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一个含有与癌调蛋白mRNA前导序列高度相似的长末端重复序列的大鼠基因组克隆的分离与分析。

Isolation and analysis of a rat genomic clone containing a long terminal repeat with high similarity to the oncomodulin mRNA leader sequence.

作者信息

Furter C S, Heizmann C W, Berchtold M W

机构信息

Institute of Pharmacology and Biochemistry, University of Zurich-Irchel, Switzerland.

出版信息

J Biol Chem. 1989 Nov 5;264(31):18276-9.

PMID:2681194
Abstract

The structure of a novel long terminal repeat (LTR) from an intracisternal A particle (IAP) DNA element in the rat (Sprague-Dawley) genome was determined. This LTR has a total length of 313 base pairs (bp). Several structural features typical for retroviral LTR promoters were identified, including a "CCAAT" box, a "TATA" box, a polyadenylation signal, and a polyadenylation site. The LTR is flanked by 3-bp inverted repeats, and it consists of the three typical LTR regions, U3, R, and U5. U3 contains 213 bp, R 46 bp, and U5 54 bp, which is within the usual size range of IAP LTRs. A sequence of 60 bp in the U3 region reveals considerable similarity to a murine IAP LTR U3 element, which is known to interact with nuclear proteins. A sequence of 69 bp in the U5 and R regions has 83 and 93% similarities to an endogenous retroviral LTR from Syrian hamster and to the cDNA leader sequence of (Buffalo) rat oncomodulin, respectively. Oncomodulin is an "EF-hand" Ca2+-binding protein and appears in many human and rodent tumors and in cells with tumor-like properties but not in normal tissues. We postulate that in the rat the tumor-specific expression of oncomodulin is controlled by a retroviral LTR promoter.

摘要

确定了大鼠(斯普拉格 - 道利)基因组中来自脑内A颗粒(IAP)DNA元件的新型长末端重复序列(LTR)的结构。该LTR全长313个碱基对(bp)。鉴定出了逆转录病毒LTR启动子典型的几个结构特征,包括一个“CCAAT”框、一个“TATA”框、一个多聚腺苷酸化信号和一个多聚腺苷酸化位点。该LTR两侧是3个碱基对的反向重复序列,它由三个典型的LTR区域U3、R和U5组成。U3包含213 bp,R包含46 bp,U5包含54 bp,这在IAP LTR的通常大小范围内。U3区域中一段60 bp的序列与已知能与核蛋白相互作用的小鼠IAP LTR U3元件有相当大的相似性。U5和R区域中一段69 bp的序列分别与叙利亚仓鼠的内源性逆转录病毒LTR以及(布法罗)大鼠癌调蛋白的cDNA前导序列有83%和93%的相似性。癌调蛋白是一种“EF手型”钙结合蛋白,出现在许多人类和啮齿动物肿瘤以及具有肿瘤样特性的细胞中,但在正常组织中不出现。我们推测在大鼠中,癌调蛋白的肿瘤特异性表达受逆转录病毒LTR启动子控制。

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