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Exp Nephrol. 1998 Nov-Dec;6(6):491-5.

Molecular interactions between albumin and proximal tubular cells.

Author information

1
Departments of Nephrology, and Cell Physiology and Pharmacology, Leicester University Medical School, Leicester, UK. njb18@le.ac.uk

Abstract

In glomerular diseases the filtration of excess proteins into the proximal tubule, together with their subsequent reabsorption may represent an important pathological mechanism underlying progressive renal scarring. The most prominent protein in glomerular filtrate, albumin, is reabsorbed by receptor-mediated endocytosis by proximal tubular cells. It binds both to scavenger-type receptors and to megalin in the proximal tubule. Some of these receptors appear to be shared with other cell types, particularly endothelial cells. The endocytic uptake of albumin is subjected to complex hormonal and enzymatic regulation. In addition to being reabsorbed in the proximal tubule, albumin may act as a signalling molecule in these cells, and may induce the expression of numerous pro-inflammatory genes. Modulation of the interaction of albumin with proximal tubular cells may eventually prove to be of therapeutic importance in the treatment of renal diseases.

PMID:
9807019
[Indexed for MEDLINE]

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