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离理解 IDR-LCR-结构的关系又近了一步。

One Step Closer to the Understanding of the Relationship IDR-LCR-Structure.

机构信息

Institute of Organismic and Molecular Evolution, Faculty of Biology, Johannes Gutenberg University of Mainz, 55128 Mainz, Germany.

Faculty of Physics, Johannes Gutenberg University of Mainz, 55128 Mainz, Germany.

出版信息

Genes (Basel). 2023 Aug 28;14(9):1711. doi: 10.3390/genes14091711.

Abstract

Intrinsically disordered regions (IDRs) in protein sequences are emerging as functionally important elements for interaction and regulation. While being generally flexible, we previously showed, by observation of experimentally obtained structures, that they contain regions of reduced sequence complexity that have an increased propensity to form structure. Here we expand the universe of cases taking advantage of structural predictions by AlphaFold. Our studies focus on low complexity regions (LCRs) found within IDRs, where these LCRs have only one or two residue types (polyX and polyXY, respectively). In addition to confirming previous observations that polyE and polyEK have a tendency towards helical structure, we find a similar tendency for other LCRs such as polyQ and polyER, most of them including charged residues. We analyzed the position of polyXY containing IDRs within proteins, which allowed us to show that polyAG and polyAK accumulate at the N-terminal, with the latter showing increased helical propensity at that location. Functional enrichment analysis of polyXY with helical propensity indicated functions requiring interaction with RNA and DNA. Our work adds evidence of the function of LCRs in interaction-dependent structuring of disordered regions, encouraging the development of tools for the prediction of their dynamic structural properties.

摘要

蛋白质序列中的无规则区域(IDRs)正在成为相互作用和调节的功能重要元素。虽然通常具有灵活性,但我们之前通过观察实验获得的结构表明,它们包含序列复杂性降低的区域,这些区域具有形成结构的增加倾向。在这里,我们利用 AlphaFold 的结构预测扩展了案例范围。我们的研究集中在 IDRs 内发现的低复杂度区域(LCRs)上,这些 LCR 只有一种或两种残基类型(分别为 polyX 和 polyXY)。除了证实以前的观察结果,即 polyE 和 polyEK 具有螺旋结构的趋势外,我们还发现其他 LCR 也有类似的趋势,例如 polyQ 和 polyER,其中大多数包含带电残基。我们分析了蛋白质中含有 polyXY 的 IDRs 的位置,这使我们能够表明 polyAG 和 polyAK 在 N 端聚集,后者在该位置显示出增加的螺旋倾向。具有螺旋倾向的 polyXY 的功能富集分析表明,需要与 RNA 和 DNA 相互作用的功能。我们的工作为 LCR 在依赖相互作用的无序区域结构形成中的功能提供了证据,鼓励开发用于预测其动态结构特性的工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dc4a/10531472/0184dcbd7a5c/genes-14-01711-g001.jpg

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