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酵母Ty1元件转座顺式作用所需序列在长末端重复序列附近的定位:微型Ty1元件分析

Localization of sequences required in cis for yeast Ty1 element transposition near the long terminal repeats: analysis of mini-Ty1 elements.

作者信息

Xu H, Boeke J D

机构信息

Department of Molecular Biology and Genetics, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205.

出版信息

Mol Cell Biol. 1990 Jun;10(6):2695-702. doi: 10.1128/mcb.10.6.2695-2702.1990.

Abstract

In order to identify and characterize sequences within Ty1 elements which are required in cis for transposition, a series of mini-Ty1 plasmids were constructed and tested for transposition. Mini-Ty1s are deletion mutants of the Ty1-H3 element; Ty1 gene products required for transposition are supplied in trans from a helper Ty1 which has intact open reading frames but lacks a 3' long terminal repeat (LTR) and therefore cannot transpose itself. Up to 5 kilobase pairs of internal sequences of the 6-kilobase-pair-long Ty1 element can be deleted without a significant effect on transposition. The smallest mini-Ty1 element capable of transposition contains the 3' LTR and the transcribed portion of the 5' LTR, 285 base pairs (bp) of internal sequence 3' to the 5' LTR, and 23 bp of internal sequence 5' to the 3' LTR. We conclude that Ty1-encoded proteins can act in trans and that cis-acting sequences in Ty1-H3 are all within or near the LTRs. Further deletion of the 285-bp internal sequence adjacent to the 5' LTR significantly reduced transposition frequency, and the mini-Ty1 RNA produced failed to be packaged into the viruslike particles efficiently. Surprisingly, several nonhomologous cellular mRNAs were also associated with viruslike particles.

摘要

为了鉴定和表征Ty1元件中顺式作用所需的转座序列,构建了一系列微型Ty1质粒并对其转座能力进行了测试。微型Ty1是Ty1-H3元件的缺失突变体;转座所需的Ty1基因产物由辅助Ty1反式提供,该辅助Ty1具有完整的开放阅读框,但缺少3'长末端重复序列(LTR),因此自身不能转座。长达6千碱基对的Ty1元件内部序列中5千碱基对的序列可以被删除,而对转座没有显著影响。能够转座的最小微型Ty1元件包含3'LTR和5'LTR的转录部分、5'LTR 3'端285个碱基对(bp)的内部序列以及3'LTR 5'端23 bp的内部序列。我们得出结论,Ty1编码的蛋白质可以反式作用,并且Ty1-H3中的顺式作用序列都在LTR内或其附近。进一步删除与5'LTR相邻的285-bp内部序列会显著降低转座频率,并且产生的微型Ty1 RNA不能有效地包装到病毒样颗粒中。令人惊讶的是,几种非同源细胞mRNA也与病毒样颗粒相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/351c/360629/3207610d6392/molcellb00042-0269-a.jpg

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