HIV-1 subtype CRF01_AE and B differ in utilization of low levels of CCR5, Maraviroc susceptibility and potential N-glycosylation sites

Joshi, Anjali; Sedano, Melina J.; Punke, Erin B.; Lee, Raphael Tc; Maurer‐Stroh, Sebastian; Kaur, Parampreet; Ng, Oon Tek; Garg, Himanshu

doi:10.1016/j.virol.2017.09.026

Cited by 4 publications

(2 citation statements)

References 76 publications

(111 reference statements)

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“…A recent study found that in the Los Alamos HIV database, N301 glycan is present in as high as 99% of subtype B sequences with R5 phenotype and more than 80% of sequences with X4 phenotype. Differently, in CRF01_AE, 94% of R5 sequences and 39% of X4 sequences have the N301 glycan site (34). This again indicates that loss of the N301 glycan is an important pathway for coreceptor switch in CRF01_AE HIV-1, but is not a primary route among subtype B viruses.…”

Section: Discussionmentioning

confidence: 99%

Rapid CD4 cell loss is caused by specific CRF01_AE cluster with V3 signatures favoring CXCR4 usage

Song¹,

Feng

et al. 2018

Preprint

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1HIV-1 evolved into various genetic subtypes and circulating recombinant forms (CRFs) 3 2 in the global epidemic, with the same subtype or CRF usually having similar phenotype. 3Being one of the world's major CRFs, CRF01_AE infection was reported to associate 3 4 with higher prevalence of CXCR4 (X4) viruses and faster CD4 decline. However, the 3 5 underlying mechanisms remain unclear. We identified eight phylogenetic clusters of 3 6 CRF01_AE in China and hypothesized that they may have different phenotypes. In the 3 7 national HIV molecular epidemiology survey, we discovered that people infected by 3 8 CRF01_AE cluster 4 had significantly lower CD4 count (391 vs. 470, p < 0.0001) and 3 9higher prevalence of predicted X4-using viruses (17.1% vs. 4.4%, p < 0.0001) 4 0 compared to those infected by cluster 5. In a MSM cohort, X4-using viruses were only 4 1 isolated from sero-convertors infected by cluster 4, which associated with rapid CD4 4 2 loss within the first year of infection (141 vs. 440, p = 0.01). Using co-receptor binding 4 3 model, we identified unique V3 signatures in cluster 4 that favor CXCR4 usage. We 4 4

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Section: Discussionmentioning

confidence: 99%

Rapid CD4 cell loss is caused by specific CRF01_AE cluster with V3 signatures favoring CXCR4 usage

Song¹,

Feng

et al. 2018

Preprint

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“…Cells were fixed at day 3 post infection and images acquired using the Nikon Eclipse Ti microscope expression [18]. Our lab has extensively studied the role of CCR5 expression levels in HIV pathogenesis [19][20][21][22][23][24][25] and believe that a reduction in CCR5 levels in mono allelic KO may reduce CCR5 levels and provide a CCR5delta32 heterozygous like phenotype in patients resulting in reduced HIV pathogenesis. However, the goal of CCR5 KO should be bi allelic KO in order to achieve HIV resistance/cure as seen in the Berlin patient.…”

Section: Discussionmentioning

confidence: 99%

Combination gene therapy for HIV using a conditional suicidal gene with CCR5 knockout

Mehmetoglu-Gurbuz

Yeh

Garg

et al. 2021

Virol J

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Background Gene therapy approaches using hematopoietic stem cells to generate an HIV resistant immune system have been shown to be successful. The deletion of HIV co-receptor CCR5 remains a viable strategy although co-receptor switching to CXCR4 remains a major pitfall. To overcome this, we designed a dual gene therapy strategy that incorporates a conditional suicide gene and CCR5 knockout (KO) to overcome the limitations of CCR5 KO alone. Methods A two-vector system was designed that included an integrating lentiviral vector that expresses a HIV Tat dependent Thymidine Kinase mutant SR39 (TK-SR39) and GFP reporter gene. The second non-integrating lentiviral (NIL) vector expresses a CCR5gRNA-CRISPR/Cas9 cassette and HIV Tat protein. Results Transduction of cells sequentially with the integrating followed by the NIL vector allows for insertion of the conditional suicide gene, KO of CCR5 and transient expression of GFP to enrich the modified cells. We used this strategy to modify TZM cells and generate a cell line that was resistant to CCR5 tropic viruses while permitting infection of CXCR4 tropic viruses which could be controlled via treatment with Ganciclovir. Conclusions Our study demonstrates proof of principle that a combination gene therapy for HIV is a viable strategy and can overcome the limitation of editing CCR5 gene alone.

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The role of conventional antibodies targeting the CD4 binding site and CD4-induced epitopes in the control of HIV-1 CRF01_AE viruses

Thida

Kuwata

Maeda

et al. 2019

Biochemical and Biophysical Research Communications

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HIV-1 subtype CRF01_AE and B differ in utilization of low levels of CCR5, Maraviroc susceptibility and potential N-glycosylation sites

Cited by 4 publications

References 76 publications

Rapid CD4 cell loss is caused by specific CRF01_AE cluster with V3 signatures favoring CXCR4 usage

Rapid CD4 cell loss is caused by specific CRF01_AE cluster with V3 signatures favoring CXCR4 usage

Combination gene therapy for HIV using a conditional suicidal gene with CCR5 knockout

The role of conventional antibodies targeting the CD4 binding site and CD4-induced epitopes in the control of HIV-1 CRF01_AE viruses

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