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Negative regulatory element associated with potentially functional promoter and enhancer elements in the long terminal repeats of endogenous murine leukemia virus-related proviral sequences.

机译：与内源性鼠白血病病毒相关前病毒序列的长末端重复序列中潜在功能性启动子和增强子相关的负调控元件。

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Three series of recombinant DNA clones were constructed, with the bacterial chloramphenicol acetyltransferase (CAT) gene as a quantitative indicator, to examine the activities of promoter and enhancer sequence elements in the 5' long terminal repeat (LTR) of murine leukemia virus (MuLV)-related proviral sequences isolated from the mouse genome. Transient CAT expression was determined in mouse NIH 3T3, human HT1080, and mink CCL64 cultured cells transfected with the LTR-CAT constructs. The 700-base-pair (bp) LTRs of three polytropic MuLV-related proviral clones and the 750-bp LTRs of four modified polytropic proviral clones, in complete structures either with or without the adjacent downstream sequences, all showed very little or negligible activities for CAT expression, while ecotropic MuLV LTRs were highly active. The MuLV-related LTRs were divided into three portions and examined separately. The 3' portion of the MuLV-related LTRs that contains the CCAAC and TATAA boxes was found to be a functional promoter, being about one-half to one-third as active as the corresponding portion of ecotropic MuLV LTRs. A MboI-Bg/II fragment, representing the distinct 190- to 200-bp inserted segment in the middle, was found to be a potential enhancer, especially when examined in combination with the simian virus 40 promoter in CCL64 cells. A PstI-MboI fragment of the 5' portion, which contains the protein-binding motifs of the enhancer segment as well as the upstream LTR sequences, showed moderate enhancer activities in CCL6 cells but was virtually inactive in NIH 3T3 cells and HT1080 cells; addition of this fragment to the ecotropic LTR-CAT constructs depressed CAT expression. Further analyses using chimeric LTR constructs located the presence of a strong negative regulatory element within the region containing the 5' portion of the enhancer and the immediate upstream sequences in the MuLV-related LTRs.

机译：以细菌氯霉素乙酰转移酶（CAT）基因为定量指标，构建了三个系列的重组DNA克隆，以检测鼠白血病病毒（MuLV）5'长末端重复序列（LTR）中启动子和增强子序列元件的活性。从小鼠基因组中分离的相关的前病毒序列。在用LTR-CAT构建体转染的小鼠NIH 3T3，人HT1080和水貂CCL64培养的细胞中确定了瞬时CAT表达。三个多变的MuLV相关原病毒克隆的700个碱基对（bp）LTR和四个修饰的多变原病毒克隆的750个碱基对的LTR，无论有或没有相邻的下游序列，其完整结构都显示很少或可忽略的活性CAT表达，而亲热的MuLV LTR非常活跃。 MuLV相关的LTR分为三个部分，并分别进行了检查。发现包含CCAAC和TATAA盒的MuLV相关LTR的3'部分是功能启动子，其活性约为正性MuLV LTR的相应部分的一半至三分之一。人们发现一个MboI-Bg / II片段代表了一个中间的190-200 bp插入片段，是一种潜在的增强子，尤其是与CCL64细胞中的猿猴病毒40启动子结合检测时。 5'部分的PstI-MboI片段包含增强子片段的蛋白结合基序以及上游LTR序列，在CCL6细胞中显示中等的增强子活性，但在NIH 3T3细胞和HT1080细胞中几乎没有活性。将该片段添加到亲热LTR-CAT构建体中，降低了CAT的表达。使用嵌合LTR构建体的进一步分析将一个强的负调控元件定位在包含增强子5'部分和MuLV相关LTR的直接上游序列的区域内。

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期刊名称 Journal of Virology
作者
L Y Chang; W K Yang; F E Myer; D M Yang;
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年(卷),期 1989(63),6
年度 1989
页码 2746–2757
总页数 12
原文格式 PDF
正文语种
中图分类人体病毒学（致病病毒）;病毒（滤过性病毒）;
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专利

1. Functional interaction between transcriptional elements in the long terminal repeat of reticuloendotheliosis virus: cooperative DNA binding of promoter- and enhancer-specific factors. [J] . A Hirano, T Wong Molecular and Cellular Biology . 1988,第12期

机译：网状内皮炎病毒长末端重复序列中转录元件之间的功能相互作用：启动子和增强子特异性因子的协同DNA结合。
2. The long terminal repeat negative control region is a critical element for insertional oncogenesis after gene transfer into hematopoietic progenitors with Moloney murine leukemia viral vectors [J] . Ikawa Y., Uchiyama T., Jagadeesh G. J., Gene therapy . 2016,第11期

机译：长末端重复负控制区是利用莫洛尼鼠白血病病毒载体将基因转移到造血祖细胞中后插入肿瘤发生的关键因素
3. Functional RNA polymerase II promoters in solitary retroviral long terminal repeats (LTR-IS elements) [J] . Ingrid Grummt, Ivan Horak, Karl K?hrer Nucleic acids research . 1985,第7期

机译：单个逆转录病毒长末端重复序列中的功能性RNA聚合酶II启动子（LTR-IS元件）
4. Terminal-Repeat Retrotransposon In Miniature (TRIM) elements and their potential utility as DNA markers in Brassica relatives [C] . Tae-Jin Yang, Soo-Jin Kwon, Jung Sun Kim, Proceedings of the 12th International Rapeseed Congress: Sustainable Development in Cruciferous Oilseed Crops Production . 2007

机译：终末微型反转录转座子（TRIM）及其在芸苔属中的潜在DNA标记作用
5. The identification of cis-regulatory elements and their cognate trans-acting molecules in the proximal promoter which enhance the expression of superficial zone protein. [D] . Kim, Hyun-Hee. 2010

机译：鉴定近端启动子中增强浅表层蛋白表达的顺式调控元件及其同源反式作用分子。
6. Note: Exchange of Viral Promoter/Enhancer Elements with Heterologous Regulatory Sequences Generates Targeted Hybrid Long Terminal Repeat Vectors for Gene Therapy of Melanoma [O] . R. M. Diaz, T. Eisen, I. R. Hart, 1998

机译：注意：用异源调控序列交换病毒启动子/增强子元件可产生靶向的杂交长末端重复载体用于黑色素瘤的基因治疗
7. Negative regulatory element associated with potentially functional promoter and enhancer elements in the long terminal repeats of endogenous murine leukemia virus-related proviral sequences [O] . L Y Chang, W K Yang, F E Myer, 1989

机译：与潜在的功能启动子和增强子元素相关的阴性调节元件，在内源小鼠白血病病毒相关的荧光序列中的长末端重复
8. Mouse Endogenous Retroviral Long Terminal Repeat (LTR) Elements and Environmental Carcinogenesis [R] . Yang, W. K. , Ch'ang, L. Y , Myer, F. E. , 1988

机译：小鼠内源性逆转录病毒长末端重复（LTR）元件和环境致癌作用

Negative regulatory element associated with potentially functional promoter and enhancer elements in the long terminal repeats of endogenous murine leukemia virus-related proviral sequences.

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