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B淋巴细胞对IgM受体连接的敏感性与成熟阶段无关,且由巨噬细胞衍生的干扰素-β局部决定。

B lymphocyte sensitivity to IgM receptor ligation is independent of maturation stage and locally determined by macrophage-derived IFN-beta.

作者信息

Demengeot J, Vasconcellos R, Modigliani Y, Grandien A, Coutinho A

机构信息

Unité d'immunobiologie, CNRS URA 1961, Institut Pasteur, Paris, France.

出版信息

Int Immunol. 1997 Nov;9(11):1677-85. doi: 10.1093/intimm/9.11.1677.

Abstract

Compartmentation of B lymphocyte populations is associated with differences in both development stage and sensitivity to Ig (sIg)-dependent triggering. In order to characterize the factors that contribute in setting the level of sensitivity of a B cell, we quantified sIgM-dependent regulation of Ig secretion in purified mature and immature B cells after ex vivo and in vivo modification of their environment. These analyses formally demonstrate that the bone marrow (BM) microenvironment locally induces high B cell sensitivity to sIgM ligation irrespective of differentiation stage. We further provide evidence that BM macrophages create a dominant environment that enhances B cell sensitivity to B cell receptor triggering. Finally, using ex vivo assays as well as type I IFN receptor-deficient mice we show that IFN-beta produced by resident BM macrophages is necessary and sufficient to define B cell sensitivity. Implications of these findings for the understanding of B cell selection processes are discussed.

摘要

B淋巴细胞群体的分隔与发育阶段及对免疫球蛋白(sIg)依赖性触发的敏感性差异相关。为了确定影响B细胞敏感性水平的因素,我们在体外和体内改变其环境后,对纯化的成熟和未成熟B细胞中sIgM依赖性免疫球蛋白分泌调节进行了定量分析。这些分析正式证明,无论分化阶段如何,骨髓(BM)微环境均可局部诱导B细胞对sIgM连接的高敏感性。我们进一步提供证据表明,BM巨噬细胞营造了一个占主导地位的环境,增强了B细胞对B细胞受体触发的敏感性。最后,通过体外试验以及I型干扰素受体缺陷小鼠,我们表明驻留的BM巨噬细胞产生的干扰素-β对于确定B细胞敏感性是必要且充分的。本文讨论了这些发现对理解B细胞选择过程的意义。

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