Functions of Notch Signaling in the Immune System: Consensus and Controversies

Functions of Notch Signaling in the Immune System: Consensus and Controversies

Functions of Notch Signaling in the Immune System: Consensus and Controversies

Functions of Notch Signaling in the Immune System: Consensus and Controversies

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Overview

Mammalian genomes encode up to four Notch receptors (Notch1–4) and five Notch ligands of the DSL (Delta/Serrate/Lag-2) family, and Notch signaling controls a wide spectrum of developmental processes. Intrathymic Notch1 signaling is essential for several distinct aspects of early T cell development. Notch signaling has also been implicated as a key regulator of peripheral T cell activation and effector cell differentiation, but its functions in these processes remain poorly understood. Notch signaling is dispensable for B cell development in the bone marrow, but it is required to generate the innate-like marginal zone B cell subset in the spleen and may also regulate plasma cell functions. Modification of Notch receptors by fringe glycosyltransferases influences many Notch-dependent aspects of hematopoiesis by altering Notch responsiveness to Delta-like versus Jagged DSL ligands. Here we review recent advances in general aspects of Notch signaling, as well as studies probing Notch functions in these immunological processes.

Product Details

BN ID: 2940013316744
Publisher: Annual Reviews
Publication date: 10/21/2011
Series: Annual Review of Immunology , #28
Sold by: Barnes & Noble
Format: eBook
Pages: 22
File size: 6 MB
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