Literature DB >> 27795410

Deep-Sequence Identification and Role in Virus Replication of a JC Virus Quasispecies in Patients with Progressive Multifocal Leukoencephalopathy.

Kenta Takahashi1, Tsuyoshi Sekizuka2, Hitomi Fukumoto1, Kazuo Nakamichi3, Tadaki Suzuki1, Yuko Sato1, Hideki Hasegawa1, Makoto Kuroda2, Harutaka Katano4.   

Abstract

JC virus (JCV) is a DNA virus causing progressive multifocal leukoencephalopathy (PML) in immunodeficient patients. In the present study, 22 genetic quasispecies with more than 1.5% variant frequency were detected in JCV genomes from six clinical samples of PML by next-generation sequencing. A mutation from A to C at nucleotide (nt) 3495 in JCV Mad1 resulting in a V-to-G amino acid substitution at amino acid (aa) position 392 of the large T antigen (TAg) was identified in all six cases of PML at 3% to 19% variant frequencies. Transfection of JCV Mad1 DNA possessing the V392G substitution in TAg into IMR-32 and human embryonic kidney 293 (HEK293) cells resulted in dramatically decreased production of JCV-encoded proteins. The virus DNA copy number was also reduced in supernatants of the mutant virus-transfected cells. Transfection of the IMR-32 and HEK293 cells with a virus genome containing a revertant mutation recovered viral production and protein expression. Cotransfection with equal amounts of wild-type genome and mutated JCV genome did not reduce the expression of viral proteins or viral replication, suggesting that the mutation did not have any dominant-negative function. Finally, immunohistochemistry demonstrated that TAg was expressed in all six pathological samples in which the quasispecies were detected. In conclusion, the V392G amino acid substitution in TAg identified frequently in PML lesions has a function in suppressing JCV replication, but the frequency of the mutation was restricted and its role in PML lesions was limited. IMPORTANCE: DNA viruses generally have lower mutation frequency than RNA viruses, and the detection of quasispecies in JCV has rarely been reported. In the present study, a next-generation sequencer identified a JCV quasispecies with an amino acid substitution in the T antigen in patients with PML. In vitro studies showed that the mutation strongly repressed the expression of JC viral proteins and reduced the viral replication. However, because the frequency of the mutation was low in each case, the total expression of virus proteins was sustained in vivo. Thus, JC virus replicates in PML lesions in the presence of a mutant virus which is able to repress virus replication.
Copyright © 2016 American Society for Microbiology.

Entities:  

Keywords:  JCV; PML; large T antigen; next-generation sequencer; progressive multifocal leukoencephalopathy; quasispecies; virus replication

Mesh:

Substances:

Year:  2016        PMID: 27795410      PMCID: PMC5165223          DOI: 10.1128/JVI.01335-16

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


  58 in total

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Authors:  Tom Van Loy; Kim Thys; Caroline Ryschkewitsch; Ole Lagatie; Maria C Monaco; Eugene O Major; Luc Tritsmans; Lieven J Stuyver
Journal:  J Virol       Date:  2014-11-12       Impact factor: 5.103

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3.  Human polyomavirus JC virus genome.

Authors:  R J Frisque; G L Bream; M T Cannella
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4.  Human polyomavirus JC promoter/enhancer rearrangement patterns from progressive multifocal leukoencephalopathy brain are unique derivatives of a single archetypal structure.

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Authors:  Tina Dalianis; Hans H Hirsch
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Journal:  Jpn J Infect Dis       Date:  2013       Impact factor: 1.362

9.  Sequencing and analysis of JC virus DNA from natalizumab-treated PML patients.

Authors:  Carl E Reid; Huo Li; Gargi Sur; Paul Carmillo; Steven Bushnell; Rich Tizard; Michele McAuliffe; Christopher Tonkin; Kenneth Simon; Susan Goelz; Paola Cinque; Leonid Gorelik; John P Carulli
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Authors:  Shamil R Sunyaev; Alexey Lugovskoy; Kenneth Simon; Leonid Gorelik
Journal:  PLoS Genet       Date:  2009-02-06       Impact factor: 5.917

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1.  Progressive multifocal leukoencephalopathy during ixazomib-based chemotherapy.

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2.  ViroFind: A novel target-enrichment deep-sequencing platform reveals a complex JC virus population in the brain of PML patients.

Authors:  Spyros Chalkias; Joshua M Gorham; Erica Mazaika; Michael Parfenov; Xin Dang; Steve DePalma; David McKean; Christine E Seidman; Jonathan G Seidman; Igor J Koralnik
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3.  Exploring the role of NCCR variation on JC polyomavirus expression from dual reporter minicircles.

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4.  Promoter activity of Merkel cell Polyomavirus variants in human dermal fibroblasts and a Merkel cell carcinoma cell line.

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5.  High expression of JC polyomavirus-encoded microRNAs in progressive multifocal leukoencephalopathy tissues and its repressive role in virus replication.

Authors:  Kenta Takahashi; Yuko Sato; Tsuyoshi Sekizuka; Makoto Kuroda; Tadaki Suzuki; Hideki Hasegawa; Harutaka Katano
Journal:  PLoS Pathog       Date:  2020-04-23       Impact factor: 6.823

6.  Database and Statistical Analyses of Transcription Factor Binding Sites in the Non-Coding Control Region of JC Virus.

Authors:  Kazuo Nakamichi; Toshio Shimokawa
Journal:  Viruses       Date:  2021-11-19       Impact factor: 5.048

Review 7.  Understanding Progressive Multifocal Leukoencephalopathy Risk in Multiple Sclerosis Patients Treated with Immunomodulatory Therapies: A Bird's Eye View.

Authors:  Elizabeth A Mills; Yang Mao-Draayer
Journal:  Front Immunol       Date:  2018-02-02       Impact factor: 7.561

8.  Viral quasispecies.

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Journal:  PLoS Genet       Date:  2019-10-17       Impact factor: 5.917

Review 9.  JCPyV VP1 Mutations in Progressive MultifocalLeukoencephalopathy: Altering Tropismor Mediating Immune Evasion?

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Journal:  Viruses       Date:  2020-10-12       Impact factor: 5.048

Review 10.  Human Brain Organoids as Models for Central Nervous System Viral Infection.

Authors:  Josse A Depla; Lance A Mulder; Renata Vieira de Sá; Morgane Wartel; Adithya Sridhar; Melvin M Evers; Katja C Wolthers; Dasja Pajkrt
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  10 in total

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