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转化的和恶性的人B淋巴细胞质膜上Gc的构型改变。

Altered configuration of Gc on the plasma membrane of transformed and malignant human B lymphocytes.

作者信息

Nel A E, Navailles M, Emerson D L, Goldschmidt-Clermont P, Pathak S K, Tsang K Y, Galbraith R M

出版信息

Clin Immunol Immunopathol. 1985 Nov;37(2):191-202. doi: 10.1016/0090-1229(85)90150-3.

Abstract

Normal human peripheral blood B cells exhibit strong membrane fluorescence for Gc (vitamin D-binding protein), and this protein can form a close spatial relationship with integral membrane immunoglobulin (mIg) with evidence of codistribution in the lipid bilayer. In contrast, fluorescence for both Gc and mIg has been found in this study to be weak or absent in several B lymphoblastoid cell lines and in chronic lymphocytic leukemia B cells. Moreover, the comobility of these components, where detectable, was also impaired. In abnormal B cells, the intensity of membrane fluorescence for Gc was substantially increased after crosslinking of mIg with antibody, and the latter was also associated with increased specific radioiodination of Gc by lactoperioxidase. These results indicate that Gc can apparently become displaced under certain circumstances within or through the lipid bilayer. The altered content or membrane topography of Gc in such abnormal B cells might be associated with impaired expression and mobility of mIg.

摘要

正常人类外周血B细胞对Gc(维生素D结合蛋白)表现出强烈的膜荧光,并且这种蛋白质可以与完整膜免疫球蛋白(mIg)形成紧密的空间关系,有证据表明在脂质双层中共分布。相比之下,在本研究中发现,几种B淋巴母细胞系和慢性淋巴细胞白血病B细胞中Gc和mIg的荧光较弱或缺失。此外,这些成分(在可检测到的情况下)的共迁移性也受损。在异常B细胞中,用抗体交联mIg后,Gc的膜荧光强度显著增加,并且后者还与乳过氧化物酶对Gc的特异性放射性碘化增加有关。这些结果表明,在某些情况下,Gc显然可以在脂质双层内或通过脂质双层发生位移。这种异常B细胞中Gc含量或膜拓扑结构的改变可能与mIg的表达和迁移受损有关。

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