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确定动物中微小RNA特异性切割AGO蛋白的作用。

Defining the contribution of microRNA-specific slicing Argonautes in animals.

作者信息

Pal Anisha, Vasudevan Vaishnav, Houle Francois, Lantin Michael, Maniates Katherine A, Quevillon Huberdeau Miguel, Abbott Allison, Simard Martin J

出版信息

bioRxiv. 2024 Jan 11:2023.01.19.524781. doi: 10.1101/2023.01.19.524781.

DOI:10.1101/2023.01.19.524781
PMID:36711744
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9882343/
Abstract

microRNAs regulate gene expression through interaction with an Argonaute protein family member. While some members of this protein family retain an enzymatic activity capable of cleaving RNA molecules complementary to Argonaute-bound small RNAs, the role of the slicing activity in the canonical microRNA pathway is still unclear in animals. To address the importance of slicing Argonautes in animals, we created strains, carrying catalytically dead endogenous ALG-1 and ALG-2, the only two slicing Argonautes essential for the miRNA pathway in this animal model. We observe that the loss of ALG-1 and ALG-2 slicing activity affects overall animal fitness and causes phenotypes, reminiscent of miRNA defects, only when grown and maintained at restrictive temperature. Furthermore, the analysis of global miRNA expression shows that the catalytic activity of ALG-1 and ALG-2 differentially regulate the level of specific subsets of miRNAs in young adults. We also demonstrate that altering the slicing activity of those miRNA-specific Argonautes does not result in any defect in the production of canonical miRNAs. Together, these data support that the slicing activity of miRNA-specific Argonautes function to maintain the levels of a set of miRNAs for optimal viability and fitness in animals particularly exposed to specific growing conditions.

摘要

微小RNA通过与AGO蛋白家族成员相互作用来调控基因表达。虽然该蛋白家族的一些成员保留了一种酶活性,能够切割与AGO结合的小RNA互补的RNA分子,但在动物中,切割活性在经典微小RNA通路中的作用仍不清楚。为了探究切割AGO蛋白在动物中的重要性,我们构建了携带催化失活的内源性ALG - 1和ALG - 2的品系,这是该动物模型中微小RNA通路仅有的两个必需的具有切割活性的AGO蛋白。我们观察到,只有在限制温度下生长和维持时,ALG - 1和ALG - 2切割活性的丧失才会影响动物的整体健康状况,并导致类似于微小RNA缺陷的表型。此外,对整体微小RNA表达的分析表明,ALG - 1和ALG - 2的催化活性差异调节年轻成虫中特定微小RNA亚群的水平。我们还证明,改变那些微小RNA特异性AGO蛋白的切割活性不会导致经典微小RNA产生的任何缺陷。总之,这些数据支持微小RNA特异性AGO蛋白的切割活性在维持一组微小RNA水平方面发挥作用,以确保动物在特别是暴露于特定生长条件下时具有最佳的生存能力和健康状况。

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