Viral persistence, reactivation, and mechanisms of long COVID, 2023, Chen et al.

Discussion in 'Long Covid research' started by SNT Gatchaman, May 5, 2023.

  1. SNT Gatchaman

    SNT Gatchaman Senior Member (Voting Rights)

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    Viral persistence, reactivation, and mechanisms of long COVID
    Benjamin Chen; Boris Julg; Sindhu Mohandas; Steven B Bradfute; RECOVER Mechanistic Pathways Task Force; Zaki A Sherif; Christian R Gomez; Thomas J Connors; Timothy J Henrich; W Brian Reeves; K Coombs; C Kim; Pras Jagannathan; Christian Bime; Erin Burke Quinlan; Michael A Portman; Maria Laura Gennaro; Jalees Rehman

    The COVID-19 global pandemic caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection has infected hundreds of millions of individuals. Following COVID-19 infection, a subset can develop a wide range of chronic symptoms affecting diverse organ systems referred to as post-acute sequelae of SARS-CoV-2 infection (PASC), also known as long COVID.

    A National Institutes of Health-sponsored initiative, RECOVER: Researching COVID to Enhance Recovery, has sought to understand the basis of long COVID in a large cohort. Given the range of symptoms that occur in long COVID, the mechanisms that may underlie these diverse symptoms may also be diverse.

    In this review, we focus on the emerging literature supporting the role(s) that viral persistence or reactivation of viruses may play in PASC. Persistence of SARS-CoV-2 RNA or antigens is reported in some organs, yet the mechanism by which they do so and how they may be associated with pathogenic immune responses is unclear. Understanding the mechanisms of persistence of RNA, antigen or other reactivated viruses and how they may relate to specific inflammatory responses that drive symptoms of PASC may provide a rationale for treatment.

    Link (eLife)
     
  2. SNT Gatchaman

    SNT Gatchaman Senior Member (Voting Rights)

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    For DNA, only if they are reactivated fully to the lytic state, where viral DNA might then be present extra-cellularly and therefore detectable in plasma? From HHV-6 encoded small non-coding RNAs define an intermediate and early stage in viral reactivation (2018) —

    (MicroRNAs aka miRNA are a subset of small non-coding RNAs aka sncRNA. Transactivation is also termed abortive-lytic.) Unclear how easily they might be detectable in blood via RNA sequencing, as above, rather than viral DNA.

    From the case report included in the 2018 paper —

     
    Last edited: May 5, 2023

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