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Chronic lymphocytic leukemic cells exhibit apoptotic signaling via TRAIL-R1.

机译:慢性淋巴细胞性白血病细胞通过TRAIL-R1表现出凋亡信号。

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摘要

Clinical trials have been initiated with Apo2L/TRAIL (Genentech) and agonistic mAbs to TRAIL receptors, -R1 and -R2 (Human Genome Sciences). The apoptosis-inducing ability of these mAbs and different TRAIL preparations, in the presence or absence of histone deacetylase inhibitors (HDACi), varied markedly against primary chronic lymphocytic leukaemia (CLL) cells and various tumor cell lines, demonstrating an unanticipated preferential apoptotic signaling via either TRAIL-R1 or -R2. Contrary to literature reports that TRAIL-induced apoptosis occurs primarily via signaling through TRAIL-R2, CLL cells, in the presence of HDACi, undergo predominantly TRAIL-R1-mediated apoptosis. Consequently, Apo2L/TRAIL, which signals primarily through TRAIL-R2, is virtually devoid of activity against CLL cells. To maximize therapeutic benefit, it is essential to ascertain whether a primary tumor signals via TRAIL-R1/-R2, prior to initiating therapy. Thus combination of an agonistic TRAIL-R1 Ab and an HDACi, such as the anticonvulsant sodium valproate, could be of value in treating CLL.
机译:Apo2L / TRAIL(Genentech)和针对TRAIL受体-R1和-R2的激动性单克隆抗体(Human Genome Sciences)已启动临床试验。在存在或不存在组蛋白脱乙酰基酶抑制剂(HDACi)的情况下,这些mAb和不同TRAIL制剂的凋亡诱导能力对原发性慢性淋巴细胞性白血病(CLL)细胞和各种肿瘤细胞系的变化明显,证明了通过TRAIL-R1或-R2。与文献相反,TRAIL诱导的细胞凋亡主要通过TRAIL-R2的信号传导发生,在HDACi存在的情况下,CLL细胞主要经历TRAIL-R1介导的细胞凋亡。因此,主要通过TRAIL-R2发出信号的Apo2L / TRAIL实际上缺乏针对CLL细胞的活性。为了最大程度地发挥治疗效果,在开始治疗之前,必须先确定是否通过TRAIL-R1 / -R2发出原发性肿瘤信号。因此,激动剂TRAIL-R1 Ab和HDACi(例如抗惊厥药丙戊酸钠)的组合可能在治疗CLL中有价值。

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