Insight into the ERVK Integrase - Propensity for DNA Damage

Overview

Journal Front Microbiol

Specialty Microbiology

Date 2016 Dec 20

PMID 27990140

Citations 7

Authors

Samantha Bray

Matthew Turnbull

Sherry Hebert

Renee N Douville

Affiliations

Soon will be listed here.

Abstract

Retroviruses create permanently integrated proviruses that exist in the host genome. Retroviral genomes encode for functionally conserved , and regions, as well as integrase (IN), which is required for retroviral integration. IN mediates viral genome insertion through 3' end processing of the viral DNA and the strand transfer reaction. This process requires the formation of a pre-integration complex, comprised of IN, viral DNA, and cellular proteins. Viral insertion causes DNA damage, leading to the requirement of host DNA repair mechanisms. Therefore, a failure of DNA repair pathways may result in genomic instability and potentially cause host cell death. Considering the numerous human diseases associated with genomic instability, the endogenous retrovirus-K (ERVK) IN should be considered as a putative contributor to DNA damage in human cells. Future research and drug discovery should focus on ERVK IN activity and its role in human conditions, such as neurological disease and cancers.

Citing Articles

Interaction of HERVs with PAMPs in Dysregulation of Immune Response Cascade Upon SARS-CoV-2 Infections.

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Human Endogenous Retrovirus-K (HML-2)-Related Genetic Variation: Human Genome Diversity and Disease.

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Retrotransposons as a Source of DNA Damage in Neurodegeneration.

Peze-Heidsieck E, Bonnifet T, Znaidi R, Ravel-Godreuil C, Massiani-Beaudoin O, Joshi R Front Aging Neurosci. 2022; 13:786897.

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Predicted Cellular Interactors of the Endogenous Retrovirus-K Integrase Enzyme.

Benoit I, Brownell S, Douville R Microorganisms. 2021; 9(7).

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