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来自自发自身免疫性活的肌无力小鼠的新型B细胞成熟因子。

Novel B-cell maturation factor from spontaneously autoimmune viable motheaten mice.

作者信息

Sidman C L, Marshall J D, Masiello N C, Roths J B, Shultz L D

出版信息

Proc Natl Acad Sci U S A. 1984 Nov;81(22):7199-202. doi: 10.1073/pnas.81.22.7199.

Abstract

Both in vivo and in vitro, mice homozygous for the viable motheaten mutation show severe immunodeficiency, polyclonal B-cell activation and Ig secretion, and spontaneous production of a lymphokine [B-cell maturation factor (BMF)] that directly drives the maturation of normal or tumor B cells to the state of active Ig secretion. BMF from motheaten mice is distinct from previously identified forms in its cells of origin (B cells) and biochemical characteristics (apparent Mr 15,000 by gel filtration and NaDodSO4/PAGE; pI 4.3 by chromatofocusing). Among the known murine single-gene models of autoimmunity, only motheaten mice show high levels of spontaneous BMF production, which therefore may be an important component in the development of this form of autoimmunity/immunodeficiency disease. The coincidence of spontaneous BMF production and uncontrolled Ig secretion within the same mutant mouse constitutes the strongest evidence to date for a significant physiological (in vivo) role for BMFs.

摘要

在体内和体外实验中,纯合子的活力性噬血细胞突变小鼠均表现出严重的免疫缺陷、多克隆B细胞活化和Ig分泌,以及自发产生一种淋巴因子[B细胞成熟因子(BMF)],该因子可直接驱动正常或肿瘤B细胞成熟至活跃的Ig分泌状态。来自噬血细胞小鼠的BMF在其起源细胞(B细胞)和生化特性方面(凝胶过滤和NaDodSO4/PAGE显示表观分子量为15,000;色谱聚焦法测定pI为4.3)与先前鉴定的形式不同。在已知的自身免疫性小鼠单基因模型中,只有噬血细胞小鼠表现出高水平的自发BMF产生,因此这可能是这种自身免疫性/免疫缺陷疾病发展的一个重要组成部分。在同一突变小鼠中自发产生BMF与不受控制的Ig分泌同时出现,这是迄今为止BMF在重要生理(体内)作用方面最有力的证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c99e/392105/5db726092080/pnas00623-0300-a.jpg

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