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激活素对OVCAR3细胞热休克应激的细胞存活作用。

Cell survival effect of activin against heat shock stress on OVCAR3.

作者信息

Fukuda J, Ito I, Tanaka T, Leung P C

机构信息

Department of Obstetrics and Gynecology, Akita University School of Medicine, Japan.

出版信息

Life Sci. 1998;63(25):2209-20. doi: 10.1016/s0024-3205(98)00505-0.

Abstract

Activin has been known as the hormone protein which regulates either cell proliferation or cell differentiation. Recently, it has also been reported that activin may have cell survival function. In this study, we have investigated, 1) the expression of inhibin subunits and activin receptors (ActRs) in ovarian carcinoma cell line (OVCAR3), 2) the binding property between activin and its receptors under the exposure to stress, and 3) the effect of activin on cell proliferation. All of inhibin subunits and ActR Ia, IIa and IIb mRNA were amplified by RT-PCR in OVCAR3. By Western blot analysis, ActR IIa and IIb proteins were detected. The binding property between activin and ActRs was analyzed with the fixed complex, using chemical cross linker. The bigger molecular weight signals, which had been shown to form the heterotrimeric complex among activin, ActR type I and ActR type II were detected after cross linking. These upper signals were apparently increased by rh-Activin and decreased by rh-Follistatin. Therefore, it was suggested that they were resultant from activin and Act-R complex. OVCAR3 was exposed to the stress (42C, 1 hour heat shock), the protein level of ActR IIa increased and ActR IIb decreased from about 3 h to 24 h after the exposure to the heat stress (HS). On the other hand, the complex between activin and ActR IIa and IIb increased from 3 h after the exposure to HS. To investigate the effect of activin and follistatin on OVCAR3 proliferation after the exposure to HS, we counted the cell number at 96 h after the treatment with activin or follistatin in the condition either with or without HS. Proliferation of the cell in the presence of HS was stimulated by rh-Activin and inhibited by rh-Follistatin. These data suggest that activin might have the function to survive and to proliferate OVCAR3, due to, at least in part the increase in its binding capacity to ActRs through either autocrine or paracrine manner.

摘要

激活素是一种调节细胞增殖或细胞分化的激素蛋白。最近,也有报道称激活素可能具有细胞存活功能。在本研究中,我们调查了:1)抑制素亚基和激活素受体(ActRs)在卵巢癌细胞系(OVCAR3)中的表达;2)在应激条件下激活素与其受体之间的结合特性;3)激活素对细胞增殖的影响。通过逆转录聚合酶链反应(RT-PCR)在OVCAR3中扩增出所有抑制素亚基以及ActR Ia、IIa和IIb的信使核糖核酸(mRNA)。通过蛋白质免疫印迹分析检测到了ActR IIa和IIb蛋白。使用化学交联剂通过固定复合物分析激活素与ActRs之间的结合特性。交联后检测到分子量更大的信号,这些信号显示在激活素、I型ActR和II型ActR之间形成了异源三聚体复合物。这些较高的信号明显因重组人激活素(rh-Activin)而增加,因重组人卵泡抑素(rh-Follistatin)而减少。因此,提示它们是激活素与Act-R复合物的产物。将OVCAR3暴露于应激(42℃,1小时热休克),热应激(HS)暴露后约3小时至24小时,ActR IIa的蛋白水平升高,ActR IIb的蛋白水平降低。另一方面,激活素与ActR IIa和IIb之间的复合物在HS暴露后3小时开始增加。为了研究HS暴露后激活素和卵泡抑素对OVCAR3增殖的影响,我们在有或无HS的条件下,在用激活素或卵泡抑素处理96小时后对细胞进行计数。在有HS存在的情况下,细胞增殖受到rh-Activin的刺激,并受到rh-Follistatin的抑制。这些数据表明,激活素可能具有使OVCAR3存活和增殖的功能,这至少部分是由于其通过自分泌或旁分泌方式增加了与ActRs的结合能力。

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