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Review
. 2024 Sep;96(9):e29886.
doi: 10.1002/jmv.29886.

Long-term persistence of mitochondrial dysfunctions after viral infections and antiviral therapies: A review of mechanisms involved

Laetitia Gay  1 Valérie Desquiret-Dumas  2   3 Nicolas Nagot  1 Clara Rapenne  2   3 Philippe Van de Perre  1 Pascal Reynier  2   3 Jean-Pierre Molès  1
Affiliations
Review

Long-term persistence of mitochondrial dysfunctions after viral infections and antiviral therapies: A review of mechanisms involved

Laetitia Gay et al. J Med Virol. 2024 Sep.

Abstract

Mitochondria are vital for most cells' functions. Viruses hijack mitochondria machinery for misappropriation of energy supply or to bypass defense mechanisms. Many of these mitochondrial dysfunctions persist after recovery from treated or untreated viral infections, particularly when mitochondrial DNA is permanently damaged. Quantitative defects and structural rearrangements of mitochondrial DNA accumulate in post-mitotic tissues as recently reported long after SARS-CoV-2 or HIV infection, or following antiviral therapy. These observations are consistent with the "hit-and-run" concept proposed decades ago to explain viro-induced cell transformation and it could apply to delayed post-viral onsets of symptoms and advocate for complementary supportive care. Thus, according to this concept, following exposure to viruses or antiviral agents, mitochondrial damage could evolve into an autonomous clinical condition. It also establishes a pathogenic link between communicable and non-communicable chronic diseases.

Keywords: antiviral treatment; delayed disease onset; genetic alterations; hit‐and‐run concept; mitochondria; virus.

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