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T cell receptor cross-reactivity between similar foreign and self peptides influences naive cell population size and autoimmunity.

Immunity.. 2014-12;  42(1):95?C107
Ryan W. Nelson, Daniel Beisang, Noah J. Tubo, Thamotharampillai Dileepan, Darin L. Wiesner, Kirsten Nielsen, Marcel WÜthrich, Bruce S. Klein, Dmitri I. Kotov, Justin A. Spanier, Brian T. Fife, James J. Moon, Marc K. Jenkins. Center for Immunology, University of Minnesota Medical School, Minneapolis, MN 55455, USA.
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Abstract

T cell receptor (TCR) cross-reactivity between major histocompatibility complex II (MHCII)-binding self and foreign peptides could influence the naive CD4+ T cell repertoire and autoimmunity. We found that nonamer peptides that bind to the same MHCII molecule only need to share five amino acids to cross-react on the same TCR. This property was biologically relevant because systemic expression of a self peptide reduced the size of a naive cell population specific for a related foreign peptide by deletion of cells with cross-reactive TCRs. Reciprocally, an incompletely deleted naive T cell population specific for a tissue-restricted self peptide could be triggered by related microbial peptides to cause autoimmuni... More

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