Literature DB >> 17332376

Asymmetric T lymphocyte division in the initiation of adaptive immune responses.

John T Chang1, Vikram R Palanivel, Ichiko Kinjyo, Felix Schambach, Andrew M Intlekofer, Arnob Banerjee, Sarah A Longworth, Kristine E Vinup, Paul Mrass, Jane Oliaro, Nigel Killeen, Jordan S Orange, Sarah M Russell, Wolfgang Weninger, Steven L Reiner.   

Abstract

A hallmark of mammalian immunity is the heterogeneity of cell fate that exists among pathogen-experienced lymphocytes. We show that a dividing T lymphocyte initially responding to a microbe exhibits unequal partitioning of proteins that mediate signaling, cell fate specification, and asymmetric cell division. Asymmetric segregation of determinants appears to be coordinated by prolonged interaction between the T cell and its antigen-presenting cell before division. Additionally, the first two daughter T cells displayed phenotypic and functional indicators of being differentially fated toward effector and memory lineages. These results suggest a mechanism by which a single lymphocyte can apportion diverse cell fates necessary for adaptive immunity.

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Year:  2007        PMID: 17332376     DOI: 10.1126/science.1139393

Source DB:  PubMed          Journal:  Science        ISSN: 0036-8075            Impact factor:   47.728


  397 in total

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