Literature DB >> 25894659

Transcriptional profiling of mouse B cell terminal differentiation defines a signature for antibody-secreting plasma cells.

Wei Shi1, Yang Liao2, Simon N Willis2, Nadine Taubenheim2, Michael Inouye3, David M Tarlinton2, Gordon K Smyth4, Philip D Hodgkin2, Stephen L Nutt2, Lynn M Corcoran2.   

Abstract

When B cells encounter an antigen, they alter their physiological state and anatomical localization and initiate a differentiation process that ultimately produces antibody-secreting cells (ASCs). We have defined the transcriptomes of many mature B cell populations and stages of plasma cell differentiation in mice. We provide a molecular signature of ASCs that highlights the stark transcriptional divide between B cells and plasma cells and enables the demarcation of ASCs on the basis of location and maturity. Changes in gene expression correlated with cell-division history and the acquisition of permissive histone modifications, and they included many regulators that had not been previously implicated in B cell differentiation. These findings both highlight and expand the core program that guides B cell terminal differentiation and the production of antibodies.

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Year:  2015        PMID: 25894659     DOI: 10.1038/ni.3154

Source DB:  PubMed          Journal:  Nat Immunol        ISSN: 1529-2908            Impact factor:   25.606


  50 in total

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Journal:  JCI Insight       Date:  2017-04-06

Review 4.  Here, There, and Anywhere? Arguments for and against the Physical Plasma Cell Survival Niche.

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Review 5.  Innate B Cells: the Archetype of Protective Immune Cells.

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6.  A Regulatory Circuit Controlling the Dynamics of NFκB cRel Transitions B Cells from Proliferation to Plasma Cell Differentiation.

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7.  Single-cell RNA sequencing reveals the heterogeneity of liver-resident immune cells in human.

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10.  Early CCR6 expression on B cells modulates germinal centre kinetics and efficient antibody responses.

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