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Literature DB >> 25855736

Regulation of Hepatitis C Virus Genome Replication by Xrn1 and MicroRNA-122 Binding to Individual Sites in the 5' Untranslated Region.

Patricia A Thibault¹, Adam Huys¹, Yalena Amador-Cañizares², Julie E Gailius², Dayna E Pinel², Joyce A Wilson³.

Abstract

UNLABELLED: miR-122 is a liver-specific microRNA (miRNA) that binds to two sites (S1 and S2) on the 5' untranslated region (UTR) of the hepatitis C virus (HCV) genome and promotes the viral life cycle. It positively affects viral RNA stability, translation, and replication, but the mechanism is not well understood. To unravel the roles of miR-122 binding at each site alone or in combination, we employed miR-122 binding site mutant viral RNAs, Hep3B cells (which lack detectable miR-122), and complementation with wild-type miR-122, an miR-122 with the matching mutation, or both. We found that miR-122 binding at either site alone increased replication equally, while binding at both sites had a cooperative effect. Xrn1 depletion rescued miR-122-unbound full-length RNA replication to detectable levels but not to miR-122-bound levels, confirming that miR-122 protects HCV RNA from Xrn1, a cytoplasmic 5'-to-3' exoribonuclease, but also has additional functions. In cells depleted of Xrn1, replication levels of S1-bound HCV RNA were slightly higher than S2-bound RNA levels, suggesting that both sites contribute, but their contributions may be unequal when the need for protection from Xrn1 is reduced. miR-122 binding at S1 or S2 also increased translation equally, but the effect was abolished by Xrn1 knockdown, suggesting that the influence of miR-122 on HCV translation reflects protection from Xrn1 degradation. Our results show that occupation of each miR-122 binding site contributes equally and cooperatively to HCV replication but suggest somewhat unequal contributions of each site to Xrn1 protection and additional functions of miR-122. IMPORTANCE: The functions of miR-122 in the promotion of the HCV life cycle are not fully understood. Here, we show that binding of miR-122 to each of the two binding sites in the HCV 5' UTR contributes equally to HCV replication and that binding to both sites can function cooperatively. This suggests that active Ago2-miR-122 complexes assemble at each site and can cooperatively promote the association and/or function of adjacent complexes, similar to what has been proposed for translation suppression by adjacent miRNA binding sites. We also confirm a role for miR-122 in protection from Xrn1 and provide evidence that miR-122 has additional functions in the HCV life cycle unrelated to Xrn1. Finally, we show that each binding site may contribute unequally to Xrn1 protection and other miR-122 functions.

Entities: Disease Gene Species

Mesh：

Substances：

Year: 2015 PMID： 25855736 PMCID： PMC4474307 DOI： 10.1128/JVI.03631-14

Source DB: PubMed Journal: J Virol ISSN： 0022-538X Impact factor: 5.103

45 in total

1. Base pairing between hepatitis C virus RNA and microRNA 122 3' of its seed sequence is essential for genome stabilization and production of infectious virus.

Authors: Tetsuro Shimakami; Daisuke Yamane; Christoph Welsch; Lucinda Hensley; Rohit K Jangra; Stanley M Lemon
Journal: J Virol Date: 2012-04-24 Impact factor: 5.103

2. miR-122 is more than a shield for the hepatitis C virus genome.

Authors: Adolfo García-Sastre; Matthew J Evans
Journal: Proc Natl Acad Sci U S A Date: 2013-01-16 Impact factor: 11.205

3. Stabilization of hepatitis C virus RNA by an Ago2-miR-122 complex.

Authors: Tetsuro Shimakami; Daisuke Yamane; Rohit K Jangra; Brian J Kempf; Carolyn Spaniel; David J Barton; Stanley M Lemon
Journal: Proc Natl Acad Sci U S A Date: 2012-01-03 Impact factor: 11.205

4. Modulation of hepatitis C virus RNA abundance and virus release by dispersion of processing bodies and enrichment of stress granules.

Authors: Cara T Pager; Sylvia Schütz; Teresa M Abraham; Guangxiang Luo; Peter Sarnow
Journal: Virology Date: 2012-11-09 Impact factor: 3.616

5. Requirements for human Dicer and TRBP in microRNA-122 regulation of HCV translation and RNA abundance.

Authors: Chao Zhang; Adam Huys; Patricia A Thibault; Joyce A Wilson
Journal: Virology Date: 2012-09-19 Impact factor: 3.616

6. MicroRNA-122 antagonism against hepatitis C virus genotypes 1-6 and reduced efficacy by host RNA insertion or mutations in the HCV 5' UTR.

Authors: Yi-Ping Li; Judith M Gottwein; Troels K Scheel; Tanja B Jensen; Jens Bukh
Journal: Proc Natl Acad Sci U S A Date: 2011-03-07 Impact factor: 11.205

7. Hepatitis C virus hijacks P-body and stress granule components around lipid droplets.

Authors: Yasuo Ariumi; Misao Kuroki; Yukihiro Kushima; Kanae Osugi; Makoto Hijikata; Masatoshi Maki; Masanori Ikeda; Nobuyuki Kato
Journal: J Virol Date: 2011-05-04 Impact factor: 5.103

8. Competing and noncompeting activities of miR-122 and the 5' exonuclease Xrn1 in regulation of hepatitis C virus replication.

Authors: You Li; Takahiro Masaki; Daisuke Yamane; David R McGivern; Stanley M Lemon
Journal: Proc Natl Acad Sci U S A Date: 2012-12-17 Impact factor: 11.205

9. MicroRNA-122-dependent and -independent replication of Hepatitis C Virus in Hep3B human hepatoma cells.

Authors: Patricia A Thibault; Adam Huys; Pearl Dhillon; Joyce A Wilson
Journal: Virology Date: 2012-12-13 Impact factor: 3.616

10. MicroRNA-122 dependent binding of Ago2 protein to hepatitis C virus RNA is associated with enhanced RNA stability and translation stimulation.

Authors: K Dominik Conrad; Florian Giering; Corinna Erfurth; Angelina Neumann; Carmen Fehr; Gunter Meister; Michael Niepmann
Journal: PLoS One Date: 2013-02-06 Impact factor: 3.240

37 in total

Review 1. Small molecules with big roles in microRNA chemical biology and microRNA-targeted therapeutics.

Authors: Rengen Fan; Chaocheng Xiao; Xinqiang Wan; Wenzhang Cha; Yufeng Miao; Yong Zhou; Chenglin Qin; Ting Cui; Fenglian Su; Xiangxiang Shan
Journal: RNA Biol Date: 2019-04-03 Impact factor: 4.652

2. miR-122 and Ago interactions with the HCV genome alter the structure of the viral 5' terminus.

Authors: Jasmin Chahal; Luca F R Gebert; Hin Hark Gan; Edna Camacho; Kristin C Gunsalus; Ian J MacRae; Selena M Sagan
Journal: Nucleic Acids Res Date: 2019-06-04 Impact factor: 16.971

Review 3. Using Genome Sequence to Enable the Design of Medicines and Chemical Probes.

Authors: Alicia J Angelbello; Jonathan L Chen; Jessica L Childs-Disney; Peiyuan Zhang; Zi-Fu Wang; Matthew D Disney
Journal: Chem Rev Date: 2018-01-11 Impact factor: 60.622

4. Polymer nanocarriers for MicroRNA delivery.

Authors: Chintan H Kapadia; Benjamin Luo; Megan N Dang; N'Dea Irvin-Choy; Danielle M Valcourt; Emily S Day
Journal: J Appl Polym Sci Date: 2019-11-12 Impact factor: 3.125

5. The exoribonuclease Xrn1 is a post-transcriptional negative regulator of autophagy.

Authors: Elizabeth Delorme-Axford; Emma Abernathy; Nicholas J Lennemann; Amélie Bernard; Aileen Ariosa; Carolyn B Coyne; Karla Kirkegaard; Daniel J Klionsky
Journal: Autophagy Date: 2018-03-21 Impact factor: 16.016

6. Human MicroRNA-548p Decreases Hepatic Apolipoprotein B Secretion and Lipid Synthesis.

Authors: Liye Zhou; M Mahmood Hussain
Journal: Arterioscler Thromb Vasc Biol Date: 2017-03-23 Impact factor: 8.311

Review 7. The emerging role and significance of circular RNAs in viral infections and antiviral immune responses: possible implication as theranostic agents.

Authors: Faryal Mehwish Awan; Burton B Yang; Anam Naz; Aneeqa Hanif; Aqsa Ikram; Ayesha Obaid; Arif Malik; Hussnain Ahmed Janjua; Amjad Ali; Sumaira Sharif
Journal: RNA Biol Date: 2020-07-13 Impact factor: 4.652