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人类组蛋白H2A.Z基因。序列与调控。

The human histone H2A.Z gene. Sequence and regulation.

作者信息

Hatch C L, Bonner W M

机构信息

Division of Cancer Treatment, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

J Biol Chem. 1990 Sep 5;265(25):15211-8.

PMID:1697587
Abstract

The gene encoding the human basal histone variant H2A.Z has been cloned and sequenced. There is a single functional H2A.Z gene with several pseudogene copies. No other histone genes were found in the 3 kilobases of upstream sequence or in the 0.7 kilobase of downstream sequence. In the upstream region, there are regions of Alu sequences, located about 1375 and 2650 base pairs before the transcription start site. The amount of the H2A.Z transcript is unlinked to DNA replication; however, the amount of the H2A.Z transcript is greatly decreased as proliferating cell cultures become quiescent due in part to a decrease in the rate of transcription. Promoter sequences upstream from the H2A.Z gene have been delineated in IMR-90 cells by chloramphenicol acetyltransferase gene expression. Maximal promoter activity was found in a chloramphenicol acetyltransferase construct that contained 234 base pairs just upstream from the transcription start site. This region includes two GC boxes and three CCAAT boxes as well as a properly positioned TATA box. The organization of the human gene is similar to that of the recently characterized chicken gene (Dalton, S., Robins, A. J., Harvey, R. P., and Wells, J. R. E. (1989) Nucleic Acids Res. 17, 1745-1756). Both have four introns with identical exon-intron borders, but three of the introns in the chicken gene are much longer than those in the human. The promoter regions of the two genes have little overall homology; however, two GC boxes and one of the CCAAT boxes are conserved.

摘要

编码人类基础组蛋白变体H2A.Z的基因已被克隆和测序。存在一个具有多个假基因拷贝的单一功能性H2A.Z基因。在上游序列的3千碱基或下游序列的0.7千碱基中未发现其他组蛋白基因。在上游区域,存在Alu序列区域,位于转录起始位点之前约1375和2650个碱基对处。H2A.Z转录本的量与DNA复制无关;然而,随着增殖细胞培养物进入静止状态,H2A.Z转录本的量会大幅减少,部分原因是转录速率降低。通过氯霉素乙酰转移酶基因表达,已在IMR-90细胞中描绘了H2A.Z基因上游的启动子序列。在一个氯霉素乙酰转移酶构建体中发现了最大启动子活性,该构建体包含转录起始位点上游仅234个碱基对。该区域包括两个GC框和三个CCAAT框以及一个位置合适的TATA框。人类基因的组织与最近表征的鸡基因相似(道尔顿,S.,罗宾斯,A.J.,哈维,R.P.,和韦尔斯,J.R.E.(1989年)《核酸研究》17,1745 - 1756)。两者都有四个内含子,外显子 - 内含子边界相同,但鸡基因中的三个内含子比人类的长得多。两个基因的启动子区域总体同源性较低;然而,两个GC框和一个CCAAT框是保守的。

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