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CNAA / Theses / 2007 / May /

Participation of cathepsin L in collagen degradation during the regression of experimental hepatic cirrhosis


Author: Tudos Radion
Degree:doctor of medicine
Speciality: 14.00.15 - Pathological Anatomy
Year:2007
Scientific adviser: Victor Râvneac
doctor habilitat, professor, Nicolae Testemitanu State University of Medicine and Pharmacy of the Republic of Moldova
Scientific consultant: Nicolae Eşanu
doctor, professor
Institution:
Scientific council:

Status

The thesis was presented on the 24 May, 2007
Approved by NCAA on the 14 June, 2007

Abstract

Adobe PDF document0.37 Mb / in romanian

Thesis

CZU 616.36-004-02-074:615.9+616-091.8

Adobe PDF document 16.00 Mb / in romanian
104 pages

Keywords

cathepsin L, liver, collagen degradation, hepatic cirrhosis regression, cathepsin B, cathepsin H, hydroxyproline, electron hystochemistry

Summary

Some mechanisms of the connective tissue catabolism in liver during hepatic cirrhosis regression were investigated. It was studied the participation of cathepsin L, as well as other lisosomal proteinases, in the process of collagen degradation in liver.

Liver cirrhosis was induced in 140 white rats by a well known method of carbon tetrachloride (CCl4) injections for 13 weeks. Histological, electron-microscopical, electron-histochemical and biochemical investigations of the liver were effectuated at the stage of the maximal development of the liver cirrhosis and during two months of cirrhosis regression (at the 7-th, 14-th, 21-th, 30-th and 60-th day after the last injection of CCl4).

Histological investigations and biochemical determination of the hydroxyproline content in liver have shown that during the regression of experimental hepatic cirrhosis an intensive process of collagen degradation takes place. This process is maximal expressed during the first month after cessation of CCl4-treatment.

It was established that in the period of hepatic cirrhosis regression an important increase of the cysteine proteinases (cathepsins B, H and L) activity in liver took place. The dynamic of the enzymes activity had a phase character and shown a high correlation with tissue hydroxiproline level, that suggest a direct implication of the enzymes in the process of collagen degradation in liver.

Electron-histochimical study has detected the cathepsin L in normal liver in the lisosomes of the hepatocytes, Kupffer cells and endoteliocytes. It was shown, that during the hepatic cirrhosis regression cathepsin L is secreted by the hepatocytes, macrophages (Kupffer cells) and fibroblaste to the extracellular space for participation in the extracellular collagen degradation. The intensive extracellular collagen catabolism in liver during the cirrhosis regression is provided by the hepatocytes, but the intracellular collagen degradation is provided by the macrophage and fibroblasts with the active participation of cathepsin L.