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Structural Basis For Activation Of The Complement System By Component C4 Cleavage.

Proc Natl Acad Sci U S A.. 2012-09;  109(38):15425 - 15430
Kidmose RT, Laursen NS, Dobó J, Kjaer TR, Sirotkina S, Yatime L, Sottrup-Jensen L, Thiel S, Gál P, Andersen GR. Department of Molecular Biology and Genetics, Aarhus University, Aarhus, Denmark.
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摘要

An essential aspect of innate immunity is recognition of molecular patterns on the surface of pathogens or altered self through the lectin and classical pathways, two of the three well-established activation pathways of the complement system. This recognition causes activation of the MASP-2 or the C1s serine proteases followed by cleavage of the protein C4. Here we present the crystal structures of the 203-kDa human C4 and the 245-kDa C4?MASP-2 substrate?enzyme complex. When C4 binds to MASP-2, substantial conformational changes in C4 are induced, and its scissile bond region becomes ordered and inserted into the protease catalytic site in a manner canonical to serine proteases. In MASP-2, an exosite located wi... More

关键词

crystallography; pattern recognition; proteolysis; structural biology