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紫外线对1型人类免疫缺陷病毒长末端重复序列的激活具有血清和毒株特异性。

Activation of HIV type 1 long terminal repeat by ultraviolet light is serum and strain specific.

作者信息

Carrier F, McCary J M, Bae I, Yarosh D B, Fornace A J

机构信息

Laboratory of Molecular Pharmacology, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

AIDS Res Hum Retroviruses. 1994 Jul;10(7):767-73. doi: 10.1089/aid.1994.10.767.

DOI:10.1089/aid.1994.10.767
PMID:7986581
Abstract

We have studied the UV responsiveness of xeroderma pigmentosum (XP) and HeLa cell lines transfected with a CAT reporter gene under the control of the HIV-1 LTR promoter. XP fibroblasts grown in 10% newborn bovine serum (NBS) were three times more responsive to UV radiation than cells grown in 10% fetal calf serum (FCS). Moreover, cocultivation of UV-irradiated XP cells with XP cells containing stable integrants of HIV-LTR CAT was found to be more than four times more effective in inducing the CAT activity when cells were maintained in 10% NBS than in 10% FCS. The level of induction was also dependent on the serum concentration. These data indicate that a serum component, possibly a cytokine(s), can enhance the UV response of both irradiated cells and unirradiated cells cocultivated with irradiated cells. The magnitude of UV responsiveness seemed also to be strain dependent. CAT activity for the HIV LTR promoter from the HTLV-IIIB (HIV-IIIB) strain was induced more than 30-fold by UV irradiation whereas activity from the LAV-1BRU strain was less than 2-fold. In contrast, both constructs were strongly induced by Tat expression. This indicates that there are differences in the induction mechanism for these two stimuli, even though UV radiation has been previously reported to induce a cellular Tat-like factor (Valerie K, et al., Nature [London] 1988;333:78-81).

摘要

我们研究了转染了在HIV-1 LTR启动子控制下的CAT报告基因的着色性干皮病(XP)和HeLa细胞系的紫外线反应性。在10%新生牛血清(NBS)中生长的XP成纤维细胞对紫外线辐射的反应比在10%胎牛血清(FCS)中生长的细胞高三倍。此外,当细胞维持在10% NBS中时,发现将紫外线照射的XP细胞与含有HIV-LTR CAT稳定整合体的XP细胞共培养在诱导CAT活性方面比在10% FCS中有效四倍以上。诱导水平也取决于血清浓度。这些数据表明,一种血清成分,可能是一种细胞因子,可以增强照射细胞以及与照射细胞共培养的未照射细胞的紫外线反应。紫外线反应性的大小似乎也取决于菌株。来自HTLV-IIIB(HIV-IIIB)菌株的HIV LTR启动子的CAT活性在紫外线照射下诱导超过30倍,而来自LAV-1BRU菌株的活性则小于2倍。相比之下,两种构建体都被Tat表达强烈诱导。这表明这两种刺激的诱导机制存在差异,尽管先前有报道称紫外线辐射可诱导一种细胞内Tat样因子(瓦莱丽·K等人,《自然》[伦敦]1988年;333:78-81)。

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