The effects of acutely increased ventricular cavity pressure on intrinsic myocardial connective tissue
SM Factor,
M Flomenbaum,
MJ Zhao,
C Eng,
and
TF Robinson
Department of Pathology, Albert Einstein College of Medicine, Bronx, New York 10461.
Studies of normal hearts have revealed a variety of intrinsic connective tissue structures that surround and interconnect myocytes and ventricular mural layers. Among these structures, springlike coiled perimysial fibers, arrayed parallel to myocytes in the interstitial space, have been described in papillary muscle and ventricle. To evaluate the role of the coiled perimysial fibers under perturbed conditions, rat ventricles were filled with barium-gelatin under different pressures and fixed, and then the myocardium was impregnated with silver to visualize the connective tissue. Ventricles were filled at 30, 70 and 100 to 120 mm Hg. The coiled perimysial fibers were studied for their orientation, stretch, integrity and relation to sarcomere length. The coils were noted to embed within the fibrous anulus and to knot into an umbilical-like mass at the apex, thus anchoring them at both ends of the ventricle. They underwent focal straightening even at 30 mm Hg, with generalized straightening and disruption at the highest pressure; changes were most pronounced in the midventricle. Sarcomeres were maintained below 2.2 micron at 30 and 70 mm Hg of cavity pressure in regions of coiled perimysial fiber stretch; only with fiber disruption at 100 to 120 mm Hg were sarcomeres significantly lengthened. Other findings included connective tissue disruption between ventricular wall layers that allowed slippage of myocytes and mural thinning. These observations suggest that coiled perimysial fibers may act as a buffer to protect myocytes from damage under the effects of high cavity pressure.
This article has been cited by other articles:
|
|
|
|
 
Y. Amano, M. Takayama, Y. Fukushima, M. Kitamura, and S. Kumita
Delayed-enhancement MRI of apical hypertrophic cardiomyopathy: assessment of the intramural distribution and comparison with clinical symptoms, ventricular arrhythmias, and cine MRI
Acta Radiol,
July 1, 2011;
52(6):
613 - 618.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
A. Borbely, J. van der Velden, Z. Papp, J. G.F. Bronzwaer, I. Edes, G. J.M. Stienen, and W. J. Paulus
Cardiomyocyte Stiffness in Diastolic Heart Failure
Circulation,
February 15, 2005;
111(6):
774 - 781.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
D. A. Kass, J. G.F. Bronzwaer, and W. J. Paulus
What Mechanisms Underlie Diastolic Dysfunction in Heart Failure?
Circ. Res.,
June 25, 2004;
94(12):
1533 - 1542.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
K. T. Weber
Cardioreparation in Hypertensive Heart Disease
Hypertension,
September 1, 2001;
38(3):
588 - 591.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
K. T. Weber
Targeting Pathological Remodeling : Concepts of Cardioprotection and Reparation
Circulation,
September 19, 2000;
102(12):
1342 - 1345.
[Full Text]
[PDF]
|
|
|
|
|
|
|
L. Lu, Z. Gunja-Smith, J. F. Woessner, P. C. Ursell, T. Nissen, R. E. Galardy, Y. Xu, P. Zhu, and G. G. Schwartz
Matrix metalloproteinases and collagen ultrastructure in moderate myocardial ischemia and reperfusion in vivo
Am J Physiol Heart Circ Physiol,
August 1, 2000;
279(2):
H601 - H609.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
C. Greyson, Y. Xu, L. Lu, and G. G. Schwartz
Right ventricular pressure and dilation during pressure overload determine dysfunction after pressure overload
Am J Physiol Heart Circ Physiol,
May 1, 2000;
278(5):
H1414 - H1420.
[Abstract]
[Full Text]
[PDF]
|
|
|
|
|
|
|
J. Kajstura, X. Zhang, Y. Liu, E. Szoke, W. Cheng, G. Olivetti, T. H. Hintze, and P. Anversa
The Cellular Basis of Pacing-Induced Dilated Cardiomyopathy : Myocyte Cell Loss and Myocyte Cellular Reactive Hypertrophy
Circulation,
October 15, 1995;
92(8):
2306 - 2317.
[Abstract]
[Full Text]
|
|
|
|
