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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >gp96, an endoplasmic reticulum master chaperone for integrins and Toll-like receptors, selectively regulates early T and B lymphopoiesis.
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gp96, an endoplasmic reticulum master chaperone for integrins and Toll-like receptors, selectively regulates early T and B lymphopoiesis.

机译:gp96是内质网整合蛋白和Toll样受体的内在伴侣伴侣,可选择性调节早期的T和B淋巴细胞生成。

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Integrins contribute to lymphopoiesis, whereas Toll-like receptors (TLRs) facilitate the myeloid replenishment during inflammation. The combined role of TLRs and integrin on hematopoiesis remains unclear. gp96 (grp94, HSP90b1) is an endoplasmic reticulum master chaperone for multiple TLRs. We report herein that gp96 is also essential for expression of 14 hematopoietic system-specific integrins. Genetic deletion of gp96 thus enables us to determine the collective roles of gp96, integrins, and TLRs in hematopoiesis. We found that gp96-null hematopoietic stem cells could support long-term myelopoiesis. B- and T-cell development, however, was severely compromised with transitional block from pro-B to pre-B cells and the inability of thymocytes to develop beyond the CD4(-)CD8(-) stage. These defects were cell-intrinsic and could be recapitulated on bone marrow stromal cell culture. Furthermore, defective lymphopoiesis correlated strongly with failure of hematopoietic progenitors to form close contact with stromal cell niche and was not the result of the defect in the assembly of antigen receptor or interleukin-7 signaling. These findings define gp96 as the only known molecular chaperone to specifically regulate T- and B-cell development.
机译:整联蛋白有助于淋巴细胞生成,而Toll样受体(TLR)促进炎症过程中的髓细胞补充。 TLR和整联蛋白在造血功能上的联合作用尚不清楚。 gp96(grp94,HSP90b1)是用于多个TLR的内质网主伴侣。我们在此报告gp96对14种造血系统特异性整合素的表达也是必不可少的。因此,gp96的遗传缺失使我们能够确定gp96,整联蛋白和TLR在造血中的集体作用。我们发现gp96无效的造血干细胞可以支持长期的骨髓生成。但是,从前B细胞到前B细胞的过渡阻滞以及胸腺细胞无法发展到CD4(-)CD8(-)阶段,严重损害了B细胞和T细胞的发育。这些缺陷是细胞固有的,可以在骨髓基质细胞培养中概括。此外,有缺陷的淋巴细胞生成与造血祖细胞不能与基质细胞生态位形成紧密接触密切相关,而不是抗原受体或白介素7信号传导缺陷的结果。这些发现将gp96定义为唯一特异性调节T细胞和B细胞发育的分子伴侣。

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