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Role of stress responses in human cell survival following exposure to ultraviolet C radiation.

机译:暴露于紫外线C辐射后应激反应在人类细胞存活中的作用。

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摘要

PURPOSE: To investigate in human skin and other cells the role of tyrosine kinase and protein kinase-C (PKC) in eliciting cell-signalling responses to UV radiation (UVR) that affect the survival of irradiated cells. MATERIALS AND METHODS: The survival of HeLa S3 cells, NCTC 2544 human keratinocytes and A431 human epidermal carcinoma cells was measured following incubation with various tyrosine kinase or PKC inhibitors and exposure to UVC (254nm) radiation. In addition, Western blotting measured PKC isozyme expression in human keratinocytes following UVC exposure. RESULTS: It was confirmed that inhibition of tyrosine kinase activation reduces the survival of UV-irradiated HeLa S3 cells. However, no effect was seen on the survival of either NCTC 2544 human keratinocytes or A431 human epidermal carcinoma cells. In contrast, specific inhibition of PKC reduced the survival of UV-irradiated keratinocytes but had no effect on HeLa cells. Comparison of the effects of different inhibitors in keratinocytes suggested that this effect was mediated mostly through PKCmu and PKClambda/iota. In addition, keratinocyte exposure to UVC induced large and temporally distinct increases in PKCmu and PKClambda/iota. CONCLUSIONS: The survival of NCTC 2544 keratinocytes, but not HeLa S3 cells, following UVC exposure is mediated by signalling through PKC, mostly PKCmu and PKClambda/iota. Further study is required to confirm these results in normal human keratinocytes.
机译:目的:研究人皮肤和其他细胞中酪氨酸激酶和蛋白激酶-C(PKC)在引起细胞对紫外线辐射(UVR)的信号传递反应中的作用,这些信号影响照射细胞的存活。材料与方法:在与各种酪氨酸激酶或PKC抑制剂孵育并暴露于UVC(254nm)辐射后,测量了HeLa S3细胞,NCTC 2544人角质形成细胞和A431人表皮癌细胞的存活率。此外,蛋白质印迹法检测了紫外线照射后人角质形成细胞中PKC同工酶的表达。结果:证实酪氨酸激酶激活的抑制降低了紫外线照射的HeLa S3细胞的存活。但是,对NCTC 2544人角质形成细胞或A431人表皮癌细胞的存活均未见影响。相反,对PKC的特异性抑制降低了紫外线辐射的角质形成细胞的存活率,但对HeLa细胞没有影响。比较不同抑制剂对角质形成细胞的作用,表明该作用主要通过PKCmu和PKClambda / iota介导。此外,角质形成细胞暴露于UVC会导致PKCmu和PKClambda / iota出现较大且暂时性的增加。结论:UVC暴露后,NCTC 2544角质形成细胞(而不是HeLa S3细胞)的存活是通过PKC信号介导的,大部分是PKCmu和PKClambda / iota。需要进一步的研究来证实正常人角质形成细胞中的这些结果。

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