抗逆转录病毒疗法对在 HIV-1 感染成人中观察到的表观遗传学年龄加速的影响。

Q1 Medicine Pathogens and Immunity Pub Date : 2020-10-22 eCollection Date: 2020-01-01 DOI:10.20411/pai.v5i1.376
Mary E Sehl, Tammy M Rickabaugh, Roger Shih, Otoniel Martinez-Maza, Steve Horvath, Christina M Ramirez, Beth D Jamieson
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引用次数: 0

摘要

背景:HIV-1感染与感染者外周血和大脑中与年龄相关的甲基化模式的加速有关,但HIV-1感染与治疗对所观察到的生物衰老加速的相对贡献尚未得到研究:在这项关于抗逆转录病毒疗法(ART)对表观遗传衰老模式影响的纵向研究中,我们提取了 15 名 HIV-1 感染者在三个时间点的外周血单核细胞 DNA:分别是抗逆转录病毒疗法前 6 个月至 1 年、开始抗逆转录病毒疗法后 6 个月至 12 个月以及开始抗逆转录病毒疗法后 18 个月至 24 个月。我们将这些轨迹与 15 名年龄匹配的未感染对照参与者在三个时间点的轨迹进行了比较,时间间隔相似。甲基化研究使用 Infinium 甲基化 450 阵列进行。我们研究了四种表观遗传时钟测量方法:年龄加速残差(AAR)、外在(EEAA)、表型(PEAA)和严峻(GEAA)表观遗传年龄加速。加权相关网络(WGCNA)分析用于识别高度共甲基化的CpGs群:结果:我们发现,在开始接受抗逆转录病毒疗法之前,HIV-1 感染者与未感染者相比,所有四项表观遗传学指标均显著升高(AAR 为 P0.001,EEAA 为 P=0.008,GEAA 为 P=0.012,PEAA 为 PP=0.059,GEAA 为 P=0.11),而与未感染者相比,HIV-1 感染者的 AAR 和 EEAA 仍显著升高。我们进一步研究了 HIV-1 感染者与未感染者在每个时间点的整体甲基化差异模式,发现有 14 组共甲基化 CpGs 在基线时在组间有显著差异,并且在开始抗逆转录病毒疗法后仍有差异。结论我们证实,与 HIV-1 感染相关的表观遗传学年龄加速在开始接受抗逆转录病毒疗法之前最为显著,这一观察结果在四种表观遗传学时钟测量中以及在使用 WGCNA 确定的共甲基化 CpGs 的其他组别中都是一致的。开始抗逆转录病毒疗法后,所有测量指标中的年龄加速度都部分降低,血清状态组之间的 PEAA 和 GEAA 不再有显著差异。我们的研究结果表明,今后有必要对 HIV-1 感染者的表观遗传学年龄加速与临床结果之间的联系进行研究。
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The Effects of Anti-retroviral Therapy on Epigenetic Age Acceleration Observed in HIV-1-infected Adults.

Background: HIV-1 infection is associated with acceleration of age-related methylation patterns in peripheral blood and brain of infected individuals although the relative contributions of HIV-1 infection versus its treatment to the observed accelerations in biological aging have not yet been investigated.

Methods: In this longitudinal study of the effects of antiretroviral therapy (ART) on epigenetic aging patterns, we extracted DNA from peripheral blood mononuclear cells from 15 HIV-1-infected individuals infected at three time points: 6 months-1year pre-ART, 6-12 months post-initiation of ART, and 18-24 months after initiating ART. We compared these trajectories with those of 15 age-matched uninfected control participants at three time points with similar intervals. Methylation studies were performed using the Infinium methylation 450 arrays. We examined four epigenetic clock measurements: Age acceleration residual (AAR), Extrinsic (EEAA), Phenotypic (PEAA), and Grim (GEAA) epigenetic age acceleration. Weighted correlation network (WGCNA) analysis was used to identify clusters of highly co-methylated CpGs.

Results: We found that prior to the initiation of ART all four epigenetic measures were significantly higher in HIV-1-infected individuals compared with uninfected individuals (P<0.001 for AAR, P=0.008 for EEAA, P=0.012 for GEAA, P<0.001 for PEAA using Wilcoxon rank sum tests between serostatus groups). These effects persisted after the initiation of ART, although the magnitude of these differences diminished. At 18-24 months post-ART initiation (time point 3), PEAA and GEAA were no longer significantly different between HIV-1-infected and uninfected individuals (P=0.059 for PEAA, P=0.11 for GEAA), while AAR and EEAA remained significantly higher in HIV-1-infected individuals compared with uninfected individuals. We further examined for global patterns of methylation differences between HIV-1-infected and uninfected at each time point, and found 14 groups of co-methylated CpGs that were significantly different between groups at baseline, and remained different after the initiation of ART. Conclusion: We confirm that epigenetic age acceleration associated with HIV-1 infection is most dramatic before ART initiation, and this observation is consistent across four epigenetic clock measurements, as well as in additional groups of co-methylated CpGs identified using WGCNA. Following initiation of ART, there is a partial reduction in age acceleration in all measures, with loss of any significant difference in PEAA and GEAA between serostatus groups. Our findings support the need for future studies examining for a link between epigenetic age acceleration and clinical outcomes in HIV-1-infected individuals.

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来源期刊
Pathogens and Immunity
Pathogens and Immunity Medicine-Infectious Diseases
CiteScore
10.60
自引率
0.00%
发文量
16
审稿时长
10 weeks
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