Abstract

Renal tubular cell injury is a critical component of the syndrome of acute renal failure secondary to ischemia and nephrotoxins. The past several years have been seen progress in understanding the cellular pathophysiology of such injury but major fundamental issues remain to be resolved and a variety of maneuvers with potential for ameliorating such injury need to have their effiacy and action clarified. This has been extremely difficult with in vivo studies because of the complex interplay of factors occurring in the intact kidney which are not subject to direct measurement or experimental manipulation. Studies with isolated subcellular organelles have been valuable but are necessarily done outside of the integrated cellular milieu in which they actually function. The P.I. has refined a preparation of isolated renal tubules in suspension enriched in proximal segments which is suitable for critical direct study, under well controlled in vitro conditions, of major processes in the cellular pathophysiology of renal tubular cell injury including energy and adenine nucleotide metabolism, cellular monovalent cation and Ca++ homeostasis, and alterations in cell lipid and phospholipid metabolism. Preliminary studies on the course of changes in these parameters in a model of ischemic injury established with the preparation will be extended and models for study of nephrotoxic injury will be developed. Preliminary studies have evaluated the potential for a number of agents including phospholipase inhibitors, Ca++ channel blockers, fatty acid free albumin, impermeant solutes and exogenous adenine nucleotide addition to alter the course of ischemic injury on this model with the finding of significant beneficial effects for several of these maneuvers. These studies will be extended to better clarify which agents are effective and optimal conditions for their use and to gain insights into their mechanisms of their action. Additional proposed studies will utilize a model refined by the P.I. of Ca++ mediated injury to the inner mitochondrial membrane to better probe the nature of the process at this important intracellular site. The studies in this proposal will, thus, provide new insight into both mechanisms of renal tubular cell injury and efficacy and mechanisms of action of maneuvers for ameliorating such injury and the associated acute renal failure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Modified Research Career Development Award (K04)
Project #
5K04DK001337-05
Application #
3072364
Study Section
Pathology A Study Section (PTHA)
Project Start
1984-07-01
Project End
1989-06-30
Budget Start
1988-07-01
Budget End
1989-06-30
Support Year
5
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Type
Schools of Medicine
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Weinberg, J M (1992) Glutathione and glycine in acute renal failure. Ren Fail 14:311-9
Weinberg, J M; Buchanan, D N; Davis, J A et al. (1991) Metabolic aspects of protection by glycine against hypoxic injury to isolated proximal tubules. J Am Soc Nephrol 1:949-58
Weinberg, J M; Davis, J A; Abarzua, M et al. (1990) Ouabain-induced lethal proximal tubule cell injury is prevented by glycine. Am J Physiol 258:F346-55
Weinberg, J M; Davis, J A; Abarzua, M et al. (1990) Protection by glycine of proximal tubules from injury due to inhibitors of mitochondrial ATP production. Am J Physiol 258:C1127-40
Weinberg, J M; Johnson, K J; de la Iglesia, F A et al. (1989) Acute alterations of tissue Ca++ and lethal tubular cell injury during HgCl2 nephrotoxicity in the rat. Toxicol Pathol 17:483-93
Weinberg, J M; Davis, J A; Abarzua, M et al. (1989) Relationship between cell adenosine triphosphate and glutathione content and protection by glycine against hypoxic proximal tubule cell injury. J Lab Clin Med 113:612-22
Weinberg, J M; Davis, J A; Shayman, J A et al. (1989) Alterations of cytosolic calcium in LLC-PK1 cells induced by vasopressin and exogenous purines. Am J Physiol 256:C967-76
Weinberg, J M (1988) Adenine nucleotide metabolism by isolated kidney tubules during oxygen deprivation. Biochem Med Metab Biol 39:319-29
Weinberg, J M; Davis, J A; Lawton, A et al. (1988) Modulation of cell nucleotide levels of isolated kidney tubules. Am J Physiol 254:F311-22
Weinberg, J M; Davis, J A; Trivedi, B (1988) Calcium compartmentation in isolated renal tubules in suspension. Biochem Med Metab Biol 39:234-45

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