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Yeast genetic interaction screen of human genes associated with amyotrophic lateral sclerosis: identification of MAP2K5 kinase as a potential drug target

Authors
Jo, MyungjinChung, Ah YoungYachie, NozomuSeo, MinchulJeon, HyejinYoungpyo NamSeo, YeojinKim, EunmiZhong, QuanVidal, MarcPark, Hae ChulRoth, Frederick P.Suk, Kyoungho
Issue Date
9월-2017
Publisher
COLD SPRING HARBOR LAB PRESS, PUBLICATIONS DEPT
Citation
GENOME RESEARCH, v.27, no.9, pp.1487 - 1500
Indexed
SCIE
SCOPUS
Journal Title
GENOME RESEARCH
Volume
27
Number
9
Start Page
1487
End Page
1500
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/82301
DOI
10.1101/gr.211649.116
ISSN
1088-9051
Abstract
To understand disease mechanisms, a large-scale analysis of human yeast genetic interactions was performed. Of 1305 human disease genes assayed, 20 genes exhibited strong toxicity in yeast. Human yeast genetic interactions were identified by en masse transformation of the human disease genes into a pool of 4653 homozygous diploid yeast deletion mutants with unique barcode sequences, followed by multiplexed barcode sequencing to identify yeast toxicity modifiers. Subsequent network analyses focusing on amyotrophic lateral sclerosis (ALS)-associated genes, such as optineurin (OPTIV) and angiogenin (ANG), showed that the human orthologs of the yeast toxicity modifiers of these ALS genes are enriched for several biological processes, such as cell death, lipid metabolism, and molecular transport. When yeast genetic interaction partners held in common between human OPTN and ANG were validated in mammalian cells and zebrafish, MAP2K5 kinase emerged as a potential drug target for ALS therapy. The toxicity modifiers identified in this study may deepen our understanding of the pathogenic mechanisms of ALS and other devastating diseases.
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