Race-specific HIV-1 disease-modifying effects associated with
            <i>CCR5</i>
            haplotypes

González, Enrique A.; Bamshad, Mike; Sato, Naoko; Mummidi, Srinivas; Dhanda, Rahul; Catano, Gabriel; Cabrera, Sonia; McBride, Megan; Cao, Xuan; Merrill, Gerald A.; O’Connell, P.; Bowden, Donald W.; Freedman, Barry I.; Anderson, Stephanie A.; Walter, Elizabeth; Evans, James S.; Stephan, Kevin; Clark, Robert A.; Tyagi, Sanjay; Ahuja, Seema S.; Dolan, Matthew J.; Ahuja, Sunil K.

doi:10.1073/pnas.96.21.12004

Cited by 237 publications

(366 citation statements)

References 23 publications

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“…Of additional interest, HIV ϩ persons with a Ϫ2459A͞A ϩ ORF⌬32͞wt diplotype demonstrated the lowest levels of plasma viremia. Furthermore, our data linking ex vivo R5 HIV susceptibility to CCR5 genotype are also consistent with additional cohort data correlating CCR5 genotype and HIV disease progression as reported by two other studies (33,35). Thus, our current ex vivo infection findings with LCs provide a plausible biologic explanation for observed epidemiologic data obtained from large cohorts of individuals regarding host genetic susceptibility to HIV infection.…”

Section: Discussionsupporting

confidence: 79%

“…4B). As four different haplotypes have been identified that contain the Ϫ2459G allele (haplotypes A-D) and three different haplotypes have been identified that contain the Ϫ2459A allele [haplotypes E, F1, and G1; excludes haplotypes containing CCR264I (F2) and ORF⌬32 (G2) (33)], it is important to note that no single Ϫ2459G haplotype was consistently associated with a low percentage of p24 ϩ LCs and no single Ϫ2459A haplotype was consistently associated with a high percentage of p24 ϩ LCs. Although significant differences in HIV infection levels in LCs among individuals who were homozygous for the wild-type ORF with either Ϫ2459A͞A,Ϫ2459A͞G, or Ϫ2459G͞G promoter genotypes were not detected, LCs isolated from Ϫ2459G͞G individuals tended to be less susceptible to HI V than LCs isolated from Ϫ2459A͞A individuals (Ϫ2459G͞G, n ϭ 13; Ϫ2459A͞A, n ϭ 15; Mann-Whitney U test, P ϭ 0.093; Fig.…”

Section: Compound Ccr5 Polymorphisms Influence R5 Hiv Infection Levelmentioning

confidence: 99%

“…Interestingly, ORF⌬32, which is known to confer protection against HIV infection, is tightly linked to the promoter Ϫ2459A allele, known to be associated with HIV disease progression (25). Although there is a growing awareness that complex polymorphic CCR5 haplotypes are associated with slower or rapid progression to AIDS (33)(34)(35)(36), less is known about how Abbreviations: LC, Langerhans cell; DC, dendritic cell; mDC, monocyte-derived DC; DC-SIGN, DC-specific ICAM-3-grabbing nonintegrin; SNP, single-nucleotide polymorphism; AZT, 3Ј-azido-3Ј-deoxythymidine; RANTES, regulated on activation normal T cell expressed and secreted.…”

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confidence: 99%

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R5 HIV productively infects Langerhans cells, and infection levels are regulated by compoundCCR5polymorphisms

Kawamura

Gulden

Sugaya

et al. 2003

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

177

163

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Langerhans cells (LCs) are suspected to be initial targets for HIV after sexual exposure (by becoming infected or by capturing virus). Here, productive R5 HIV infection of LC ex vivo and LC-mediated transmission of virus to CD4 ؉ T cells were both found to depend on CCR5. By contrast, infection of monocyte-derived dendritic cells and transfer of infection from monocyte-derived dendritic cells to CD4 ؉ T cells were mediated by CCR5-dependent as well as DCspecific ICAM-3-grabbing nonintegrin-dependent pathways. Furthermore, in 62 healthy individuals, R5 HIV infection levels in LCs ex vivo were associated with CCR5 genotype. Specifically, genotyping for ORF⌬32 revealed that LCs isolated from ORF⌬32͞wt individuals were significantly less susceptible to HIV when compared with LCs isolated from ORFwt͞wt individuals (P ‫؍‬ 0.016). Strikingly, further genetic analyses of the A-2459G CCR5 promoter polymorphism in ORF⌬32͞wt heterozygous individuals revealed that LCs isolated from ؊2459A͞G ϩ ORF⌬32͞wt individuals were markedly less susceptible to HIV than were LCs from ؊2459A͞A ϩ ORF⌬32͞wt individuals (P ‫؍‬ 0.012). Interestingly, these genetic susceptibility data in LCs parallel those of genetic susceptibility studies performed in cohorts of HIV-infected individuals. Thus, we suggest that CCR5-mediated infection of LCs, and not capture of virus by LCs, provides a biologic basis for understanding certain aspects of host genetic susceptibility to initial HIV infection.

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Section: Discussionsupporting

confidence: 79%

Section: Compound Ccr5 Polymorphisms Influence R5 Hiv Infection Levelmentioning

confidence: 99%

mentioning

confidence: 99%

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R5 HIV productively infects Langerhans cells, and infection levels are regulated by compoundCCR5polymorphisms

Kawamura

Gulden

Sugaya

et al. 2003

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

177

163

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“…Other studies have shown correlations between disease progression and the CCR2-64 I/V amino acid substitution and between CCR5 promoter haplotype/haplotype combinations (diplotype) [10,19,[23][24][25][26][27][28]. We were unable to demonstrate any relationship between these diplotypes and the in vitro phenotype; however, these additional analyses may have been limited by the small numbers of individuals in the diplotype in vitro phenotype categories observed in this study.…”

Section: Resultscontrasting

confidence: 47%

CCR5 promoter polymorphism determines macrophage CCR5 density and magnitude of HIV-1 propagation in vitro

Salkowitz

Bruse

Meyerson

et al. 2003

Clinical Immunology

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“…The errors introduced by this assumption should be very small, as RH index differences between racial groups are generally small (see Table 1 in Winkler et al). 12 However, it was recently shown that the RH indices of the haplotypes containing newly identified polymorphisms in the promoter region of CCR5 [19][20][21] are higher in African Americans than they are in European Americans. 19 Therefore, the RH index in African populations in this study is likely to be underestimated and our conclusion of high RH in Africa still stands.…”

Section: Resultsmentioning

confidence: 99%

Distribution of three HIV-1 resistance-conferring polymorphisms (SDF1-3′A, CCR2-64I, and CCR5-Δ32) in global populations

Sun

et al. 2000

Eur J Hum Genet

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Chemokine receptors (CCR5, CXCR4 and CCR2) have been shown to be important co-receptors for HIV infection. Mutations at CCR5 (CCR5-∆32), CCR2 (CCR2-64I), and stromal-derived factor SDF1 (SDF1-3'A), a primary ligand for CXCR4, are known to have protective effects against HIV-1 infection and the onset of AIDS symptoms. We studied the three-locus genotype frequency distributions in 70 worldwide populations from a sample of 2341 individuals without any known history of HIV-1 infection and AIDS symptoms. From these data, we estimated the risk of AIDS onset (relative hazard, RH) of each population. This survey shows that the substantial allele frequency differences of each of these mutations translate into an extensive variation in relative hazards for AIDS in worldwide populations. However, no evidence of natural selection against the mutant gene carriers is detected. Finally, the combined three-locus genotype data predict the highest relative hazard (RH) in South-East Asia and Africa where AIDS is known to be more prevalent. European Journal of Human Genetics (2000) 8, 975-979.

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Race-specific HIV-1 disease-modifying effects associated with CCR5 haplotypes

Cited by 237 publications

References 23 publications

R5 HIV productively infects Langerhans cells, and infection levels are regulated by compoundCCR5polymorphisms

R5 HIV productively infects Langerhans cells, and infection levels are regulated by compoundCCR5polymorphisms

CCR5 promoter polymorphism determines macrophage CCR5 density and magnitude of HIV-1 propagation in vitro

Distribution of three HIV-1 resistance-conferring polymorphisms (SDF1-3′A, CCR2-64I, and CCR5-Δ32) in global populations

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