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  4. Epitranscriptomic cytidine methylation of the hepatitis B viral RNA is essential for viral reverse transcription and particle production.
 
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Epitranscriptomic cytidine methylation of the hepatitis B viral RNA is essential for viral reverse transcription and particle production.

Journal
Proceedings of the National Academy of Sciences of the United States of America
Journal Volume
121
Journal Issue
24
Start Page
e2400378121
ISSN
1091-6490
Date Issued
2024-06-11
Author(s)
Su, Pei-Yi Alma
Chang, Chih-Hsu
Yen, Shin-Chwen Bruce
Wu, Hsiu-Yi
Tung, Wan-Ju
Hu, Yu-Pei
Chen, Yen-Yu Ian
Lin, Miao-Hsia  
Shih, Chiaho
Chen, Pei-Jer  
Tsai, Kevin
DOI
10.1073/pnas.2400378121
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/723040
Abstract
Epitranscriptomic RNA modifications have emerged as important regulators of the fate and function of viral RNAs. One prominent modification, the cytidine methylation 5-methylcytidine (mC), is found on the RNA of HIV-1, where mC enhances the translation of HIV-1 RNA. However, whether mC functionally enhances the RNA of other pathogenic viruses remains elusive. Here, we surveyed a panel of commonly found RNA modifications on the RNA of hepatitis B virus (HBV) and found that HBV RNA is enriched with mC as well as ten other modifications, at stoichiometries much higher than host messenger RNA (mRNA). Intriguingly, mC is mostly found on the epsilon hairpin, an RNA element required for viral RNA encapsidation and reverse transcription, with these mC mainly deposited by the cellular methyltransferase NSUN2. Loss of mC from HBV RNA due to NSUN2 depletion resulted in a partial decrease in viral core protein (HBc) production, accompanied by a near-complete loss of the reverse transcribed viral DNA. Similarly, mutations introduced to remove the methylated cytidines resulted in a loss of HBc production and reverse transcription. Furthermore, pharmacological disruption of mC deposition led to a significant decrease in HBV replication. Thus, our data indicate mC methylations as a critical mediator of the epsilon elements' function in HBV virion production and reverse transcription, suggesting the therapeutic potential of targeting the mC methyltransfer process on HBV epsilon as an antiviral strategy.
Subjects
NSUN2
RNA modifications
hepatitis B virus
m5C
reverse transcription
SDGs

[SDGs]SDG3

Type
journal article

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