| Literature DB >> 33476374 |
Jingzhen Li1, Fei Liu1, Yuexia Lv1, Kui Sun1, Yuntong Zhao2, Jamas Reilly3, Yangjun Zhang1, Jiayi Tu1, Shanshan Yu1, Xiliang Liu1, Yayun Qin1, Yuwen Huang1, Pan Gao1, Danna Jia1, Xiang Chen1, Yunqiao Han1, Xinhua Shu3, Daji Luo2, Zhaohui Tang1, Mugen Liu1.
Abstract
Dysfunction of splicing factors often result in abnormal cell differentiation and apoptosis, especially in neural tissues. Mutations in pre-mRNAs processing factor 31 (PRPF31) cause autosomal dominant retinitis pigmentosa, a progressive retinal degeneration disease. The transcriptome-wide splicing events specifically regulated by PRPF31 and their biological roles in the development and maintenance of retina are still unclear. Here, we showed that the differentiation and viability of retinal progenitor cells (RPCs) are severely perturbed in prpf31 knockout zebrafish when compared with other tissues at an early embryonic stage. At the cellular level, significant mitotic arrest and DNA damage were observed. These defects could be rescued by the wild-type human PRPF31 rather than the disease-associated mutants. Further bioinformatic analysis and experimental verification uncovered that Prpf31 deletion predominantly causes the skipping of exons with a weak 5' splicing site. Moreover, genes necessary for DNA repair and mitotic progression are most enriched among the differentially spliced events, which may explain the cellular and tissular defects in prpf31 mutant retinas. This is the first time that Prpf31 is demonstrated to be essential for the survival and differentiation of RPCs during retinal neurogenesis by specifically modulating the alternative splicing of genes involved in DNA repair and mitosis.Entities:
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Year: 2021 PMID: 33476374 PMCID: PMC7913766 DOI: 10.1093/nar/gkab003
Source DB: PubMed Journal: Nucleic Acids Res ISSN: 0305-1048 Impact factor: 16.971