A Conserved Mechanism of APOBEC3 Relocalization by Herpesviral Ribonucleotide Reductase Large Subunits

Cheng, Adam Z; Moraes, Sofia N; Attarian, Claire; Yockteng-Melgar, Jaime; Jarvis, Matthew C.; Biolatti, Matteo; Galitska, Ganna; Dell’Oste, Valentina; Frappier, Lori; Bierle, Craig J.; Rice, Stephen A.; Harris, Reuben S.

doi:10.1128/jvi.01539-19

Cited by 33 publications

(78 citation statements)

References 79 publications

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“…The A3 footprint on EBV is spatially limited to the lagging strands around the lytic replication origins. Interestingly, both EBV and KSHV were recently demonstrated to encode viral proteins capable of inhibiting A3B activity [ 28 , 65 ]. Those viral proteins (EBV BORF2 and KSHV ORF61) are both the large subunit of the ribonucleotide reductase, expressed during lytic replication and providing the precursors necessary for viral DNA synthesis.…”

Section: Discussionmentioning

confidence: 99%

Footprint of the host restriction factors APOBEC3 on the genome of human viruses

et al. 2020

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APOBEC3 enzymes are innate immune effectors that introduce mutations into viral genomes. These enzymes are cytidine deaminases which transform cytosine into uracil. They preferentially mutate cytidine preceded by thymidine making the 5'TC motif their favored target. Viruses have evolved different strategies to evade APOBEC3 restriction. Certain viruses actively encode viral proteins antagonizing the APOBEC3s, others passively face the APOBEC3 selection pressure thanks to a depleted genome for APOBEC3-targeted motifs. Hence, the APOBEC3s left on the genome of certain viruses an evolutionary footprint. The aim of our study is the identification of these viruses having a genome shaped by the APOBEC3s. We analyzed the genome of 33,400 human viruses for the depletion of APO-BEC3-favored motifs. We demonstrate that the APOBEC3 selection pressure impacts at least 22% of all currently annotated human viral species. The papillomaviridae and polyomaviridae are the most intensively footprinted families; evidencing a selection pressure acting genome-wide and on both strands. Members of the parvoviridae family are differentially targeted in term of both magnitude and localization of the footprint. Interestingly, a massive APOBEC3 footprint is present on both strands of the B19 erythroparvovirus; making this viral genome one of the most cleaned sequences for APOBEC3-favored motifs. We also identified the endemic coronaviridae as significantly footprinted. Interestingly, no such footprint has been detected on the zoonotic MERS-CoV, SARS-CoV-1 and SARS-CoV-2 coronaviruses. In addition to viruses that are footprinted genome-wide, certain viruses are footprinted only on very short sections of their genome. That is the case for the gamma-herpesviridae and adenoviridae where the footprint is localized on the lytic origins of replication. A mild footprint can also be detected on the negative strand of the reverse transcribing HIV-1, HIV-2, HTLV-1 and HBV viruses. Together, our data illustrate the extent of the APOBEC3 selection pressure on the human viruses and identify new putatively APOBEC3-targeted viruses.

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Section: Discussionmentioning

confidence: 99%

Footprint of the host restriction factors APOBEC3 on the genome of human viruses

et al. 2020

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“…Indeed, remnants of vif genelike ORFs have been identified in endogenous lentiviruses (43)(44)(45). In addition, it has recently been reported that herpesviruses encode ribonucleotide reductase large subunits that degrade human A3 proteins (5,46,47) and that the A3 antagonists of Epstein-Barr virus and Kaposi's sarcoma-associated herpesvirus specifically recognize the loop 7 structure of A3B (5). Therefore, A3 antagonists encoded by viruses other than retroviruses may also have exerted selective pressure on the loop 7 structures of A3 genes.…”

Section: Discussionmentioning

confidence: 99%

Retroviruses drive the rapid evolution of mammalianAPOBEC3genes

Ito

Gifford

Sato

2019

Proc. Natl. Acad. Sci. U.S.A.

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APOBEC3(A3) genes are members of theAID/APOBECgene family that are found exclusively in mammals.A3genes encode antiviral proteins that restrict the replication of retroviruses by inducing G-to-A mutations in their genomes and have undergone extensive amplification and diversification during mammalian evolution. Endogenous retroviruses (ERVs) are sequences derived from ancient retroviruses that are widespread mammalian genomes. In this study we characterize theA3repertoire and use the ERV fossil record to explore the long-term history of coevolutionary interaction between A3s and retroviruses. We examine the genomes of 160 mammalian species and identify 1,420AID/APOBEC-related genes, including representatives of previously uncharacterized lineages. We show thatA3genes have been amplified in mammals and that amplification is positively correlated with the extent of germline colonization by ERVs. Moreover, we demonstrate that the signatures of A3-mediated mutation can be detected in ERVs found throughout mammalian genomes and show that in mammalian species with expandedA3repertoires, ERVs are significantly enriched for G-to-A mutations. Finally, we show thatA3amplification occurred concurrently with prominent ERV invasions in primates. Our findings establish that conflict with retroviruses is a major driving force for the rapid evolution of mammalianA3genes.

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“…In this regard, our group has recently uncovered a novel mechanism of HCMV evasion from A3 restriction activity based on the progressive loss of APOBEC hot spots from its genome during evolution [ 10 ]. A3 inactivation as a means to evade host immune surveillance does not seem to be solely restricted to HCMV as other viruses, such as HSV-1 and Kaposi’s sarcoma-associated herpesvirus (KSHV), can delocalize A3 proteins and, in doing so, neutralize their antiviral activity through a conserved ribonucleotide reductase (RNR)-dependent mechanism [ 64 ]. More recently, APOBECs have been involved in SARS-CoV-2 RNA editing [ 65 ].…”

Section: Apobec Genes Vs Hpvs: Restriction Factors or Dna Editorsmentioning

confidence: 99%

HPV Meets APOBEC: New Players in Head and Neck Cancer

Riva

Albano

Gugliesi

et al. 2021

IJMS

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Besides smoking and alcohol, human papillomavirus (HPV) is a factor promoting head and neck squamous cell carcinoma (HNSCC). In some human tumors, including HNSCC, a number of mutations are caused by aberrantly activated DNA-modifying enzymes, such as the apolipoprotein B mRNA editing enzyme catalytic polypeptide-like (APOBEC) family of cytidine deaminases. As the enzymatic activity of APOBEC proteins contributes to the innate immune response to viruses, including HPV, the role of APOBEC proteins in HPV-driven head and neck carcinogenesis has recently gained increasing attention. Ongoing research efforts take the cue from two key observations: (1) APOBEC expression depends on HPV infection status in HNSCC; and (2) APOBEC activity plays a major role in HPV-positive HNSCC mutagenesis. This review focuses on recent advances on the role of APOBEC proteins in HPV-positive vs. HPV-negative HNSCC.

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A Conserved Mechanism of APOBEC3 Relocalization by Herpesviral Ribonucleotide Reductase Large Subunits

Cited by 33 publications

References 79 publications

Footprint of the host restriction factors APOBEC3 on the genome of human viruses

Footprint of the host restriction factors APOBEC3 on the genome of human viruses

Retroviruses drive the rapid evolution of mammalianAPOBEC3genes

HPV Meets APOBEC: New Players in Head and Neck Cancer

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