Literature DB >> 3139323

Alkaline phosphatase activity of glutaraldehyde-treated bovine pericardium used in bioprosthetic cardiac valves.

A R Maranto1, F J Schoen.   

Abstract

Bioprosthetic valves fail frequently because of pathological mineralization, a process that begins in cell remnants of the glutaraldehyde (GLUT) fixed tissue. Other pathological cardiovascular calcification and physiological mineralization in skeletal/dental tissues are both largely initiated in cell-derived membranous structures (often called "matrix vesicles"), and the enzyme alkaline phosphatase (AP) likely has an important function in the pathogenesis of mineral nucleation. This study tested the hypothesis that AP might also be present in and contribute to calcification of bioprosthetic valves. AP activity of fresh and GLUT-treated bovine pericardium was measured by the conversion of p-nitrophenyl phosphate to p-nitrophenol. Following 24 hours in 0.6% HEPES-buffered GLUT and storage for 2 weeks in 0.2% GLUT, considerable AP hydrolytic activity remained in GLUT-treated tissue relative to that of fresh tissue (Vmax, 24 vs. 45 mumol reaction product/min/mg tissue protein, respectively), although binding was somewhat reduced (Km, 1.9 X 10(3) vs. 1.4 X 10(3) microM substrate, respectively). Enzyme reaction product was demonstrated in both fixed and fresh tissue by light microscopic histochemical studies, confirming the biochemical results. Reaction product was noted along membranes of vascular endothelial cells and interstitial fibroblasts, the sites of early calcific deposits in bioprosthetic valves, by ultrastructural examination of GLUT-treated tissue. We conclude that GLUT-treated bovine pericardium retains much of the hydrolytic activity of AP, an enzyme associated with normal skeletal and pathological cardiovascular and noncardiovascular mineralization, and suggest that further examination of the mechanistic role of this enzyme may stimulate new approaches for slowing or preventing calcification of bioprosthetic tissue.

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Year:  1988        PMID: 3139323     DOI: 10.1161/01.res.63.4.844

Source DB:  PubMed          Journal:  Circ Res        ISSN: 0009-7330            Impact factor:   17.367


  8 in total

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Review 2.  Molecular and cellular aspects of calcific aortic valve disease.

Authors:  Dwight A Towler
Journal:  Circ Res       Date:  2013-07-05       Impact factor: 17.367

3.  Triglycidyl amine crosslinking combined with ethanol inhibits bioprosthetic heart valve calcification.

Authors:  Jeanne M Connolly; Marina A Bakay; Ivan S Alferiev; Robert C Gorman; Joseph H Gorman; Howard S Kruth; Paul E Ashworth; Jaishankar K Kutty; Frederick J Schoen; Richard W Bianco; Robert J Levy
Journal:  Ann Thorac Surg       Date:  2011-09       Impact factor: 4.330

4.  Mechanisms of the in vivo inhibition of calcification of bioprosthetic porcine aortic valve cusps and aortic wall with triglycidylamine/mercapto bisphosphonate.

Authors:  H Scott Rapoport; Jeanne M Connolly; James Fulmer; Ning Dai; Brandon H Murti; Robert C Gorman; Joseph H Gorman; Ivan Alferiev; Robert J Levy
Journal:  Biomaterials       Date:  2006-10-06       Impact factor: 12.479

5.  Role of glutaraldehyde in calcification of porcine aortic valve fibroblasts.

Authors:  K M Kim; G A Herrera; H D Battarbee
Journal:  Am J Pathol       Date:  1999-03       Impact factor: 4.307

6.  The effects of the covalent attachment of 3-(4-hydroxy-3,5-di-tert-butylphenyl) propyl amine to glutaraldehyde pretreated bovine pericardium on structural degeneration, oxidative modification, and calcification of rat subdermal implants.

Authors:  Abigail J Christian; Ivan S Alferiev; Jeanne M Connolly; Harry Ischiropoulos; Robert J Levy
Journal:  J Biomed Mater Res A       Date:  2014-12-28       Impact factor: 4.396

7.  Lipid extraction attenuates the calcific degeneration of bovine pericardium used in cardiac valve bioprostheses.

Authors:  M A Rossi; D M Braile; M D Teixeira; D R Souza; L C Peres
Journal:  J Exp Pathol (Oxford)       Date:  1990-04

8.  Mechanical and biocompatible characterization of a cross-linked collagen-hyaluronic acid wound dressing.

Authors:  James F Kirk; Gregg Ritter; Isaac Finger; Dhyana Sankar; Joseph D Reddy; James D Talton; Chandra Nataraj; Sonoko Narisawa; José Luis Millán; Ronald R Cobb
Journal:  Biomatter       Date:  2013-07-29
  8 in total

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