Ribosomal frameshifting at normal codon repeats recodes functional chimeric proteins in human

Author:

Ren Guiping12ORCID,Gu Xiaoqian12,Zhang Lu12,Gong Shimin12,Song Shuang12,Chen Shunkai12,Chen Zhenjing12,Wang Xiaoyan12,Li Zhanbiao12,Zhou Yingshui12,Li Longxi12,Yang Jiao12,Lai Fan12,Dang Yunkun12ORCID

Affiliation:

1. State Key Laboratory for Conservation and Utilization of Bio-Resource in Yunnan, Key Laboratory for Southwest Microbial Diversity of the Ministry of Education, Yunnan Key Laboratory of Cell Metabolism and Diseases, Center for Life Science, School of Life Sciences, Yunnan University , Kunming  650021 , China

2. Southwest United Graduate School , Kunming 650092 , China

Abstract

Abstract Ribosomal frameshifting refers to the process that ribosomes slip into +1 or −1 reading frame, thus produce chimeric trans-frame proteins. In viruses and bacteria, programmed ribosomal frameshifting can produce essential trans-frame proteins for viral replication or regulation of other biological processes. In humans, however, functional trans-frame protein derived from ribosomal frameshifting is scarcely documented. Combining multiple assays, we show that short codon repeats could act as cis-acting elements that stimulate ribosomal frameshifting in humans, abbreviated as CRFS hereafter. Using proteomic analyses, we identified many putative CRFS events from 32 normal human tissues supported by trans-frame peptides positioned at codon repeats. Finally, we show a CRFS-derived trans-frame protein (HDAC1-FS) functions by antagonizing the activities of HDAC1, thus affecting cell migration and apoptosis. These data suggest a novel type of translational recoding associated with codon repeats, which may expand the coding capacity of mRNA and diversify the regulation in human.

Funder

National Natural Science Foundation of China

Open Research Program of State Key Laboratory for Conservation and Utilization of Bio-Resources in Yunnan

Yunnan Province Science and Technology Department

Yunnan University

Publisher

Oxford University Press (OUP)

Subject

Genetics

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