Different T cell receptor signals determine CD8+ memory versus effector development.

Journal: Science (New York, N.Y.)
Published:
Abstract

Following infection, naïve CD8+ T cells bearing pathogen-specific T cell receptors (TCRs) differentiate into a mixed population of short-lived effector and long-lived memory T cells to mediate an adaptive immune response. How the TCR regulates memory T cell development has remained elusive. Using a mutant TCR transgenic model, we found that point mutations in the TCR beta transmembrane domain (betaTMD) impair the development and function of CD8+ memory T cells without affecting primary effector T cell responses. Mutant T cells are deficient in polarizing the TCR and in organizing the nuclear factor kappaB signal at the immunological synapse. Thus, effector and memory states of CD8+ T cells are separable fates, determined by differential TCR signaling.

Authors
Emma Teixeiro, Mark Daniels, Sara Hamilton, Adam Schrum, Rafael Bragado, Stephen Jameson, Ed Palmer
Relevant Conditions

Listeriosis

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