Identifying Recombination Hot Spots in the HIV-1 Genome

Smyth, Redmond P.; Schlub, Timothy E.; Grimm, Andrew; Waugh, Caryll; Ellenberg, Paula; Chopra, Abha; Mallal, S.; Cromer, Deborah; Mak, Johnson; Davenport, Miles P.

doi:10.1128/jvi.03014-13

Cited by 48 publications

(40 citation statements)

References 69 publications

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“…This hotspot has previously been reported in a study on HIV-1 subtype B 72 . The hotspot positions II and IV have also been reported previously 73 . To date, eighteen distinct subtype G-related CRFs have been described (www.hiv.lanl.gov).…”

Section: Discussionsupporting

confidence: 77%

Characterisation of HIV-1 Molecular Epidemiology in Nigeria: Origin, Diversity, Demography and Geographic Spread

Nazziwa

Faria

Chaplin

et al. 2020

Sci Rep

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Nigeria has the highest number of AIDS-related deaths in the world. In this study, we characterised the HIV-1 molecular epidemiology by analysing 1442 HIV-1 pol sequences collected 1999-2014 from four geopolitical zones in Nigeria using state-of-the-art maximum-likelihood and Bayesian phylogenetic analyses. The main circulating forms were the circulating recombinant form (CRF) 02_AG (44% of the analysed sequences), CRF43_02G (16%), and subtype G (8%). Twenty-three percent of the sequences represented unique recombinant forms (URFs), whereof 37 (11%) could be grouped into seven potentially novel CRFs. Bayesian phylodynamic analysis suggested that five major Nigerian HIV-1 subepidemics were introduced in the 1960s and 1970s, close to the Nigerian Civil War. The analysis also indicated that the number of effective infections decreased in Nigeria after the introduction of free antiretroviral treatment in 2006. Finally, Bayesian phylogeographic analysis suggested gravity-like dynamics in which virus lineages first emerge and expand within large urban centers such as Abuja and Lagos, before migrating towards smaller rural areas. This study provides novel insight into the Nigerian HIV-1 epidemic and may have implications for future HIV-1 prevention strategies in Nigeria and other severely affected countries.

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Section: Discussionsupporting

confidence: 77%

Characterisation of HIV-1 Molecular Epidemiology in Nigeria: Origin, Diversity, Demography and Geographic Spread

Nazziwa

Faria

Chaplin

et al. 2020

Sci Rep

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show abstract

“…We have recently shown that the rate of template switching varies across the HIV genome [31], and thus a gene-specific switching rate may be more appropriate. Owing to the limited availability of sequence data, it was not possible for us neither to compare the template-switching rate in this region with a rate in other regions nor to calculate the presence of recombination 'hotspots' over the env region.…”

Section: Discussionmentioning

confidence: 99%

Estimating the in-vivo HIV template switching and recombination rate

Cromer

Grimm

Schlub

et al. 2016

Aids

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“…Currently, there are at least 98 CRFs , and numerous URFs identified, composed of pure and other recombinant subtypes including under‐sampled parental lineages that cannot be reasonably classified within the established HIV‐1 M subtypes . Recombination‐prone sites have been identified ; however, recombination events are scattered along the whole HIV genome . Most genotypic HIV‐1 M data is determined through partial genomic sequencing of one or a few limited regions.…”

Section: Introductionmentioning

confidence: 99%

Near full genome characterization of HIV‐1 unique recombinant forms in Cameroon reveals dominant CRF02_AG and F2 recombination patterns

et al. 2019

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Introduction In Cameroon, a manifold diversity of HIV strains exists with CRF02_AG and unique recombinant forms (URFs) being the predominant strains. In recent years, a steady increase in URFs and clade F2 viruses has been monitored through partial genome sequencing. There is an information gap in the characterization of emerging URFs along the full genome, which is needed to address the challenges URFs pose towards diagnosis, treatment and HIV‐1 vaccine design. Method Eighteen Cameroonian URFs from samples collected between the years 2000 and 2015 were studied using a newly developed near full genome sequencing (NFGS) protocol based on variable nested RT‐PCRs with a versatile primer set. Near full genomes were characterized for recombination patterns and sequence signatures with possible impact on antiretroviral treatment or Env‐directed immune responses. Third‐generation sequencing (3GS) of near full or half genomes (HGs) gave insight into intra‐patient URF diversity. Results The characterized URFs were composed of a broad variety of subtypes and recombinants including A, F, G, CRF01_AE, CRF02_AG and CRF22_01A1. Phylogenetic analysis unveiled dominant CRF02_AG and F2 recombination patterns. 3GS indicated a high intra‐patient URF diversity with up to four distinct viral sub‐populations present in plasma at the same time. URF pol genomic analysis revealed a number of accessory drug resistance mutations (DRMs) in the ART‐naïve participants. Genotypic env analysis suggests CCR5 usage in 14/18 samples and identified deviations at residues, critical for gp120/gp41 interphase and CD4 binding site broadly neutralizing antibodies in more than half of the studied URFs. V1V2 sites of immune pressure in the human RV144 vaccine study varied in more than a third of URFs. Conclusions This study identified novel mosaic patterns in URFs in Cameroon. In line with the regional predominance of CRF_02AG and the increased prevalence of clade F2, prominent CRF_02AG and F2 background patterns were observed underlying the URFs. In the context of the novel mosaic genomes, the impact of the identified accessory DRMs and Env epitope variations on treatment and immune control remains elusive. The evolving diversity of HIV‐1 URFs in Cameroon requires continuous monitoring to respond to the increasing challenges for diagnosis, antiretroviral treatment and prevention.

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Identifying Recombination Hot Spots in the HIV-1 Genome

Cited by 48 publications

References 69 publications

Characterisation of HIV-1 Molecular Epidemiology in Nigeria: Origin, Diversity, Demography and Geographic Spread

Characterisation of HIV-1 Molecular Epidemiology in Nigeria: Origin, Diversity, Demography and Geographic Spread

Estimating the in-vivo HIV template switching and recombination rate

Near full genome characterization of HIV‐1 unique recombinant forms in Cameroon reveals dominant CRF02_AG and F2 recombination patterns

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