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Human cytomegalovirus harnesses host L1 retrotransposon for efficient replication

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Title
Human cytomegalovirus harnesses host L1 retrotransposon for efficient replication
Author(s)
Sung-Yeon Hwang; Hyewon Kim; Denisko, Danielle; Zhao, Boxun; Lee, Dohoon; Jiseok Jeong; Kim, Jinuk; Kiwon Park; Junhyun Park; Dongjoon Jeong; Sehong Park; Choi, Hee-Jung; Kim, Sun; Lee, Eunjung Alice; Kwangseog Ahn
Publication Date
2024-09
Journal
Nature Communications, v.15, no.1
Publisher
Nature Publishing Group
Abstract
Genetic parasites, including viruses and transposons, exploit components from the host for their own replication. However, little is known about virus-transposon interactions within host cells. Here, we discover a strategy where human cytomegalovirus (HCMV) hijacks L1 retrotransposon encoded protein during its replication cycle. HCMV infection upregulates L1 expression by enhancing both the expression of L1-activating transcription factors, YY1 and RUNX3, and the chromatin accessibility of L1 promoter regions. Increased L1 expression, in turn, promotes HCMV replicative fitness. Affinity proteomics reveals UL44, HCMV DNA polymerase subunit, as the most abundant viral binding protein of the L1 ribonucleoprotein (RNP) complex. UL44 directly interacts with L1 ORF2p, inducing DNA damage responses in replicating HCMV compartments. While increased L1-induced mutagenesis is not observed in HCMV for genetic adaptation, the interplay between UL44 and ORF2p accelerates viral DNA replication by alleviating replication stress. Our findings shed light on how HCMV exploits host retrotransposons for enhanced viral fitness. © The Author(s) 2024.
URI
https://pr.ibs.re.kr/handle/8788114/15671
DOI
10.1038/s41467-024-51961-y
Appears in Collections:
Center for RNA Research(RNA 연구단) > 1. Journal Papers (저널논문)
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