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DREAM 转基因小鼠中 B 细胞增殖增加和 Ig 产生减少。

Increased B cell proliferation and reduced Ig production in DREAM transgenic mice.

机构信息

Centro Nacional de Biotecnología, Consejo Superior de Investigaciones Científicas, Madrid, Spain.

出版信息

J Immunol. 2010 Dec 15;185(12):7527-36. doi: 10.4049/jimmunol.1000152. Epub 2010 Nov 8.

Abstract

DREAM/KChIP-3 is a calcium-dependent transcriptional repressor highly expressed in immune cells. Transgenic mice expressing a dominant active DREAM mutant show reduced serum Ig levels. In vitro assays show that reduced Ig secretion is an intrinsic defect of transgenic B cells that occurs without impairment in plasma cell differentiation, class switch recombination, or Ig transcription. Surprisingly, transgenic B cells show an accelerated entry in cell division. Transcriptomic analysis of transgenic B cells revealed that hyperproliferative B cell response could be correlated with a reduced expression of Klf9, a cell-cycle regulator. Pulse-chase experiments demonstrated that the defect in Ig production is associated with reduced translation rather than with increased protein degradation. Importantly, transgenic B cells showed reduced expression of the Eif4g3 gene, which encodes a protein related to protein translation. Our results disclose, to our knowledge, a novel function of DREAM in proliferation and Ig synthesis in B lymphocytes.

摘要

DREAM/KChIP-3 是一种在免疫细胞中高度表达的钙依赖性转录阻遏物。表达显性激活 DREAM 突变体的转基因小鼠表现出血清 Ig 水平降低。体外实验表明,Ig 分泌减少是转基因 B 细胞的内在缺陷,这种缺陷发生在浆细胞分化、类别转换重组或 Ig 转录不受损害的情况下。令人惊讶的是,转基因 B 细胞表现出细胞分裂的加速进入。对转基因 B 细胞的转录组分析表明,过度增殖的 B 细胞反应可能与细胞周期调节剂 Klf9 的表达降低有关。脉冲追踪实验表明,Ig 产生的缺陷与翻译减少而不是蛋白质降解增加有关。重要的是,转基因 B 细胞表现出编码与蛋白质翻译有关的蛋白质的 Eif4g3 基因表达降低。我们的研究结果揭示了 DREAM 在 B 淋巴细胞增殖和 Ig 合成中的一个新的功能,据我们所知。

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