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Inhibition of self-binding antibodies (autobodies) by a VH-derived peptide.

作者信息

Kang C Y, Brunck T K, Kieber-Emmons T, Blalock J E, Kohler H

机构信息

IDEC Pharmaceuticals Corporation, La Jolla, CA 92037.

出版信息

Science. 1988 May 20;240(4855):1034-6. doi: 10.1126/science.3368787.

Abstract

The self-binding properties of a dominant idiotypic antibody (T15) and a minor idiotypic antibody (M603), both specific for phosphorylcholine, were examined as models of self-binding antibodies (autobodies). Observed differences in the self-binding affinity of T15 and M603 relate to variable sequence differences in their respective heavy and light chains. A molecular recognition theory based on the translation of coding and noncoding DNA strands was used to identify complementary amino acid sequences responsible for self-binding. The second hypervariable region of the heavy chain domain, extending into the third framework region, was predicted as the primary self-binding locus. Among peptides synthesized with different variable heavy and light chain regions, a 24-residue peptide spanning the second hypervariable and third framework regions of the heavy chain of T15 was nearly as effective as phosphorycholine in inhibiting the self-binding complexes.

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