SOLUBLE HUMAN-COMPLEMENT RECEPTOR TYPE-1 - INVIVO INHIBITOR OF COMPLEMENT SUPPRESSING POSTISCHEMIC MYOCARDIAL INFLAMMATION AND NECROSIS

被引：892

作者：

WEISMAN, HF

BARTOW, T

LEPPO, MK

MARSH, HC

CARSON, GR

CONCINO, MF

BOYLE, MP

ROUX, KH

WEISFELDT, ML

FEARON, DT

机构：

[1] JOHNS HOPKINS UNIV, SCH MED, DEPT MED, BALTIMORE, MD 21205 USA

[2] T CELL SCI INC, CAMBRIDGE, MA 02139 USA

[3] FLORIDA STATE UNIV, DEPT BIOL SCI, TALLAHASSEE, FL 32306 USA

来源：

SCIENCE | 1990年 / 249卷 / 4965期

关键词：

D O I：

10.1126/science.2371562

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

The complement system is an important mediator of the acute inflammatory response, and an effective inhibitor would suppress tissue damage in many autoimmune and inflammatory diseases. Such an inhibitor might be found among the endogenous regulatory proteins of complement that block the enzymes that activate C3 and C5. Of these proteins, complement receptor type 1 (CR1; CD35) has the most inhibitory potential, but its restriction to a few cell types limits its function in vivo. This limitation was overcome by the recombinant, soluble human CR1, sCR1, which lacks the transmembrane and cytoplasmic domains. The sCR1 bivalently bound dimeric forms of its ligands, C3b and methylamine-treated C4 (C4-ma), and promoted their inactivation by factor I. In nanomolar concentrations, sCR1 blocked complement activation in human serum by the two pathways. The sCR1 had complement inhibitory and anti-inflammatory activities in a rat model of reperfusion injury of ischemic myocardium, reducing myocardial infarction size by 44 percent. These findings identify sCR1 as a potential agent for the suppression of complement-dependent tissue injury in autoimmune and inflammatory diseases.

引用

页码：146 / 151

页数：6

共 65 条

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