information is determined using a sensor not mounted on the probe. According to one preferred embodiment, the local information is determined using a sensor external to the body. According to another preferred embodiment, the local information is determined using a sensor on the probe.

According to one preferred embodiment of the present invention, the local information and the position of the probe are determined at substantially the same time. In another preferred embodiment of the present invention, the local information and the position of the probe are determined at substantially different times.

In a preferred embodiment of the present invention, the method includes determining a relationship between changes in positions of the probe and determined local information at at least one location. Preferably, the method further includes determining local pathologies in the heart based on the at least one local relationship.

In a preferred embodiment of the present invention, the method includes determining local information at at least two phases of the heart cycle and wherein combining the positions comprises combining the positions and the local information to form a phase dependent map of local information. Preferably, the method further includes analyzing changes in the determined local information. Preferably, the method further includes determining local pathologies in the heart based on the changes in the local information. Preferably, the changes are a function of the heart cycle and further comprising determining the phase of the heart cycle at which the local information is determined.

In a preferred embodiment of the present invention, the method includes determining local electrical activity at the location and wherein the changes are related to local electrical activity at the location.

In a preferred embodiment of the present invention, the method includes analyzing the map to determine underutilized portions of the heart. Additionally or alternatively, the method includes analyzing the map to determine procedures for improving the operation of the heart.

In a preferred embodiment of the present invention, the local information comprises a chemical concentration value. Additionally or alternatively, the local information comprises a thickness of the heart at the location. Preferably, the thickness of the heart is determined using an ultrasonic transducer mounted on the probe.

In a preferred embodiment of the present invention, the local information includes the thickness of the heart and the method further includes determining a reaction of the heart to an activation signal by analyzing changes in the thickness of the heart.

In a preferred embodiment of the present invention, the local information comprises a measure of a perfusion of the heart at the location. Additionally or alternatively, the local information comprises a measure of the work performed by the heart portion at the location. Additionally or alternatively, the local information comprises local electrical activity. Preferably, the electrical activity comprises a local electrogram. Additionally or alternatively, the electrical activity comprises a local activation time.

Additionally or alternatively, the electrical activity comprises a local plateau duration of heart tissue at the location.

In a preferred embodiment of the present invention, the method includes determining a local change in the geometry of the heart. Preferably, the method further includes determining local pathologies in the heart based on the local changes in geometry. Preferably, the local change comprises a change in a local radius of the heart wall at the location. Preferably, the method includes determining an intra-cardiac pressure of the heart.

In a preferred embodiment of the present invention, the method includes determining a relative tension of the heart at the location by applying Laplace's law to the change in the local radius.

In a preferred embodiment of the present invention, the method includes determining the activity of the heart at the location. Preferably, determining the activity comprises determining a relative motion profile of the location on the heart wall relative to neighboring locations. Preferably, the method further includes determining local pathologies in the heart based on the relative motion profile. Preferably, determining the activity comprises determining a motion profile of the heart at the location. Preferably, the method includes determining local pathologies in the heart based on the motion profile. Preferably, the method includes monitoring the stability of the contact between the probe and the heart based on the motion profile. Preferably, monitoring comprises detecting changes in the motion profile for different heart cycles. Additionally or alternatively, monitoring comprises detecting differences in positions of the probe at the same phase for different heart cycles.

In a preferred embodiment of the present invention, the method includes reconstructing a surface portion of the heart. Preferably, the method further includes determining local pathologies in the heart based on the reconstructed surface portion.

In a preferred embodiment of the present invention, the method includes binning positions according to characteristics of the heart cycle. Preferably, the method further includes separately combining the information in each bin into a map. Preferably, the method further includes determining differences between the maps. Preferably, the method further includes determining local pathologies in the heart based on the determined differences between maps.

In a preferred embodiment of the present invention, the characteristics comprise a heart rate. Additionally or alternatively, the characteristics comprise a morphology of an ECG of the heart.

In a preferred embodiment of the present invention, the method includes binning local information according to characteristics of the heart cycle. Preferably, the characteristics comprise a heart rate. Additionally or alternatively, the characteristics comprise a morphology of an ECG of the heart.

In a preferred embodiment of the present invention, the positions of the probe are positions relative to a reference location. Preferably, the reference location is a predetermined portion of the heart. Preferably, a position of the reference location is determined using a position sensor. Preferably, the method includes periodically determining a position of the reference location. Preferably, the position of the reference location is acquired at the same phase of consecutive cardiac cycles.

In one preferred embodiment of the present invention, the probe is located in a coronary vein or artery.

In another preferred embodiment of the present invention, the probe is located outside a blood vessel.

In still another preferred embodiment of the present invention, the probe is located in a coronary vein or artery.

There is also provided in accordance with a preferred embodiment of the invention, a method of diagnosis including:

constructing a first map of a heart as described above;

performing a medical procedure on the heart; and

constructing a second map of the heart.

There is provided in accordance with another preferred embodiment of the invention a method of cardiac shaping including:

(a) choosing a portion of a heart having a certain amount of muscle tissue thereat;

(b) determining a pacing regime for changing the workload of the portion; and

(c) pacing the heart using the determined pacing regime. Preferably, the workload of the portion is increased in order to increase the amount of muscle tissue therein. Alternatively, the workload of the portion is decreased in order to decrease the amount of muscle tissue thereat.

Preferably, the workload is changed by changing a plateau duration in the portion. Alternatively or additionally, the workload is changed by changing an activation time in the portion.

There is also provided in accordance with yet another preferred embodiment of the invention a method of cardiac shaping including:

(a) choosing a portion of a heart having a certain amount of muscle tissue thereat;

(b) determining a pacing regime for changing the plateau duration of the portion; and

(c) pacing the heart using the determined pacing regime. Preferably, the plateau duration of the portion is changed in order to increase the amount of muscle tissue therein. Alternatively, the plateau duration of the portion is changed in order to decrease the amount of muscle tissue thereat.

Preferably, the plateau duration is changed by applying a local voltage in the portion. Alternatively or additionally, the plateau duration is changed by changing an activation time in the portion.

Preferably, cardiac shaping includes constructing a map of at least a part of the heart.

Preferably, cardiac shaping includes:

(d) determining after a time the effect of (c); and

(e) repeating (a)-(d) if a desired effect is not reached.

There is further provided in accordance with still another preferred embodiment of the invention a method of implanting a pacemaker electrode including:

(a) pacing a heart from a first location;

(b) determining a cardiac parameter associated with pacing at the location;

(c) repeating (a) and (b) for a second location; and

(d) implanting the electrode at the location in which the cardiac parameter is optimal. Preferably, the cardiac parameter includes stroke volume. Alternatively or additionally, the cardiac parameter includes intra-cardiac pressure. Preferably, the cardiac parameter is determined by measuring using an invasive probe.

There is also provided in accordance with a preferred embodiment of the invention a method of pacing a heart including:

(a) measuring a local physiological value at a plurality of locations in the heart;

(b) determining a pacing regime which changes the temporal or spatial distribution of the physiological value; and

(c) pacing the heart using the determined pacing regime. Preferably, changing the distribution includes maintaining physiological values within a range. Preferably, the range is a locally determined range.

Preferably, (a)-(c) are performed by a pacemaker. Alternatively or additionally, the physiological values are determined substantially simultaneously. Alternatively or additionally, the physiological value includes perfusion. Alternatively or additionally, the physiological value includes stress. Alternatively or additionally, the physiological value is plateau duration.

There is provided in accordance with an additional preferred embodiment of the invention a method of adaptive pacing including:

(a) determining a preferred pacing regime for a heart which is optimal with respect to a physiological variable; and

(b) pacing the heart using the preferred pacing regime. Preferably, determining a preferred pacing regime includes generating a map of the activation profile of the heart. Preferably, determining a preferred pacing regime includes generating a map of the reaction profile of the heart. Preferably, adaptive pacing includes analyzing an activation map or a reaction map of the heart to determine portions of the heart which are under-utilized due to an existing activation profile of the heart.

Preferably, pacing is initiated by implanting at least one pacemaker electrode in the heart. Further preferably, the at least one pacemaker electrode includes a plurality of electrodes.

Preferably, pacing is initiated by changing the electrification of a plurality of previously implanted pacemaker electrodes.

Preferably, the physiological variable is a stroke volume.

There is provided in accordance with yet another preferred embodiment of the invention, a method of pacing including:

(a) pacing a heart using a first pacing scheme; and

(b) changing the pacing scheme to a second pacing scheme, where the change in pacing is not directly related to arrhythmias, fibrillation or heart rate in the heart. Preferably, each of the pacing regimes optimizes the utilization of different portions of the heart. Alternatively or additionally, the changing of the pacing regimes temporally distributes workload between different portions of the heart.

There is also provided in accordance with a preferred embodiment of the invention, a pacemaker including:

a plurality of electrodes;

a source of electricity for electrifying the electrodes; and

a controller which changes the electrification of the electrodes in response to a plurality of measured local values of a heart to achieve an optimization of a cardiac parameter of the heart.

Preferably, the measured values include a local activation time. Alternatively or additionally, the local values include a local plateau duration. Preferably, the local values are measured using the electrodes. Alternatively or additionally, the values are measured using a sensor.

Preferably, the local values include non-electrical local physiological values.

Preferably, the cardiac parameter includes a stroke volume. Alternatively or additionally, the cardiac parameter includes an intra-cardiac pressure. Preferably, the cardiac parameter is measured by the pacemaker.

There is also provided in accordance with a preferred embodiment of the invention, a method of detecting structural anomalies in a heart, including:

(a) bringing an invasive probe into contact with a location on a wall of the heart;

(b) determining a position of the invasive probe;

(c) repeating (a)-(b) for a plurality of locations of the heart;

(d) combining the positions to form a time-dependent map of at least a portion of the heart; and

(e) analyzing the map to determine structural anomalies in the heart. Preferably, the positions are acquired during systole, and analyzing includes determining a bulge in the geometry of the heart. Alternatively or additionally, analyzing the map includes analyzing the map to determine an abnormal size of the heart. Alternatively or additionally, analyzing the map includes analyzing the map to determine an abnormal size of a chamber of the heart.

Preferably, (b) is repeated at least a second time, at the same location and at a different phase of the cardiac cycle than (b).

There is provided in accordance with still another preferred embodiment of the invention a method of adding a conductive pathway in a heart between a first segment of the heart and a second segment of the heart, including:

providing a conductive device having a distal end and a proximal end;

electrically connecting the distal end of the device to the first location; and

electrically connecting the proximal end of the device to the second location.

There is also provided in accordance with still another preferred embodiment of the invention a conductive device for creating conductive pathways in the heart, including:

a first lead adapted for electrical connection to a first portion of the heart;

a second lead adapted for electrical connection to a second portion of the heart;

a capacitor for storing electrical charge generated at the first portion of the heart and for discharging the electrical charge at the second portion of the heart.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1A is a schematic cross-section diagram of a heart;

FIGS. 1B-1E are schematic cross-section diagrams showing the heart in each of four phases of a cardiac cycle;

FIG. 1F is a graph showing the blood volume in a left ventricle of the heart during a cardiac cycle;

FIG. 1G is a graph showing the filling rate of the left ventricle during a cardiac cycle;

FIG. 2 is a partial schematic view of a heart showing the arrangement of cardiac muscle fibers around a left ventricle;

FIG. 3 is a schematic cross-section diagram of a heart showing the electrical conduction system of the heart;

FIG. 4 is a graph showing changes in the voltage potential of a single cardiac muscle cell in reaction to an activation signal;

FIGS. 5A-C are partial schematic cross-sectional perspective views of a heart showing application of Laplace's law to determination of tension in the heart;

FIG. 6 is a schematic cross-sectional side view of a heart showing a preferred apparatus for generating a map of the heart;

FIG. 7 is a flowchart of a preferred method of constructing the map of FIG. 6;

FIG. 8 is a generalized graph showing the dependence of a resistance on the distance of the catheter from heart muscle tissue;

FIGS. 9A-D show various local changes in the geometry of the heart;

FIG. 10 shows a multi-headed catheter for sensing local geometric changes according to a preferred embodiment of the invention;

FIG. 11 is a flowchart showing a preferred binning method;

FIGS. 12A-D show pathological cases where a change in pacing of a heart is desirable; and

FIG. 13 is a schematic side view of an implanted pacemaker according to a preferred embodiment of the invention.

DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

A first preferred embodiment of the invention relates to mapping the geometry of the heart and time related changes in the geometry of the heart. FIG. 6 is a schematic side view of a preferred apparatus for performing the mapping. FIG. 7 is a flowchart showing a preferred method for performing a mapping.

Referring to FIG. 6, a distal tip 74 of a mapping catheter 72 is inserted into heart 20 and brought into contact with heart 20 at a location 75. Preferably, the position of tip 74 is determined using a position sensor 76. Sensor 76 is preferably a position sensor as described in PCT application US95/01103, "Medical diagnosis, treatment and imaging systems", filed Jan. 24, 1995, in U.S. Pat. No. 5,391,199 or in U.S. Pat. No. 5,443,489, all assigned to the same assignee as the instant application and the disclosures of which are incorporated herein by reference, and which typically require an external magnetic field generator 73. Alternatively, other position sensors as known in the art are used, for example, ultrasonic, RF and rotating magnetic field sensors. Alternatively or additionally, tip 74 is marked with a marker whose position can be determined from outside of heart 20, for example, a radio-opaque marker for use with a fluoroscope. Preferably, at least one reference catheter 78 is inserted into heart 20 and placed in a fixed position relative to heart 20. By comparing the positions of catheter 72 and catheter 78 the position of tip 74 relative to the heart can be accurately determined even if heart 20 exhibits overall motion within the chest. Preferably the positions are compared at least once every cardiac cycle, more preferably, during diastole. Alternatively, position sensor 76 determines the position of tip 74 relative to catheter 78, for example, using ultrasound, so no external sensor or generator 73 is required. Alternatively, catheter 78 is outside the heart, such as outside the body or in the esophagus.

It should be appreciated that a geometric map can be constructed even if position sensor 76 only determines position and not orientation. However, since sensor 76 is typically located at a small distance from tip 74, at least two orientation angles are desirable to increase the accuracy of the position determination of tip 74.

Referring to FIG. 7, a typical mapping process includes:

(a) bringing catheter tip 74 into contact with the wall of heart 20, at location 75;

(b) determining at least one position of tip 74;

(c) adding the position value to the map;

(d) moving catheter 72 to a second location, such as a location 77;

(e) repeating steps (b)-(d); and

(f) (optionally) reconstructing the surface of heart 20 from the determined positions.

Reconstructing the surface of heart 20 may comprise reconstructing inner or outer surfaces of heart 20, depending on the location of catheter tip 74. Methods of reconstructing a surface from a plurality of data points are well known in the art.

Preferably, catheter 72 is a steerable tip catheter, so that repositioning of tip 74 is facilitated. Steerable catheters are further described in PCT application US95/01103 and in U.S. Pat. Nos. 5,404,297, 5,368,592, 5,431,168, 5,383,923, 5,368,564, 4,921,482, 5,195,968, the disclosures of which are incorporated herein by reference.

In a preferred embodiment of the invention, each position value has an associated time value, preferably relative to a predetermined point in the cardiac cycle. Preferably, multiple position determinations are performed, at different points in the cardiac cycle, for each placement of tip 74. Thus, a geometric map comprises a plurality of geometric snapshots of heart 20, each snapshot associated with a different instant of the cardiac cycle. The cardiac cycle is preferably determined using a standard ECG device. Alternatively or additionally, a local reference activation time is determined using an electrode on catheter 72. Heart 20 may be paced in a known manner, such as by catheter 78 or may be naturally paced.

In an alternative preferred embodiment of the invention, position values are acquired also while tip 74 is not in contact with heart 20. These position values can be used to help generation of an image of the inner surface of heart 20.

As can be appreciated, contact between tip 74 and heart 20 must be assured. In particular, it is important to know when tip 74 comes into contact with heart 20 after repositioning of tip 74 and the stability of tip 74 at a location, such as whether tip 74 moves from location 75 without operator intervention as a result of motion of heart 20 must be known. One method of monitoring the contact between tip 74 and location 75 is through analysis of the trajectory of tip 74. The inner wall of heart 20 has many crevices and tip 74 typically lodges in one of these crevices, such that tip 74 moving together with location 75. It can be expected that tip 74 will return to the same spatial position each cardiac cycle. Thus, if tip 74 does not return to the same position each diastole, contact between tip 74 and location 75 is not stable. Further, some types of slippage can be detected by determining whether the entire trajectory of tip 74 substantially repeats itself. Furthermore, some types of slippage add artifacts to the trajectory which can be detected by comparing the trajectory against trajectories of nearby segments of the heart or against a model of the motion of the heart.

It is also known that initiation of contact between tip 74 and heart 20 causes artifacts in a locally measured electrogram. Thus, in a preferred embodiment of the invention, tip 74 includes an electrode 79 which measures the local electrical activity. Artifacts in the measured activity indicate that tip 74 is not in stable contact with location 75. Preferably, the local electrical activity and in particular the local activation time and local plateau length are stored in association with each location in heart 20.

In an additional embodiment of the invention, the contact pressure between tip 74 and location 75 is measured, using a pressure sensor, to determine the existence and stability of contact therebetween.

In a preferred embodiment of the invention electrode 79 is used to measure the impedance between tip 74 and a ground outside the patient. The impedance between tip 74 and the ground is affected by the distance of tip 74 from the wall of heart and by the quality of contact therebetween. The effect can be explained in the following manner. Long cells such as muscle cells and nerves exhibit electrical conductivities which are non-isotropic and frequency dependent. Blood, which fills heart 20, exhibits conduction which is relatively frequency independent and isotropic, and its resistance is approximately half the average resistance of muscle tissue. The greatest amount of frequency dependence of body structures is found between 30 and 200 Hz. However, frequencies in the range 30 Hz-10 MHz are useful. For example, at 50 kHz, contact can be most easily determined from changes in the impedance and at 0.5 MHz, accumulation of residue on the catheter from charring of heart muscle during ablation can be determined from changes in the impedance.

FIG. 8 is a generalized graph showing the dependence of a resistance, between tip 74 and an external lead attached to the patient, on the distance of tip 74 from location 75, at 50 KHz.

Local geometric changes in the heart are also clinically interesting. FIG. 9A shows a local movement of a segment 90 of heart 20. Movement of segment 90 relative to the cardiac cycle and/or movement of other segments of heart 20 indicates forces acting at segment 90. These forces may be as a result of local contraction at segment 90 or as a result of contraction of other portions of heart 20. Movement of segment 90 before an activation signal reaches segment 90 may indicate that segment 90 is not activated at an optimal time and, thus, that it does not contribute a maximum amount to the output of heart 20. Movement without an activation signal usually indicates non-muscular tissue, such as scar tissue. The activation time is preferably measured using electrode 79 (FIG. 6).

FIG. 9B shows another way of determining the reaction of muscle tissue to an activation signal. A first location 92 is located a distance D1 from a second location 94 and a distance D2 from a third location 96. In a normal heart D1 and D2 can be expected to contract at substantially the same time by a substantially equal amount. However, if the tissue between location 92 and location 94 is non-reactive, D1 might even grow when D2 contracts (Laplace's law). In addition a time lag between the contraction of D1 and of D2 is probably due to block in the conduction of the activation signal.

FIGS. 9C and 9D show the determination of local changes in the radius of heart 20, which can be together with the pressure to determine the local tension using Laplace's law. In FIG. 9C a plurality of locations 98, 100 and 102 exhibit a local radius R1 and in FIG. 9D, the local radius decreases to R2, which indicates that the muscle fiber at locations 98, 100 and 102 is viable. It should be noted, that since the pressure in heart 20 is spatially equalized, a ratio between the tension at different parts of heart 20 can be determined even if an absolute value cannot be determined.

In a preferred embodiment of the invention, a plurality of catheters are placed at locations 98, 100 and 102, so that changes in the local geometry can be determined in a single cardiac cycle. Alternatively or additionally, a multi-head catheter, each head having a position sensor, is used to map local geometrical changes. FIG. 10 shows a multi-head catheter 104 having a plurality of position sensors 106 for mapping local geometric changes.

Another clinically important local change is a change in the thickness of a wall segment of heart 20. Muscle fibers thicken when they contract, so an increase in the thickness of the wall segment indicates that muscle fibers in the wall segment are contracting. Thinning of the wall segment indicates that the wall segment is stretching. Either there are not enough muscle fibers in the wall segment to overcome the tension on the wall segment or the muscle fibers in the wall segment are not activated in synchrony with the rest of heart 20, resulting in pressure increases which are not counteracted by local tension increases. Late increases in the thickness of the wall segment usually indicate that the activation signal was delayed at the segment. Local changes in thickness can also be compared to a locally determined activation time, to determine a local reaction time. In addition, comparison of differences in thickening between several adjacent wall segments is indicative of the activation time, much like changes in local geometry.

The local thickness of the wall segment is preferably determined using an ultrasonic sensor mounted on catheter 72 or catheter 78. Forward looking ultrasonic sensors (FLUS), suitable for mounting on catheter 72 for determining the local thickness of the wall segment are described in PCT application US95/01103 and in U.S. Pat. No. 5,373,849, the disclosures of which are incorporated therein by reference. A side looking ultrasonic sensor (SLUS), suitable for mounting on catheter 78 is described in PCT publication WO 95/07657, the disclosure of which is incorporated herein by reference. Alternatively or additionally, an external sensor, such as an echocardiograph determines the thickness of the wall segment adjacent tip 94.

In a preferred embodiment of the invention sensors, additional to position sensor 76, are mounted at tip 74. As already described, at least one electrode 79 is preferably mounted at tip 74 to map the local electrical activity which can be integrated with the geometric map to form an electro-mechanical map. For example, contraction duration can be compared to local electrical plateau length or local activation time can be compared to local reaction time using an electro-mechanical map.

Additionally or alternatively, a chemical sensor is mounted at tip 74 to determine changes in the local ionic concentrations or local chemical concentrations. Typically, such a chemical sensor is mounted on a needle which is inserted into the myocardium.

Alternatively or additionally, a perfusion meter is mounted on tip 74 to determine the amount of perfusion. Examples of perfusion meters include: a Doppler ultrasound perfusion meter or a Doppler laser perfusion meter, such as disclosed in "Design for an ultrasound-based instrument for measurement of tissue blood flow", by Burns, S. M. and Reid, M. H., in "Biomaterials, Artificial Cells and Artificial Organs", Volume 17, Issue 1 page 61-68, 1989, the disclosure of which is incorporated herein by reference. Such a perfusion meter preferably indicates the flow volume and/or the flow velocity.

Alternatively or additionally, a scintillation detector is mounted on tip 74 to detect radiation emitted by radio-pharmaceuticals injected into or ingested by the patient. If a suitable low energy radio-pharmaceutical is used, the scintillation detector will be sensitive to radiation from portions of heart 20 substantially in contact with tip 74. For example, local perfusion can be determined.

In another preferred embodiment of the invention, an optical sensor is mounted on tip 74. As is known in the art, oxygenated blood reflects a spectrum which is different from the spectrum reflected by non-oxygenated blood. By determining the reflectance of portions of heart 20, the perfusion thereof can be determined. Additionally or alternatively, optical reflectivity patterns or texture is used to differentiate between different tissue types, for example, fibrous, viable muscle and damaged muscle. Preferably, the optical sensor is a camera or a fiber-optic image guide. Further preferably, an IR (infra-red) sensitive sensor is used. Typically, illumination at tip 74 is provided by a light source mounted on tip 74 or by light transmitted through a fiber-optic light-guide.

Alternatively or additionally, a cold-tip catheter is used to map the effect of ablating a portion of the heart. It is known in the art that hypothermic cardiac muscle does not initiate or react to electrical signals. Cold-tip catheters, such as disclosed in PCT publication WO 95/19738 of 27 Jul. 1995, the disclosure of which is incorporated herein by reference, can be used to inhibit the electrical activity of a local wall segment while simultaneously mapping the local geometrical effects of the inhibition.

Other locally sensed variables include, temperature, which may indicate perfusion or activation, osmolarity, conduction velocity, repolarization time, repolarization duration, and impedance, which may indicate tissue type and viability.

Mapping is typically performed when heart 20 is externally paced, such as using another catheter, either to set a constant heart rate or to generate certain arrhythmias. Electrode 79 is useful in identifying and analyzing arrhythmias. In addition electrode 79 can be used as a pacemaker to determine the effect of pacing from a certain location, such as initiating VT.

Several types of maps are generally acquired. One type maps local physiological values as a function of location on the heart, for example conductance. In this type of map, the position of tip 74 is typically determined at the same phase of the cardiac cycle for each new location and is unrelated to the acquisition of the local value. The local value may be time dependent. For example, a map of the instant local thickness of the heart wall as a function of the phase of the cardiac cycle. Another example, is local electrogram as a function of time. The value may be continuously acquired over the entire cardiac cycle, only over a portion thereof or at a single instant synchronized to the position determination and/or the cardiac cycle. A geometric map includes information about the geometry of the heart, for example shape and volume, and/or changes in the geometry of the heart as a function of time, for example, thickness, local curvature and shape. An electro-mechanical map includes information about the coupling between electrical signals and mechanical changes in the heart, for example, thickening as a function of activation time. Other types of maps include chemical-mechanical maps, which correlate mechanical and chemical action of the heart, energy expenditure maps which show local expenditures of energy, perfusion maps which show local perfusion of cardiac muscle and a map of the ratio between energy expenditure and local perfusion.

As explained above, maps can be used to determine clinical information about the heart. Preferably, maps are constructed and analyzed in preparation for a therapeutic procedure or in assessing the success of a therapeutic procedure. For example, scar tissue neither reacts to nor conducts an electrical signal, while hibernating muscle tissue conducts the activation signal but does not react to it. A map, as described above, can be used to differentiate between these and other types of tissue.

Aneurysms are readily detectable on a geometric map, as bulges during systole. Furthermore, potential aneurysms can be detected soon after an AMI (acute myocardial infraction) from local reactions to an activation signal and local reactions to changes in intra-cardiac pressure.

The maps can be used to improve pumping efficiency of the heart. In an efficiently operating heart, each heart segment has an optimal relation between its activation time and the cardiac cycle. Using one of the above described maps, the relationship between the local activation time and the cardiac cycle can be determined. Using a finite-element model of the heart as a pump, underutilized segments of the heart can be determined. The potential for improvement in the heart output can be determined from the model and different methods of improving heart function, such as described below, can be tested.

A preferred embodiment of the invention provides a solution to mapping when heart 20 has a non-constant rate. In one case, the heart rate varies, however, it is not arrhythmic. In this case, each heart beat may be treated as one time unit, with an appropriate scaling. Where heart beat is arrhythmic, either naturally, or by choice (manual pacing), position and other sensed values are binned according to ECG or electrogram morphology, beat length, activation location, relative activation time or other determined cardiac parameters. Thus, a plurality of maps may be constructed, each of which corresponds to one bin. FIG. 11 is a flowchart of a preferred binning method. Local information is acquired simultaneously with an associated 12 lead body surface ECG. The morphology of the acquired ECG is correlated with a plurality of stored ECG traces. The local information is stored in a bin which has the highest correlation. Preferably, if the correlation is below a predetermined limit, a new bin is created having the acquired ECG as its associated ECG.

It should be appreciated that locally determined characteristics, such as local electrogram, are associated with a particular segment of heart 20, so that local twisting, moving and contractions can be determined. In many prior art systems, a map of the electrical activity of heart 20 is not associated with specific segments of heart 20 but with general features.

A preferred embodiment of the invention utilizes adaptive mechanisms of the human heart to change the heart, in particular the distribution of muscle mass in the heart.

A general property of muscle tissue, including cardiac muscle, is that muscle tissue hypertrophies in reaction to increased stress and atrophies in reaction to reduced stress. According to a preferred embodiment of the invention, the stress and/or workload in the heart are redistributed to affect the distribution of cardiac muscle mass. Preferably, redistribution of stress and/or workload is achieved by changing the location of pacing in the hea