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人B细胞中的Fas表达与细胞凋亡

Fas expression and apoptosis in human B cells.

作者信息

Schattner E, Friedman S M

机构信息

Department of Medicine, New York Hospital, NY 10021, USA.

出版信息

Immunol Res. 1996;15(3):246-57. doi: 10.1007/BF02918252.

Abstract

Mechanisms of B cell apoptosis are critical in reducing aberrant B cell proliferations such as those that arise in autoimmune disease and in B cell malignancies. The physiologic interaction of CD4+ helper T cells and B lymphocytes has been extensively studied over the past two decades. Although CD4+ T cells are considered primarily to offer positive costimulatory signals for B cell differentiation into active immunoglobulin-secreting cells, recent studies have shown that CD4+ T cells are crucial in downregulating the humoral immune response. In the course of cognate interaction between CD40 ligand (CD40L)-bearing CD4+ T cells and CD40-expressing germinal center B cells, CD40 ligation results in augmented Fas expression at the B cell surface. Like CD40L, Fas ligand is expressed on activated CD4+ Th1 cells and when bound to Fas receptor on the B cell surface, initiates an apoptotic signal in that cell. Thus, CD4+ T cells limit the growth of autologous germinal center B cells by first inducing Fas expression and then instigating a death signal via Fas ligand. In this work, we will consider these observations about CD4+ T-cell-induced, Fas-mediated B cell death in the context of other factors that affect apoptosis in B cells, normal and malignant.

摘要

B细胞凋亡机制对于减少异常的B细胞增殖至关重要,比如在自身免疫性疾病和B细胞恶性肿瘤中出现的那些增殖。在过去二十年里,CD4⁺辅助性T细胞与B淋巴细胞之间的生理相互作用得到了广泛研究。尽管CD4⁺T细胞主要被认为能为B细胞分化成活跃的免疫球蛋白分泌细胞提供正向共刺激信号,但最近的研究表明,CD4⁺T细胞在下调体液免疫反应方面至关重要。在携带CD40配体(CD40L)的CD4⁺T细胞与表达CD40的生发中心B细胞的同源相互作用过程中,CD40连接会导致B细胞表面Fas表达增加。与CD40L一样,Fas配体在活化的CD4⁺Th1细胞上表达,当与B细胞表面的Fas受体结合时,会在该细胞中引发凋亡信号。因此,CD4⁺T细胞通过首先诱导Fas表达,然后经由Fas配体引发死亡信号,来限制自体生发中心B细胞的生长。在这项工作中,我们将结合影响正常和恶性B细胞凋亡的其他因素,来考虑这些关于CD4⁺T细胞诱导的、Fas介导的B细胞死亡的观察结果。

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