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T cell receptor-extracellular constant regions as hetero-cross-linkers for immunoglobulin variable regions.

作者信息

Seimiya H, Naito M, Mashima T, Yasui H, Kuwana Y, Kurosawa Y, Tsuruo T

机构信息

Institute of Applied Microbiology, University of Tokyo.

出版信息

J Biochem. 1993 Jun;113(6):687-91. doi: 10.1093/oxfordjournals.jbchem.a124104.

Abstract

The T cell receptor alpha and beta chains are covalently linked via a disulfide bond in their extracellular constant regions. To use these domains as specific hetero-cross-linkers of two different polypeptides, we created genetic constructs encoding a chimeric antibody Fab fragment in which mouse immunoglobulin constant regions from a phosphorylcholine-specific antibody were substituted for human alpha beta-T cell receptor (TCR) extracellular constant regions (for solubilization, the transmembrane- and cytoplasmic-regions of the receptor were deleted). These constructs, i.e., chimeric heavy (VHC beta C kappa) and light (VLC alpha) chains, were cotransfected into murine SP2/0 myeloma cells for expression. Cells transfected with the genes expressed mRNAs for chimeric heavy and light chains. Without CD3 molecules, the two chimeric chains specifically associated via a disulfide bond to form a chimeric Fab fragment in the cells. These data indicate that the TCR C alpha- and C beta-regions might be used as potent specific hetero-cross-linkers for protein engineering.

摘要

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