Author:
Reinheckel T.,Deussing J.,Roth W.,Peters C.
Abstract
Abstract
The lysosomal cysteine peptidases cathepsin B and
cathepsin L are abundant and ubiquitously expressed
members of the papain family, and both enzymes
contribute to the terminal degradation of proteins in
the lysosome. However, there is accumulating evidence
for specific functions of lysosomal proteases
in health and disease. The generation of knock out
mouse strains that are deficient in lysosomal proteases
provides a valuable tool for evaluation of existing
hypotheses and gaining new insights into the in vivo
functions of these proteases. In this minireview, we
summarise and discuss the findings obtained by
analysis of mice that are devoid of cathepsin B or
cathepsin L. In brief, cathepsin L appears to be critically
involved in epidermal homeostasis, regulation of
the hair cycle, and MHC class IImediated antigen
presentation in cortical epithelial cells of the thymus.
Cathepsin B plays a major role in pathological
trypsinogen activation in the early course of experimental
pancreatitis and contributes significantly to
TNFα induced hepatocyte apoptosis.
Subject
Clinical Biochemistry,Molecular Biology,Biochemistry
Cited by
155 articles.
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