THE STRUCTURAL BASIS FOR BINDING OF COMPLEMENT BY IMMUNOGLOBULIN M

Author:

Hurst Mary M.1,Volanakis John E.1,Hester Raymond B.1,Stroud Robert M.1,Bennett J. Claude1

Affiliation:

1. From the Division of Clinical Immunology and Rheumatology and the Department of Microbiology, University of Alabama Medical Center, Birmingham, Alabama 35294

Abstract

An insight into the structural features of human IgM that are responsible for its capacity to bind the first component of complement (C) has been obtained by examining the ability of IgM subfragments to bind active C1 (C1). The smallest two fragments found to bind C1 were the major CNBr fragment of the Fc portion of IgM and the CH4 fragment of the carboxy-terminal domain. The smallest fragment which fixes C1 has a disaggregated mol wt of 6,800, consists of 60 residues, and contains no carbohydrate. Structural considerations and sequence overlaps suggest that the amino-terminal side of the CH4 domain (24 amino acid residues) might be responsible for fixing C1.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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3. Complement—immunoglobulin interactions;Current Opinion in Immunology;1995-02

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