趋化因子受体与趋化因子基因多态性在HIV/AIDS中的新型遗传关联及基因-基因相互作用
Novel genetic associations and gene-gene interactions of chemokine receptor and chemokine genetic polymorphisms in HIV/AIDS.
作者信息
Valverde-Villegas Jacqueline M, de Medeiros Rúbia M, de Andrade Karine P, Jacovas Vanessa C, Dos Santos Breno R, Simon Daniel, de Matos Almeida Sabrina E, Chies José A B
机构信息
aDepartamento de Genética e Programa de Pós-graduação em Genética e Biologia Molecular da Universidade Federal do Rio Grande do Sul (PPGBM) bFundação Estadual de Produção e Pesquisa em Saúde (FEPPS) cServiço de Infectologia, Grupo Hospitalar Nossa Senhora da Conceição (GHC), Porto Alegre dUniversidade Luterana do Brasil (ULBRA), Canoas eInstituto de Ciências da Saúde, Universidade Feevale (FEEVALE), Novo Hamburgo, Rio Grande do Sul, Brazil.
出版信息
AIDS. 2017 Jun 1;31(9):1235-1243. doi: 10.1097/QAD.0000000000001491.
OBJECTIVE
To investigate the influence of candidate polymorphisms on chemokine receptor/ligand genes on HIV infection and AIDS progression (HIV/AIDS).
DESIGN
Fifteen polymorphisms of the CCR3, CCR4, CCR5, CCR6, CCR8, CXCR3, CXCR6, CCL20, CCL22 and CXCL10 genes were analysed in 206 HIV-positive patients classified as rapid progressors (n = 40), or nonrapid progressors (n = 166), and in 294 HIV-seronegative patients.
METHODS
The polymorphisms were genotyped using minisequencing. Genetic models were tested using binomial logistic regression; nonparametric multifactor dimensionality reduction (MDR) was used to detect gene-gene interactions.
RESULTS
The CCR3 rs3091250 [TT, adjusted odds ratio (AOR): 2.147, 95% confidence interval (CI) 1.076-4.287, P = 0.030], CCR8 rs2853699 (GC/CC, AOR: 1.577, 95% CI 1.049-2.371, P = 0.029), CXCL10 rs56061981 (CT/TT, AOR: 1.819, 95% CI 1.074-3.081, P = 0.026) and CCL22 rs4359426 (CA/AA, AOR: 1.887, 95% CI 1.021-3.487, P = 0.043) polymorphisms were associated with susceptibility to HIV infection. The CCL20 rs13034664 (CC, OR: 0.214, 95% CI 0.063-0.730, P = 0.014) and CCL22 rs4359426 (CA/AA, OR: 2.685, 95% CI 1.128-6.392, P = 0.026) variants were associated with rapid progression to AIDS. In MDR analyses revealed that the CXCL10 rs56061981 and CCL22 rs4359426 combination was the best model, with 57% accuracy (P = 0.008) for predicting susceptibility to HIV infection.
CONCLUSION
Our results provide new insights into the influence of candidate chemokine receptor/ligand polymorphisms and significant evidence for gene-gene interactions on HIV/AIDS susceptibility.
目的
研究趋化因子受体/配体基因的候选多态性对HIV感染及艾滋病进展(HIV/AIDS)的影响。
设计
对206例HIV阳性患者(分为快速进展者40例,非快速进展者166例)及294例HIV血清阴性患者,分析CCR3、CCR4、CCR5、CCR6、CCR8、CXCR3、CXCR6、CCL20、CCL22和CXCL10基因的15个多态性。
方法
采用微测序法对多态性进行基因分型。使用二项逻辑回归检验遗传模型;采用非参数多因素降维法(MDR)检测基因-基因相互作用。
结果
CCR3 rs3091250[TT,校正比值比(AOR):2.147,95%置信区间(CI)1.076 - 4.287,P = 0.030]、CCR8 rs2853699(GC/CC,AOR:1.577,95%CI 1.049 - 2.371,P = 0.029)、CXCL10 rs56061981(CT/TT,AOR:1.819,95%CI 1.074 - 3.081,P = 0.026)和CCL22 rs4359426(CA/AA,AOR:1.887,95%CI 1.021 - 3.487,P = 0.043)多态性与HIV感染易感性相关。CCL20 rs13034664(CC,OR:0.214,95%CI 0.063 - 0.730,P = 0.014)和CCL22 rs4359426(CA/AA,OR:2.685,95%CI 1.128 - 6.392,P = 0.026)变异与快速进展至艾滋病相关。MDR分析显示,CXCL10 rs56061981和CCL22 rs4359426组合是预测HIV感染易感性的最佳模型,准确率为57%(P = 0.008)。
结论
我们的结果为候选趋化因子受体/配体多态性的影响提供了新见解,并为基因-基因相互作用对HIV/AIDS易感性的影响提供了重要证据。
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