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Induction of transcription from the long terminal repeat of Moloney murine sarcoma provirus by UV-irradiation, x-irradiation, and phorbol ester.

机译：通过紫外线，x射线和佛波醇酯诱导莫洛尼氏鼠肉瘤原病毒长末端重复序列的转录。

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摘要

The long terminal repeat (LTR) of Moloney murine sarcoma virus (Mo-MuSV) was used as a model system to study the stress response of mammalian cells to physical carcinogens. The chloramphenicol acetyltransferase (CAT) gene was inserted between two Mo-MuSV LTRs, and the LTR-CAT-LTR construct was used for virus production and was integrated into the genome of NIH 3T3 cells in the proviral form. This construct was used to assure that the integrated CAT gene was driven by the promoter of the LTR. Expression of the CAT gene was stimulated 4-fold by UV irradiation, and the peak of activity was observed at 18 hr. In contrast, stimulation of the CAT expression after x-irradiation was 2-fold and occurred at 6 hr. Phorbol myristate acetate also stimulated CAT activity 4-fold with a peak at 6 hr. Down-regulation of protein kinase C blocked totally the response to x-irradiation but only partially the response to UV. The protein kinase inhibitor H7 blocked the response to treatment by UV, x-ray, and phorbol ester.

机译：莫洛尼鼠肉瘤病毒（Mo-MuSV）的长末端重复序列（LTR）被用作模型系统来研究哺乳动物细胞对物理致癌物的应激反应。将氯霉素乙酰基转移酶（CAT）基因插入两个Mo-MuSV LTR之间，并将LTR-CAT-LTR构建体用于病毒生产，并以原病毒形式整合到NIH 3T3细胞的基因组中。该构建体用于确保整合的CAT基因由LTR的启动子驱动。 CAT基因的表达被紫外线照射刺激了4倍，并且在18小时观察到活性的峰值。相比之下，X射线照射后CAT表达的刺激是2倍，并在6小时时发生。乙酸肉豆蔻酸乙酸酯还刺激CAT活性4倍，在6小时达到峰值。蛋白激酶C的下调完全阻止了对X射线的响应，但仅部分阻止了对UV的响应。蛋白激酶抑制剂H7阻断了对UV，X射线和佛波酯的治疗反应。

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Lin, C S; Goldthwait, D A; Samols, D;
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年度 1990
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专利

1. Delineation of transcriptional control signals within the Moloney murine sarcoma virus long terminal repeat. [J] . B J Graves, R N Eisenman, S L McKnight Molecular and Cellular Biology . 1985,第8期

机译：描绘了莫洛尼鼠肉瘤病毒长末端重复序列中的转录控制信号。
2. Alternate utilization of two regulatory domains within the Moloney murine sarcoma virus long terminal repeat. [J] . B J Graves, S P Eisenberg, D M Coen, Molecular and Cellular Biology . 1985,第8期

机译：莫洛尼鼠肉瘤病毒长末端重复序列中两个调节域的交替利用。
3. Modulation of Moloney leukemia virus long terminal repeat transcriptional activity by the murine CD4 silencer in retroviral vectors [J] . Indraccolo S., Habeler W., Zamarchi R., Virology . 2000,第1期

机译：逆转录病毒载体中鼠CD4沉默子对莫洛尼氏白血病病毒长末端重复转录活性的调节
4. Passive repression of HIV-1 long terminal repeat enhancer controlled viral transcription in HIV-1 infected cells [C] . S.R.K.Hoffmann, L.Bisset, J.Schupbach, the International Peptide Symposium . 2001

机译：HIV-1长末端重复增强剂受控病毒转录的被动压制在HIV-1感染细胞中
5. Rat mutant cells showing temperature sensitivity for transformation by wild-type Moloney murine sarcoma virus [D] . Inoue, Hirokazu 1984

机译：大鼠突变细胞对野生型莫洛尼鼠肉瘤病毒转化具有温度敏感性
6. Induction of transcription from the long terminal repeat of Moloney murine sarcoma provirus by UV-irradiation x-irradiation and phorbol ester. [O] . C S Lin, D A Goldthwait, D Samols 1990

机译：通过紫外线x射线和佛波醇酯诱导莫洛尼氏鼠肉瘤原病毒长末端重复序列的转录。
7. Sequence-specific DNA binding of the proto-oncoprotein ets-1 defines a transcriptional activator sequence within the long terminal repeat of the Moloney murine sarcoma virus. [O] . C V Gunther, J A Nye, R S Bryner, 1990

机译：甲酰癌蛋白ETS-1的序列特异性DNA结合在Moloney鼠Sarcoma病毒的长末端重复中定义了转录活化剂序列。
8. Evaluation of Moloney Murine Sarcoma and Leukemia Virus Complex as a Model for Airborne Oncogenic Virus Biohazards: Survival of Airborne Virus and Exposure of Mice. [R] . Hinshaw, V. S., Schaffer, F. L., Chatigny, M. A. 1975

机译：评估莫洛尼小鼠肉瘤和白血病病毒复合物作为空气传播致癌病毒生物危害的模型：空气传播病毒的存活和小鼠的暴露。

Induction of transcription from the long terminal repeat of Moloney murine sarcoma provirus by UV-irradiation, x-irradiation, and phorbol ester.

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