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Selective translational repression of truncated proteins from frameshift mutation-derived mRNAs in tumors SCIE SCOPUS

Title
Selective translational repression of truncated proteins from frameshift mutation-derived mRNAs in tumors
Authors
You, KTLi, LSKim, NGKang, HJKoh, KHChwae, YJKim, KMKim, YKPark, SMJang, SKKim, H
Date Issued
2007-05
Publisher
PUBLIC LIBRARY SCIENCE
Abstract
Frameshift and nonsense mutations are common in tumors with microsatellite instability, and mRNAs from these mutated genes have premature termination codons (PTCs). Abnormal mRNAs containing PTCs are normally degraded by the nonsense-mediated mRNA decay (NMD) system. However, PTCs located within 50-55 nucleotides of the last exon-exon junction are not recognized by NMD (NMD-irrelevant), and some PTC-containing mRNAs can escape from the NMD system (NMD-escape). We investigated protein expression from NMD-irrelevant and NMD-escape PTC-containing mRNAs by Western blotting and transfection assays. We demonstrated that transfection of NMD-irrelevant PTC-containing genomic DNA of MARCKS generates truncated protein. In contrast, NMD-escape PTC-containing versions of hMSH3 and TGFBR2 generate normal levels of mRNA, but do not generate detectable levels of protein. Transfection of NMD-escape mutant TGFBR2 genomic DNA failed to generate expression of truncated proteins, whereas transfection of wild-type TGFBR2 genomic DNA or mutant PTC-containing TGFBR2 cDNA generated expression of wild-type protein and truncated protein, respectively. Our findings suggest a novel mechanism of gene expression regulation for PTC-containing mRNAs in which the deleterious transcripts are regulated either by NMD or translational repression.
URI
https://oasis.postech.ac.kr/handle/2014.oak/12629
DOI
10.1371/JOURNAL.PBIO.0050109
ISSN
1544-9173
Article Type
Article
Citation
PLOS BIOLOGY, vol. 5, no. 5, page. 1098 - 1109, 2007-05
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장승기JANG, SUNG KEY
Dept of Life Sciences
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