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PAP8/pTAC6 是核蛋白复合物的一部分,具有病毒来源的 RNA 识别结构域。

PAP8/pTAC6 Is Part of a Nuclear Protein Complex and Displays RNA Recognition Motifs of Viral Origin.

机构信息

CNRS, CEA, INRA, IRIG-LPCV, University Grenoble-Alpes, F-38000 Grenoble, France.

CNRS, CEA, IBS, University Grenoble Alpes, F-38000 Grenoble, France.

出版信息

Int J Mol Sci. 2022 Mar 11;23(6):3059. doi: 10.3390/ijms23063059.

Abstract

Chloroplast biogenesis depends on a complex transcriptional program involving coordinated expression of plastid and nuclear genes. In particular, photosynthesis-associated plastid genes are expressed by the plastid-encoded polymerase (PEP) that undergoes a structural rearrangement during chloroplast formation. The prokaryotic-type core enzyme is rebuilt into a larger complex by the addition of nuclear-encoded PEP-associated proteins (PAP1 to PAP12). Among the PAPs, some have been detected in the nucleus (PAP5 and PAP8), where they could serve a nuclear function required for efficient chloroplast biogenesis. Here, we detected PAP8 in a large nuclear subcomplex that may include other subunits of the plastid-encoded RNA polymerase. We have made use of PAP8 recombinant proteins in to decouple its nucleus- and chloroplast-associated functions and found hypomorphic mutants pointing at essential amino acids. While the origin of the PAP8 gene remained elusive, we have found in its sequence a micro-homologous domain located within a large structural homology with a rhinoviral RNA-dependent RNA polymerase, highlighting potential RNA recognition motifs in PAP8. PAP8 in vitro RNA binding activity suggests that this domain is functional. Hence, we propose that the acquisition of PAPs may have occurred during evolution by different routes, including lateral gene transfer.

摘要

叶绿体生物发生依赖于一个复杂的转录程序,涉及质体和核基因的协调表达。特别是,与光合作用相关的质体基因是由质体编码的聚合酶(PEP)表达的,PEP 在叶绿体形成过程中经历结构重排。原核型核心酶通过添加核编码的 PEP 相关蛋白(PAP1 到 PAP12)重建为更大的复合物。在 PAP 中,一些已经在核中检测到(PAP5 和 PAP8),它们可能在核中发挥对有效的叶绿体生物发生所必需的功能。在这里,我们在一个可能包括质体编码 RNA 聚合酶其他亚基的大型核亚复合物中检测到 PAP8。我们利用 PAP8 重组蛋白在体外分离其核和叶绿体相关功能,并发现功能减弱的突变体指向必需氨基酸。虽然 PAP8 基因的起源仍然难以捉摸,但我们在其序列中发现了一个微同源结构域,该结构域位于与鼻病毒 RNA 依赖性 RNA 聚合酶的大结构同源性内,突出了 PAP8 中的潜在 RNA 识别基序。PAP8 的体外 RNA 结合活性表明该结构域具有功能。因此,我们提出 PAP 的获得可能是通过不同的途径发生的,包括横向基因转移。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3ed0/8954402/a4f7dbbddace/ijms-23-03059-g001.jpg

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