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环状 RNA Ythdc2 通过两种翻译策略生成多肽,以促进病毒逃逸。

CircYthdc2 generates polypeptides through two translation strategies to facilitate virus escape.

机构信息

Laboratory of Fish Molecular Immunology, College of Fisheries and Life Science, Shanghai Ocean University, Shanghai, China.

Laboratory for Marine Biology and Biotechnology, Qingdao Marine Science and Technology Center, Qingdao, China.

出版信息

Cell Mol Life Sci. 2024 Feb 15;81(1):91. doi: 10.1007/s00018-024-05148-9.

Abstract

It is known that about 10 circular RNAs (circRNAs) can encode functional polypeptides in higher mammals. However, it is not clear whether the functional polypeptides that can be translated by circRNAs are only the products of the evolution of higher animals, or also widely exist in other lower organisms. In addition, it is also unclear whether the two ways of translating polypeptides using IRES and mA in the one circRNA are exclusive or coexistent. Here, we discovered a novel circRNA derived from the 3'-5' RNA helicase Ythdc2 (Ythdc2) gene in lower vertebrate fish, namely circYthdc2, which can translate into a 170 amino acid polypeptide (Ythdc2-170aa) through IRES sequence or mA modification, and is involved in antiviral immune of fish. Moreover, SCRV infection can promote circYthdc2 translate Ythdc2-170aa. Then, we found that both Ythdc2-170aa and Ythdc2 can promote the degradation of STING by promoting the ubiquitination modification of K11 and K48 link of STING, and weaken the host's antiviral innate immunity. Notably, when circYthdc2 is abundant, Ythdc2 preferentially degrades circYthdc2 and no longer promotes the degradation of STING. Further studies have shown that circYthdc2 is highly conserved from lower vertebrates to higher mammals, and human circYthdc2 can also encode the same polypeptide and play a similar function to that of fish circYthdc2. This discovery confirms for the first time that the ability of circRNA to encode functional proteins is evolutionarily conserved, and finds that the ways of polypeptide translation by the same circRNA were diverse, which is of great significance for further elucidating the function and evolution of circRNAs in vertebrates.

摘要

已知在高等哺乳动物中,大约有 10 个环状 RNA(circRNA)可以编码功能性多肽。然而,目前尚不清楚能够被 circRNA 翻译的功能性多肽是否仅为高等动物进化的产物,或者在其他较低等生物中也广泛存在。此外,circRNA 中使用 IRES 和 mA 两种方式翻译多肽是否相互排斥或同时存在也不清楚。在这里,我们在低等脊椎动物鱼类中发现了一种新型的环状 RNA,它来源于 3' - 5' RNA 解旋酶 Ythdc2(Ythdc2)基因,即 circYthdc2,它可以通过 IRES 序列或 mA 修饰翻译成 170 个氨基酸的多肽(Ythdc2-170aa),并参与鱼类的抗病毒免疫。此外,SCRV 感染可以促进 circYthdc2 翻译 Ythdc2-170aa。然后,我们发现 Ythdc2-170aa 和 Ythdc2 都可以通过促进 STING 的 K11 和 K48 连接的泛素化修饰来促进 STING 的降解,从而削弱宿主的抗病毒先天免疫。值得注意的是,当 circYthdc2 丰富时,Ythdc2 优先降解 circYthdc2,不再促进 STING 的降解。进一步的研究表明,circYthdc2 从低等脊椎动物到高等哺乳动物都高度保守,并且人源性 circYthdc2 也可以编码相同的多肽并发挥与鱼类 circYthdc2 相似的功能。这一发现首次证实了 circRNA 编码功能性蛋白质的能力在进化上是保守的,并发现同一 circRNA 翻译多肽的方式是多样化的,这对进一步阐明 circRNA 在脊椎动物中的功能和进化具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a3da/11073332/a96651ec413d/18_2024_5148_Fig1_HTML.jpg

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