Literature DB >> 18566367

Systematic comparison of gene expression between murine memory and naive B cells demonstrates that memory B cells have unique signaling capabilities.

Mary M Tomayko1, Shannon M Anderson, Catherine E Brayton, Saheli Sadanand, Natalie C Steinel, Timothy W Behrens, Mark J Shlomchik.   

Abstract

Memory B cells play essential roles in the maintenance of long-term immunity and may be important in the pathogenesis of autoimmune disease, but how these cells are distinguished from their naive precursors is poorly understood. To address this, it would be important to understand how gene expression differs between memory and naive B cells to elucidate memory-specific functions. Using model systems that help overcome the lack of murine memory-specific markers and the low frequency of Ag-specific memory and naive cells, we undertook a global comparison of gene expression between memory B cells and their naive precursors. We identified genes with differential expression and confirmed the differential expression of many of these by quantitative RT-PCR and of some of these at the protein level. Our initial analysis revealed differential expression patterns of genes that regulate signaling. Memory B cells have increased expression of genes important in regulating adenosine signaling and in modulating cAMP responses. Furthermore, memory B cells up-regulate receptors that are essential for embryonic stem cell self-renewal. We further demonstrate that one of these, leukemia inhibitory factor receptor, can initiate functional signaling in memory B cells whereas it does not in naive B cells. Thus, memory and naive B cells are intrinsically wired to signal differently from one another and express a functional signaling pathway that is known to maintain stem cells in other lineages.

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Year:  2008        PMID: 18566367      PMCID: PMC4437802          DOI: 10.4049/jimmunol.181.1.27

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  92 in total

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Authors:  B Schittek; K Rajewsky
Journal:  Nature       Date:  1990-08-23       Impact factor: 49.962

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Authors:  A G Smith; J K Heath; D D Donaldson; G G Wong; J Moreau; M Stahl; D Rogers
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  44 in total

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Review 3.  Immune history and influenza virus susceptibility.

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6.  BLyS inhibition eliminates primary B cells but leaves natural and acquired humoral immunity intact.

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Review 7.  Cancer stem cells in multiple myeloma.

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8.  Naïve and memory B cells exhibit distinct biochemical responses following BCR engagement.

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