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转座酶 N 端无规卷曲区的功能特征分析。

Functional Characterization of the N-Terminal Disordered Region of the Transposase.

机构信息

Institute of Enzymology, Research Centre for Natural Sciences, Eötvös Loránd Research Network, 1117 Budapest, Hungary.

Doctoral School of Biology, Institute of Biology, ELTE Eötvös Loránd University, 1117 Budapest, Hungary.

出版信息

Int J Mol Sci. 2022 Sep 7;23(18):10317. doi: 10.3390/ijms231810317.

Abstract

The DNA transposon is an active element initially isolated from the cabbage looper moth, but members of this superfamily are also present in most eukaryotic evolutionary lineages. The functionally important regions of the transposase are well described. There is an RNase H-like fold containing the DDD motif responsible for the catalytic DNA cleavage and joining reactions and a C-terminal cysteine-rich domain important for interaction with the transposon DNA. However, the protein also contains a ~100 amino acid long N-terminal disordered region (NTDR) whose function is currently unknown. Here we show that deletion of the NTDR significantly impairs transposition, although the extent of decrease is strongly cell-type specific. Moreover, replacing the NTDR with scrambled but similarly disordered sequences did not rescue transposase activity, indicating the importance of sequence conservation. Cell-based transposon excision and integration assays reveal that the excision step is more severely affected by NTDR deletion. Finally, bioinformatic analyses indicated that the NTDR is specific for the superfamily and is also present in domesticated, transposase-derived proteins incapable of catalyzing transposition. Our results indicate an essential role of the NTDR in the "fine-tuning" of transposition and its significance in the functions of originated co-opted genes.

摘要

DNA 转座子是一种最初从甘蓝夜蛾中分离出来的活性元件,但这个超家族的成员也存在于大多数真核进化谱系中。转座酶的功能重要区域已有详细描述。它具有一个 RNase H 样折叠结构,包含负责催化 DNA 切割和连接反应的 DDD 基序,以及一个 C 末端富含半胱氨酸的结构域,对于与转座子 DNA 的相互作用很重要。然而,该蛋白还包含一个约 100 个氨基酸长的无规则结构域(NTDR),其功能目前尚不清楚。在这里,我们发现 NTDR 的缺失会显著影响转座,尽管其降低程度在很大程度上取决于细胞类型。此外,用乱序但同样无规则的序列替换 NTDR 并不能挽救转座酶的活性,这表明序列保守性的重要性。基于细胞的转座子切除和整合实验表明,切除步骤受 NTDR 缺失的影响更为严重。最后,生物信息学分析表明,NTDR 是该超家族所特有的,也存在于驯化的、不能催化转座的转座酶衍生蛋白中。我们的结果表明,NTDR 在转座的“微调”中起着至关重要的作用,并且在起源的被共适应基因的功能中具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/af6c/9499001/f6f49f10886c/ijms-23-10317-g001.jpg

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