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A humanized anti-human Fas antibody, R-125224, induces apoptosis in type I activated lymphocytes but not in type II cells

机译:人源化抗人类Fas抗体R-125224诱导I型活化淋巴细胞凋亡,但不诱导II型细胞凋亡

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Fas-mediated apoptosis plays an important role in the immune system, including the elimination of autoreactive lymphoid cells. The Fas-mediated signaling pathway is classified into two types, type I and type II, in human lymphoid cell lines. We investigated whether a humanized anti-human Fas mAb, R-125224, has cell selectivity in induction of apoptosis. R-125224 induced apoptosis in H9 cells, SKW6.4 cells and activated human lymphocytes when cross-linked with anti-human IgG. On the other hand, R-125224 did not induce apoptosis in HPB-ALL cells, Jurkat cells or human hepatocytes. By analysis of death-inducing signaling complex formation, it was demonstrated that R-125224 induced apoptosis selectively in type I cells but not in type II cells. Type I cells also expressed more Fas and had more Fas-clustering activity than type II cells. Moreover, co-localization of these clusters and GM1, which is an sphingoglycolipid associated with lipid rafts, was detected. It was also shown that R-125224 treatment could reduce the number of activated human CD3+Fas+ cells in a SCID mouse model in vivo. Thus, we demonstrated that R-125224 induces apoptosis specifically in type I cells in vitro and in vivo.
机译:Fas介导的凋亡在免疫系统中起重要作用,包括消除自身反应性淋巴样细胞。 Fas介导的信号通路在人淋巴样细胞系中分为I型和II型两种。我们调查了人源化的抗人Fas mAb R-125224是否具有诱导细胞凋亡的细胞选择性。当与抗人IgG交联时,R-125224诱导H9细胞,SKW6.4细胞和活化的人淋巴细胞凋亡。另一方面,R-125224不会在HPB-ALL细胞,Jurkat细胞或人肝细胞中诱导凋亡。通过死亡诱导信号复合物形成的分析,证明R-125224在I型细胞中选择性诱导凋亡,而在II型细胞中则不诱导凋亡。 I型细胞也比II型细胞表达更多的Fas并且具有更多的Fas聚簇活性。此外,检测到这些簇和GM1的共定位,GM1是与脂质筏相关的鞘脂糖脂。还显示了R-125224处理可在SCID小鼠模型中减少活化的人CD3 + Fas + 细胞的数量。因此,我们证明了R-125224在体外和体内特异性诱导I型细胞凋亡。

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