Molecular mechanism of human ISG20L2 for the ITS1 cleavage in the processing of 18S precursor ribosomal RNA

Author:

Ma Yinliang1,Wang Jiaxu12,He Xingyi1,Liu Yuhang1,Zhen Shuo1,An Lina1,Yang Qian1,Niu Fumin1,Wang Hong1,An Boran3,Tai Xinyue1,Yan Zhenzhen1,Wu Chen1ORCID,Yang Xiaoyun14ORCID,Liu Xiuhua1ORCID

Affiliation:

1. College of Life Sciences, Hebei Innovation Center for Bioengineering and Biotechnology, Institute of Life Sciences and Green Development, Hebei University , Baoding 071002  Hebei , China

2. College of Life Sciences, State Key Laboratory of Cell Differentiation and Regulation, Henan International Joint Laboratory of Pulmonary Fibrosis, Henan Normal University , Xinxiang 453002 Henan , China

3. Affiliated Hospital of Hebei University, Hebei University , Baoding 071002  Hebei , China

4. Department of Biology, Southern University of Science and Technology , Shenzhen 518055  Guangdong , China

Abstract

Abstract The exonuclease ISG20L2 has been initially characterized for its role in the mammalian 5.8S rRNA 3′ end maturation, specifically in the cleavage of ITS2 of 12S precursor ribosomal RNA (pre-rRNA). Here, we show that human ISG20L2 is also involved in 18S pre-rRNA maturation through removing the ITS1 region, and contributes to ribosomal biogenesis and cell proliferation. Furthermore, we determined the crystal structure of the ISG20L2 nuclease domain at 2.9 Å resolution. It exhibits the typical αβα fold of the DEDD 3′-5′ exonuclease with a catalytic pocket located in the hollow near the center. The catalytic residues Asp183, Glu185, Asp267, His322 and Asp327 constitute the DEDDh motif in ISG20L2. The active pocket represents conformational flexibility in the absence of an RNA substrate. Using structural superposition and mutagenesis assay, we mapped RNA substrate binding residues in ISG20L2. Finally, cellular assays revealed that ISG20L2 is aberrantly up-regulated in colon adenocarcinoma and promotes colon cancer cell proliferation through regulating ribosome biogenesis. Together, these results reveal that ISG20L2 is a new enzymatic member for 18S pre-rRNA maturation, provide insights into the mechanism of ISG20L2 underlying pre-rRNA processing, and suggest that ISG20L2 is a potential therapeutic target for colon adenocarcinoma.

Funder

National Natural Science Foundation of China

Publisher

Oxford University Press (OUP)

Subject

Genetics

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