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Hepatocyte growth factor regulated tyrosine kinase substrate in the peripheral development and function of B-cells

机译:肝细胞生长因子调节酪氨酸激酶底物在B细胞的外周发育和功能中的作用

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摘要

Hepatocyte growth factor (HGF)-regulated tyrosine kinase substrate (Hrs) is a vesicular sorting protein that functions as one of the endosomal-sorting proteins required for transport (ESCRT). Hrs, which binds to ubiquitinated proteins through its ubiquitin-interacting motif (UIM), contributes to the lysosomal transport and degradation of ubiquitinated membrane proteins. However, little is known about the relationship between B-cell functions and ESCRT proteins in vivo. Here we examined the immunological roles of Hrs in B-cell development and functions using B-cell-specific Hrs-deficient (Hrs flox/flox;mb1cre/+:Hrs-cKO) mice, which were generated using a cre-LoxP recombination system. Hrs deficiency in B-cells significantly reduced T-cell-dependent antibody production in vivo and impaired the proliferation of B-cells treated in vitro with an anti-IgM monoclonal antibody but not with LPS. Although early development of B-cells in the bone marrow was normal in Hrs-cKO mice, there was a significant decrease in the number of the peripheral transitional B-cells and marginal zone B-cells in the spleen of Hrs-cKO mice. These results indicate that Hrs plays important roles during peripheral development and physiological functions of B lymphocytes.
机译:肝细胞生长因子(HGF)调节的酪氨酸激酶底物(Hrs)是一种囊泡分选蛋白,其功能是转运所需的内体分选蛋白(ESCRT)之一。 Hrs通过其泛素相互作用基序(UIM)与泛素化蛋白结合,有助于溶酶体转运和泛素化膜蛋白降解。但是,关于体内B细胞功能与ESCRT蛋白之间的关系知之甚少。在这里,我们检查了Hrs在B细胞发育和使用B细胞特异性Hrs缺陷型(Hrs flox / flox; mb1cre / +:Hrs-cKO)小鼠的免疫功能中的作用,这些小鼠是通过cre-LoxP重组系统生成的。 B细胞中的Hrs缺乏症会显着降低体内T细胞依赖性抗体的产生,并损害体外用抗IgM单克隆抗体而非LPS处理的B细胞的增殖。尽管Hrs-cKO小鼠骨髓中B细胞的早期发育正常,但Hrs-cKO小鼠脾脏中外周过渡B细胞和边缘区B细胞的数量明显减少。这些结果表明,Hrs在B淋巴细胞的外周发育和生理功能中起重要作用。

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