Impact of polymorphisms in the HCP5 and HLA-C, and ZNRD1 genes on HIV viral load

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Impact of polymorphisms in the HCP5 and HLA-C, and ZNRD1 genes on HIV viral load. / Thørner, Lise Wegner; Erikstrup, Christian; Harritshøj, Lene Holm; Larsen, Margit Hørup; Kronborg, Gitte; Pedersen, Court; Larsen, Carsten Schade; Pedersen, Gitte; Gerstoft, Jan; Obel, Niels; Ullum, Henrik.

I: Infection, Genetics and Evolution, Bind 41, 07.2016, s. 185-190.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

Thørner, LW, Erikstrup, C, Harritshøj, LH, Larsen, MH, Kronborg, G, Pedersen, C, Larsen, CS, Pedersen, G, Gerstoft, J, Obel, N & Ullum, H 2016, 'Impact of polymorphisms in the HCP5 and HLA-C, and ZNRD1 genes on HIV viral load', Infection, Genetics and Evolution, bind 41, s. 185-190. https://doi.org/10.1016/j.meegid.2016.03.037

APA

Thørner, L. W., Erikstrup, C., Harritshøj, L. H., Larsen, M. H., Kronborg, G., Pedersen, C., Larsen, C. S., Pedersen, G., Gerstoft, J., Obel, N., & Ullum, H. (2016). Impact of polymorphisms in the HCP5 and HLA-C, and ZNRD1 genes on HIV viral load. Infection, Genetics and Evolution, 41, 185-190. https://doi.org/10.1016/j.meegid.2016.03.037

Vancouver

Thørner LW, Erikstrup C, Harritshøj LH, Larsen MH, Kronborg G, Pedersen C o.a. Impact of polymorphisms in the HCP5 and HLA-C, and ZNRD1 genes on HIV viral load. Infection, Genetics and Evolution. 2016 jul.;41:185-190. https://doi.org/10.1016/j.meegid.2016.03.037

Author

Thørner, Lise Wegner ; Erikstrup, Christian ; Harritshøj, Lene Holm ; Larsen, Margit Hørup ; Kronborg, Gitte ; Pedersen, Court ; Larsen, Carsten Schade ; Pedersen, Gitte ; Gerstoft, Jan ; Obel, Niels ; Ullum, Henrik. / Impact of polymorphisms in the HCP5 and HLA-C, and ZNRD1 genes on HIV viral load. I: Infection, Genetics and Evolution. 2016 ; Bind 41. s. 185-190.

Bibtex

@article{24733d21bd994790917d5fc69be11371,
title = "Impact of polymorphisms in the HCP5 and HLA-C, and ZNRD1 genes on HIV viral load",
abstract = "AIMS: Single nucleotide polymorphisms (SNPs) in the human leucocyte antigen (HLA) complex P5 (HCP5), HLA-C, and near the zinc ribbon domain containing 1 (ZNRD1) have been shown to influence viral load (VL) set point in HIV-infected individuals with a known seroconversion onset. We aimed to determine the influence of HCP5 rs2395029, HLA-C rs9264942, and ZNRD1 rs3869068 on VL in antiretroviral-na{\"i}ve individuals and on time to the first VL<51 copies/ml and on CD4(+) T-cell recovery after initiation of combination antiretroviral therapy (cART).MATERIAL AND METHODS: We genotyped the rs2395029 (A>C), rs9264942 (T>C), and rs3869068 (C>T) SNPs in 1897 Caucasians from The Danish HIV Cohort Study - a prospective, nationwide, population-based study of HIV-infected individuals in Denmark. General linear models evaluated the effect of SNPs on VL in antiretroviral-na{\"i}ve individuals 0-18months after diagnosis and on CD4(+) T-cell recovery during cART. Cox proportional hazard regression analysis assessed the association with time to first VL<51 copies/ml. All models were assuming additive genetic effects.RESULTS: The rs2395029, rs9264942, and rs3869068 minor alleles were associated with lower VL in antiretroviral-na{\"i}ve individuals (rs2395029: [mean VL (copies/ml)], A/A: 70,795 [61,660-79,433], A/C: 33,884 [19,498-58,884], P=0.002; rs9264942: TT: 81,283 [67,608-97,724], T/C: 63,096 [54,954-75,858], CC: 38,905 [25,119-58,884], P<0.0001; rs3869068, CC: 72,444 [63,096-83,176], C/T: 45,709 [33,113-64,565], TT: 58,884 [20,417-169,824], P=0.01). Moreover, the C-alleles of rs2395029 and rs9264942 were associated with shorter time to VL<51 copies/ml: (HR [95% confidence interval], 1.67 [1.09-1.72], P=0.008; 1.16 [1.06-1.28], P=0.002; 1.30 [1.08-1.53], P=0.005, respectively, adjusted for last VL before cART). None of the SNPs predicted CD4(+) T-cell recovery during cART.CONCLUSIONS: The minor alleles of rs2395029, rs9264942, and rs3689068 associate with lower VL among antiretroviral-na{\"i}ve individuals and with shorter time to first VL<51copies/ml during cART even after adjustment for VL before cART.",
author = "Th{\o}rner, {Lise Wegner} and Christian Erikstrup and Harritsh{\o}j, {Lene Holm} and Larsen, {Margit H{\o}rup} and Gitte Kronborg and Court Pedersen and Larsen, {Carsten Schade} and Gitte Pedersen and Jan Gerstoft and Niels Obel and Henrik Ullum",
note = "Copyright {\textcopyright} 2016 Elsevier B.V. All rights reserved.",
year = "2016",
month = jul,
doi = "10.1016/j.meegid.2016.03.037",
language = "English",
volume = "41",
pages = "185--190",
journal = "Infection, Genetics and Evolution",
issn = "1567-1348",
publisher = "Elsevier",

}

RIS

TY - JOUR

T1 - Impact of polymorphisms in the HCP5 and HLA-C, and ZNRD1 genes on HIV viral load

AU - Thørner, Lise Wegner

AU - Erikstrup, Christian

AU - Harritshøj, Lene Holm

AU - Larsen, Margit Hørup

AU - Kronborg, Gitte

AU - Pedersen, Court

AU - Larsen, Carsten Schade

AU - Pedersen, Gitte

AU - Gerstoft, Jan

AU - Obel, Niels

AU - Ullum, Henrik

N1 - Copyright © 2016 Elsevier B.V. All rights reserved.

PY - 2016/7

Y1 - 2016/7

N2 - AIMS: Single nucleotide polymorphisms (SNPs) in the human leucocyte antigen (HLA) complex P5 (HCP5), HLA-C, and near the zinc ribbon domain containing 1 (ZNRD1) have been shown to influence viral load (VL) set point in HIV-infected individuals with a known seroconversion onset. We aimed to determine the influence of HCP5 rs2395029, HLA-C rs9264942, and ZNRD1 rs3869068 on VL in antiretroviral-naïve individuals and on time to the first VL<51 copies/ml and on CD4(+) T-cell recovery after initiation of combination antiretroviral therapy (cART).MATERIAL AND METHODS: We genotyped the rs2395029 (A>C), rs9264942 (T>C), and rs3869068 (C>T) SNPs in 1897 Caucasians from The Danish HIV Cohort Study - a prospective, nationwide, population-based study of HIV-infected individuals in Denmark. General linear models evaluated the effect of SNPs on VL in antiretroviral-naïve individuals 0-18months after diagnosis and on CD4(+) T-cell recovery during cART. Cox proportional hazard regression analysis assessed the association with time to first VL<51 copies/ml. All models were assuming additive genetic effects.RESULTS: The rs2395029, rs9264942, and rs3869068 minor alleles were associated with lower VL in antiretroviral-naïve individuals (rs2395029: [mean VL (copies/ml)], A/A: 70,795 [61,660-79,433], A/C: 33,884 [19,498-58,884], P=0.002; rs9264942: TT: 81,283 [67,608-97,724], T/C: 63,096 [54,954-75,858], CC: 38,905 [25,119-58,884], P<0.0001; rs3869068, CC: 72,444 [63,096-83,176], C/T: 45,709 [33,113-64,565], TT: 58,884 [20,417-169,824], P=0.01). Moreover, the C-alleles of rs2395029 and rs9264942 were associated with shorter time to VL<51 copies/ml: (HR [95% confidence interval], 1.67 [1.09-1.72], P=0.008; 1.16 [1.06-1.28], P=0.002; 1.30 [1.08-1.53], P=0.005, respectively, adjusted for last VL before cART). None of the SNPs predicted CD4(+) T-cell recovery during cART.CONCLUSIONS: The minor alleles of rs2395029, rs9264942, and rs3689068 associate with lower VL among antiretroviral-naïve individuals and with shorter time to first VL<51copies/ml during cART even after adjustment for VL before cART.

AB - AIMS: Single nucleotide polymorphisms (SNPs) in the human leucocyte antigen (HLA) complex P5 (HCP5), HLA-C, and near the zinc ribbon domain containing 1 (ZNRD1) have been shown to influence viral load (VL) set point in HIV-infected individuals with a known seroconversion onset. We aimed to determine the influence of HCP5 rs2395029, HLA-C rs9264942, and ZNRD1 rs3869068 on VL in antiretroviral-naïve individuals and on time to the first VL<51 copies/ml and on CD4(+) T-cell recovery after initiation of combination antiretroviral therapy (cART).MATERIAL AND METHODS: We genotyped the rs2395029 (A>C), rs9264942 (T>C), and rs3869068 (C>T) SNPs in 1897 Caucasians from The Danish HIV Cohort Study - a prospective, nationwide, population-based study of HIV-infected individuals in Denmark. General linear models evaluated the effect of SNPs on VL in antiretroviral-naïve individuals 0-18months after diagnosis and on CD4(+) T-cell recovery during cART. Cox proportional hazard regression analysis assessed the association with time to first VL<51 copies/ml. All models were assuming additive genetic effects.RESULTS: The rs2395029, rs9264942, and rs3869068 minor alleles were associated with lower VL in antiretroviral-naïve individuals (rs2395029: [mean VL (copies/ml)], A/A: 70,795 [61,660-79,433], A/C: 33,884 [19,498-58,884], P=0.002; rs9264942: TT: 81,283 [67,608-97,724], T/C: 63,096 [54,954-75,858], CC: 38,905 [25,119-58,884], P<0.0001; rs3869068, CC: 72,444 [63,096-83,176], C/T: 45,709 [33,113-64,565], TT: 58,884 [20,417-169,824], P=0.01). Moreover, the C-alleles of rs2395029 and rs9264942 were associated with shorter time to VL<51 copies/ml: (HR [95% confidence interval], 1.67 [1.09-1.72], P=0.008; 1.16 [1.06-1.28], P=0.002; 1.30 [1.08-1.53], P=0.005, respectively, adjusted for last VL before cART). None of the SNPs predicted CD4(+) T-cell recovery during cART.CONCLUSIONS: The minor alleles of rs2395029, rs9264942, and rs3689068 associate with lower VL among antiretroviral-naïve individuals and with shorter time to first VL<51copies/ml during cART even after adjustment for VL before cART.

U2 - 10.1016/j.meegid.2016.03.037

DO - 10.1016/j.meegid.2016.03.037

M3 - Journal article

C2 - 27083073

VL - 41

SP - 185

EP - 190

JO - Infection, Genetics and Evolution

JF - Infection, Genetics and Evolution

SN - 1567-1348

ER -

ID: 176835865