Structural basis for Gemin5 decamer-mediated mRNA binding

Author:

Guo Qiong,Zhao Shidong,Francisco-Velilla RosarioORCID,Zhang Jiahai,Embarc-Buh AzmanORCID,Abellan SalvadorORCID,Lv Mengqi,Tang Peiping,Gong Qingguo,Shen HuaizongORCID,Sun LinfengORCID,Yao XuebiaoORCID,Min JinrongORCID,Shi Yunyu,Martínez-Salas EncarnacionORCID,Zhang KaimingORCID,Xu ChaoORCID

Abstract

AbstractGemin5 in the Survival Motor Neuron (SMN) complex serves as the RNA-binding protein to deliver small nuclear RNAs (snRNAs) to the small nuclear ribonucleoprotein Sm complex via its N-terminal WD40 domain. Additionally, the C-terminal region plays an important role in regulating RNA translation by directly binding to viral RNAs and cellular mRNAs. Here, we present the three-dimensional structure of the Gemin5 C-terminal region, which adopts a homodecamer architecture comprised of a dimer of pentamers. By structural analysis, mutagenesis, and RNA-binding assays, we find that the intact pentamer/decamer is critical for the Gemin5 C-terminal region to bind cognate RNA ligands and to regulate mRNA translation. The Gemin5 high-order architecture is assembled via pentamerization, allowing binding to RNA ligands in a coordinated manner. We propose a model depicting the regulatory role of Gemin5 in selective RNA binding and translation. Therefore, our work provides insights into the SMN complex-independent function of Gemin5.

Funder

National Natural Science Foundation of China

the Thousand Young Talent program

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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