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Y盒蛋白的复合杂合性因翻译抑制丧失而导致不育。

Compound Heterozygosity for Y Box Proteins Causes Sterility Due to Loss of Translational Repression.

作者信息

Snyder Elizabeth, Soundararajan Ramani, Sharma Manju, Dearth Andrea, Smith Benjamin, Braun Robert E

机构信息

The Jackson Laboratory, Bar Harbor, Maine, United States of America.

出版信息

PLoS Genet. 2015 Dec 8;11(12):e1005690. doi: 10.1371/journal.pgen.1005690. eCollection 2015 Dec.

Abstract

The Y-box proteins YBX2 and YBX3 bind RNA and DNA and are required for metazoan development and fertility. However, possible functional redundancy between YBX2 and YBX3 has prevented elucidation of their molecular function as RNA masking proteins and identification of their target RNAs. To investigate possible functional redundancy between YBX2 and YBX3, we attempted to construct Ybx2-/-;Ybx3-/- double mutants using a previously reported Ybx2-/- model and a newly generated global Ybx3-/- model. Loss of YBX3 resulted in reduced male fertility and defects in spermatid differentiation. However, homozygous double mutants could not be generated as haploinsufficiency of both Ybx2 and Ybx3 caused sterility characterized by extensive defects in spermatid differentiation. RNA sequence analysis of mRNP and polysome occupancy in single and compound Ybx2/3 heterozygotes revealed loss of translational repression almost exclusively in the compound Ybx2/3 heterozygotes. RNAseq analysis also demonstrated that Y-box protein dose-dependent loss of translational regulation was inversely correlated with the presence of a Y box recognition target sequence, suggesting that Y box proteins bind RNA hierarchically to modulate translation in a range of targets.

摘要

Y盒蛋白YBX2和YBX3可结合RNA和DNA,是后生动物发育和生育所必需的。然而,YBX2和YBX3之间可能存在的功能冗余阻碍了对它们作为RNA掩盖蛋白的分子功能的阐明以及对其靶RNA的鉴定。为了研究YBX2和YBX3之间可能存在的功能冗余,我们尝试使用先前报道的Ybx2-/-模型和新构建的全基因组Ybx3-/-模型构建Ybx2-/-;Ybx3-/-双突变体。YBX3的缺失导致雄性生育力下降和精子细胞分化缺陷。然而,由于Ybx2和Ybx3的单倍剂量不足导致不育,其特征为精子细胞分化存在广泛缺陷,因此无法产生纯合双突变体。对单Ybx2/3杂合子和复合Ybx2/3杂合子中mRNP和多核糖体占据情况的RNA序列分析表明,几乎仅在复合Ybx2/3杂合子中存在翻译抑制的丧失。RNA测序分析还表明,Y盒蛋白剂量依赖性的翻译调控丧失与Y盒识别靶序列的存在呈负相关,这表明Y盒蛋白以分级方式结合RNA,以调节一系列靶标的翻译。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c2f9/4672889/d57d3b8526fd/pgen.1005690.g001.jpg

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