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携带大型复杂染色体畸变的 D. melanogaster 品系中“缺陷”逆转座元 gtwin 的扩增。

Amplification of "defective" retrotransposon gtwin in D. melanogaster strain carrying large complex chromosomal aberration.

机构信息

Engelhardt Institute of Molecular Biology RAS, 32 Vavilova st., Moscow, 119991, Russia.

出版信息

Mol Genet Genomics. 2010 Nov;284(5):373-81. doi: 10.1007/s00438-010-0573-0. Epub 2010 Sep 22.

Abstract

Transposable elements (TE) are found in all eukaryotic genomes and play a significant role in their structure and functioning. The majority of mobile elements are silent in the genomes indicating the existence of cell control mechanisms of their activity. Establishment of immunity to TE is of great interest, but it cannot be studied directly and there are only few examples of present or recent active transpositions of mobile elements. G32, a Drosophila melanogaster strain, is characterized by the presence of large complex chromosomal aberration in the 3rd chromosome, active transpositions of gtwin in the past, and its stability at present. To address the question as to what had happened to the element while the cell took it under the control, we performed the detailed cytological and molecular analyses of gtwin's structure and its distribution in G32. Two variants of gtwin were found, one of which is amplified in G32 despite the alteration of tRNA-primer binding site. This element is accumulated in the aberrant chromosome and associated with the inversions breakpoints. Gtwin copies are predominantly localized in euchromatic regions and at least three of them are situated in heterochromatin. One copy was found in the piRNA cluster that might have caused silencing of the element.

摘要

转座元件 (TE) 存在于所有真核生物基因组中,在其结构和功能中起着重要作用。大多数移动元件在基因组中是沉默的,这表明存在细胞控制其活性的机制。建立对 TE 的免疫是非常重要的,但不能直接研究,而且目前只有少数移动元件的现有或最近的活性转座的例子。Drosophila melanogaster 品系 G32 的特点是 3 号染色体上存在大的复杂染色体畸变,过去 gtwin 的活跃转座,以及目前的稳定性。为了解决当细胞对元件进行控制时元件发生了什么的问题,我们对 gtwin 的结构及其在 G32 中的分布进行了详细的细胞学和分子分析。发现了两种 gtwin 变体,其中一种在 G32 中扩增,尽管 tRNA-引物结合位点发生了改变。这个元件在异常染色体中积累,并与倒位断点相关。gtwin 拷贝主要定位于常染色质区域,至少有三个位于异染色质区域。一个拷贝位于 piRNA 簇中,可能导致了元件的沉默。

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