2009
DOI: 10.1038/emboj.2009.20
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Signalling of the BCR is regulated by a lipid rafts-localised transcription factor, Bright

Abstract: Regulation of BCR signalling strength is crucial for B-cell development and function. Bright is a B-cell-restricted factor that complexes with Bruton's tyrosine kinase (Btk) and its substrate, transcription initiation factor-I (TFII-I), to activate immunoglobulin heavy chain gene transcription in the nucleus. Here we show that a palmitoylated pool of Bright is diverted to lipid rafts of resting B cells where it associates with signalosome components. After BCR ligation, Bright transiently interacts with sumoyl… Show more

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Cited by 44 publications
(105 citation statements)
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References 121 publications
(209 reference statements)
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“…B-1b cells have been proposed to be the primary source of T cell-independent antibody production and long-term protection against S. pneumoniae (33,34). Consistent with this proposition and with our previous data obtained from PC-KLH-immunized DN Bright transgenic mice (39,48), Bright knockout mice exhibited reduced IgM responses to primary immunization with intact S. pneumoniae serotype RSA32 cell wall-associated PC (Fig. 6C, left panel).…”
Section: B-1 Cell Generation and Function Is Impaired In Brightsupporting
confidence: 89%
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“…B-1b cells have been proposed to be the primary source of T cell-independent antibody production and long-term protection against S. pneumoniae (33,34). Consistent with this proposition and with our previous data obtained from PC-KLH-immunized DN Bright transgenic mice (39,48), Bright knockout mice exhibited reduced IgM responses to primary immunization with intact S. pneumoniae serotype RSA32 cell wall-associated PC (Fig. 6C, left panel).…”
Section: B-1 Cell Generation and Function Is Impaired In Brightsupporting
confidence: 89%
“…Strong blocks to conventional (B-2) pro-and pre-B development were observed in Bright Ϫ/Ϫ bone marrow. Peripheral Bright Ϫ/Ϫ B cell subsets (e.g., transitional and marginal zone B cells [MZB]), in which Bright is most highly expressed in normal cells (39,48), were also significantly reduced (Fig. 5B).…”
Section: Resultsmentioning
confidence: 99%
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“…Upon Ag engagement, the ITAMs become phosphorylated by the Src family kinase Lyn and provide a binding site for the SH2 domaincontaining kinase Syk, which triggers the signaling cascades (6,7). Previous biochemical studies provided evidence that one of the earliest events that accompanies the phosphorylation of the BCR by Lyn is the association of the BCR with detergent-insoluble, sphingolipid-and cholesterol-rich membrane microdomains that were defined as lipid rafts (8,9). Subsequently, the BCR rapidly delivers Ag to intracellular compartments where it is proteolytically cleaved, which results in clonal expansion and differentiation of Ag-specific B cells into plasma cells or memory B cells (5).…”
mentioning
confidence: 99%