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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >BCALM (AC099524.1) Is a Human B Lymphocyte-Specific Long Noncoding RNA That Modulates B Cell Receptor-Mediated Calcium Signaling
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BCALM (AC099524.1) Is a Human B Lymphocyte-Specific Long Noncoding RNA That Modulates B Cell Receptor-Mediated Calcium Signaling

机译:BCALM(AC099524.1)是一种人体B淋巴细胞特异性长的长度非编码RNA,用于调节B细胞受体介导的钙信号传导

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摘要

Of the thousands of long noncoding RNAs (lncRNA) identified in lymphocytes, very few have defined functions. In this study, we report the discovery and functional elucidation of a human B cell-specific lncRNA with high levels of expression in three types of B cell cancer and normal B cells. The AC099524.1 gene is upstream of the gene encoding the B cell-specific phospholipase C gamma 2 (PLCG2), a B cell-specific enzyme that stimulates intracellular Ca2+ signaling in response to BCR activation. AC099524.1 (B cell-associated lncRNA modulator of BCR-mediated Ca+ signaling [BCALM]) transcripts are localized in the cytoplasm and, as expected, CRISPR/Cas9 knockout of AC099524.1 did not affect PLCG2 mRNA or protein expression. lncRNA interactome, RNA immunoprecipitation, and coimmunoprecipitation studies identified BCALM-interacting proteins in B cells, including phospholipase D 1 (PLD1), and kinase adaptor proteins AKAP9 (AKAP450) and AKAP13 (AKAP-Lbc). These two AKAP proteins form signaling complexes containing protein kinases A and C, which phosphorylate and activate PLD1 to produce phosphatidic acid (PA). BCR stimulation of BCALM-deficient B cells resulted in decreased PLD1 phosphorylation and increased intracellular Ca+ flux relative to wild-type cells. These results suggest that BCALM promotes negative feedback that downmodulates BCR-mediated Ca+ signaling by promoting phosphorylation of PLD1 by AKAP-associated kinases, enhancing production of PA. PA activates SHP-1, which negatively regulates BCR signaling. We propose the name BCALM for B-Cell Associated LncRNA Modulator of BCR-mediated Ca+ signaling. Our findings suggest a new, to our knowledge, paradigm for lncRNA-mediated modulation of lymphocyte activation and signaling, with implications for B cell immune response and BCR-dependent cancers.
机译:在淋巴细胞中鉴定的数千个长的NORCODING RNA(LNCRNA),很少有函数。在这项研究中,我们在三种类型的B细胞癌和正常B细胞​​中报告了具有高水平表达的人B细胞特异性LNCRNA的发现和功能阐明。 AC099524.1基因是编码B细胞特异性磷脂酶Cγ2(PLCG2)的基因的上游,B细胞特异性酶响应BCR活化刺激细胞内Ca2 +信号传导。 AC099524.1(B BCR介导的CA +信号传导[BCALM]的BCR相关的LNCRNA调节剂在细胞质中局部化,如预期的那样,AC099524.1的CRISPR / CAS9敲除不影响PLCG2 mRNA或蛋白质表达。 LNCRNA互乱组,RNA免疫沉淀和CoImMunoppipitionIpipition研究鉴定了B细胞中的Bcalm相互作用蛋白,包括磷脂酶D 1(PLD1)和激酶衔接子Akap9(Akap450)和Akap13(Akap-LBC)。这两种AKAP蛋白形成含有蛋白激酶A和C的信号配合物,其磷酸化和活化PLD1产生磷脂酸(PA)。 BCRM缺陷B细胞的BCR刺激导致PLD1磷酸化降低和相对于野生型细胞增加的细胞内Ca +通量。这些结果表明,BCALM通过通过Akap相关激酶促进PLD1的磷酸化,增强PA的产生,促进衰减BCR介导的Ca +信号传导的负反馈。 PA激活SHP-1,对BCR信令负调节。我们向BCR介导的CA +信号传导的B细胞相关LNCrNA调节剂提出了BCALM的名称。我们的研究结果表明了我们的知识,涉及LNCRNA介导的淋巴细胞活化和信号传导调节的范式,具有对B细胞免疫应答和BCR依赖性癌症的影响。

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