Maria Raffaella Petrara, Elena Ruffoni, Francesco Carmona, Ilaria Cavallari, Sandra Zampieri, Marzia Morello, Paola Del Bianco, Osvalda Rampon, Nicola Cotugno, Paolo Palma, Paolo Rossi, Carlo Giaquinto, Silvia Giunco, Anita De Rossi
{"title":"艾滋病病毒库与过早衰老:感染围产期艾滋病病毒的青少年和年轻成人患衰老相关疾病的风险因素。","authors":"Maria Raffaella Petrara, Elena Ruffoni, Francesco Carmona, Ilaria Cavallari, Sandra Zampieri, Marzia Morello, Paola Del Bianco, Osvalda Rampon, Nicola Cotugno, Paolo Palma, Paolo Rossi, Carlo Giaquinto, Silvia Giunco, Anita De Rossi","doi":"10.1371/journal.ppat.1012547","DOIUrl":null,"url":null,"abstract":"<p><p>Despite receiving antiretroviral therapy (ART), an increasing number of adolescents and young adults with perinatally acquired HIV (PHIVAYA) are at risk of developing premature senescence and aging-associated illnesses, including cancer. Given this concern, it is crucial to assess aging biomarkers and their correlation with the HIV reservoir in order to comprehensively characterize and monitor these individuals. Fifty-five PHIVAYA (median age: 23, interquartile range [IQR]: 20-27 years, and 21 [18-23] years on ART at the time of study sampling) were studied along with 23 age-matched healthy controls. The PHIVAYA exhibited significantly higher percentages of activated, senescent, exhausted CD4 and CD8 T cells, shorter telomeres, reduced thymic output, and higher levels of circulating inflammatory markers (PAMPs, DAMPs, and pro-inflammatory cytokines IL-6, IL-8, and TNFα) as well as denervation biomarkers (neural cell adhesion molecule 1 [NCAM1] and C-terminal Agrin fragment [CAF]), compared to controls. HIV-DNA levels positively correlated with activated, senescent, exhausted CD4 and CD8 T cells, circulating biomarkers levels, and inversely with regulatory T and B cells and telomere length. According to their viremia over time, PHIVAYA were subgrouped into 14 Not Suppressed (NS)-PHIVAYA and 41 Suppressed (S)-PHIVAYA, of whom 6 who initiated ART within one year of age and maintained sustained viral suppression overtime were defined as Early Suppressed (ES)-PHIVAYA and the other 35 as Late Suppressed (LS)-PHIVAYA. ES-PHIVAYA exhibited significantly lower HIV-DNA reservoir, decreased percentages of senescent and exhausted CD4 and CD8 T cells, reduced levels of circulating inflammatory and denervation biomarkers, but longer telomere compared to LS- and NS-PHIVAYA. They differed significantly from healthy controls only in a few markers, including higher percentages of regulatory T and B cells, and higher levels of DAMPs. Overall, these results underscore the importance of initiating ART early and maintaining viral suppression to limit the establishment of the viral reservoir and to counteract immune and cellular premature aging. 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Given this concern, it is crucial to assess aging biomarkers and their correlation with the HIV reservoir in order to comprehensively characterize and monitor these individuals. Fifty-five PHIVAYA (median age: 23, interquartile range [IQR]: 20-27 years, and 21 [18-23] years on ART at the time of study sampling) were studied along with 23 age-matched healthy controls. The PHIVAYA exhibited significantly higher percentages of activated, senescent, exhausted CD4 and CD8 T cells, shorter telomeres, reduced thymic output, and higher levels of circulating inflammatory markers (PAMPs, DAMPs, and pro-inflammatory cytokines IL-6, IL-8, and TNFα) as well as denervation biomarkers (neural cell adhesion molecule 1 [NCAM1] and C-terminal Agrin fragment [CAF]), compared to controls. HIV-DNA levels positively correlated with activated, senescent, exhausted CD4 and CD8 T cells, circulating biomarkers levels, and inversely with regulatory T and B cells and telomere length. According to their viremia over time, PHIVAYA were subgrouped into 14 Not Suppressed (NS)-PHIVAYA and 41 Suppressed (S)-PHIVAYA, of whom 6 who initiated ART within one year of age and maintained sustained viral suppression overtime were defined as Early Suppressed (ES)-PHIVAYA and the other 35 as Late Suppressed (LS)-PHIVAYA. ES-PHIVAYA exhibited significantly lower HIV-DNA reservoir, decreased percentages of senescent and exhausted CD4 and CD8 T cells, reduced levels of circulating inflammatory and denervation biomarkers, but longer telomere compared to LS- and NS-PHIVAYA. They differed significantly from healthy controls only in a few markers, including higher percentages of regulatory T and B cells, and higher levels of DAMPs. Overall, these results underscore the importance of initiating ART early and maintaining viral suppression to limit the establishment of the viral reservoir and to counteract immune and cellular premature aging. 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引用次数: 0
摘要
尽管接受了抗逆转录病毒疗法(ART),但越来越多的围产期感染艾滋病病毒(PHIVAYA)的青少年和年轻成年人面临着过早衰老和衰老相关疾病(包括癌症)的风险。有鉴于此,评估衰老生物标志物及其与艾滋病病毒库的相关性对于全面描述和监测这些人至关重要。研究人员对 55 名 PHIVAYA(中位年龄:23 岁,四分位数间距 [IQR]:20-27 岁,研究取样时接受抗逆转录病毒疗法 21 [18-23] 年)和 23 名年龄匹配的健康对照者进行了研究。与对照组相比,PHIVAYA 组的 CD4 和 CD8 T 细胞活化、衰老、衰竭的比例明显更高,端粒更短,胸腺输出量减少,循环炎症标志物(PAMPs、DAMPs 和促炎症细胞因子 IL-6、IL-8 和 TNFα)以及去势生物标志物(神经细胞粘附分子 1 [NCAM1] 和 C 端 Agrin 片段 [CAF])水平更高。HIV-DNA 水平与活化、衰老、衰竭的 CD4 和 CD8 T 细胞、循环生物标志物水平呈正相关,与调节性 T 细胞和 B 细胞以及端粒长度呈反相关。根据病毒血症的时间变化,PHIVAYA 被分为 14 个未被抑制 (NS)-PHIVAYA 和 41 个被抑制 (S)-PHIVAYA 组,其中 6 个在一岁内开始接受抗逆转录病毒疗法并在一段时间内保持持续病毒抑制的被定义为早期被抑制 (ES)-PHIVAYA 组,另外 35 个被定义为晚期被抑制 (LS)-PHIVAYA 组。与LS-和NS-PHIVAYA相比,ES-PHIVAYA的HIV-DNA储存量明显降低,衰老和衰竭的CD4和CD8 T细胞比例下降,循环炎症和变性生物标志物水平降低,但端粒更长。与健康对照组相比,他们仅在少数标记物上存在明显差异,包括调节性 T 细胞和 B 细胞的比例较高,以及 DAMPs 水平较高。总之,这些结果强调了尽早开始抗逆转录病毒疗法并保持病毒抑制以限制病毒库的建立并抵御免疫和细胞早衰的重要性。这些研究结果还提出了对早衰和老年相关疾病高危人群进行微创监测的新方法。
HIV reservoir and premature aging: risk factors for aging-associated illnesses in adolescents and young adults with perinatally acquired HIV.
Despite receiving antiretroviral therapy (ART), an increasing number of adolescents and young adults with perinatally acquired HIV (PHIVAYA) are at risk of developing premature senescence and aging-associated illnesses, including cancer. Given this concern, it is crucial to assess aging biomarkers and their correlation with the HIV reservoir in order to comprehensively characterize and monitor these individuals. Fifty-five PHIVAYA (median age: 23, interquartile range [IQR]: 20-27 years, and 21 [18-23] years on ART at the time of study sampling) were studied along with 23 age-matched healthy controls. The PHIVAYA exhibited significantly higher percentages of activated, senescent, exhausted CD4 and CD8 T cells, shorter telomeres, reduced thymic output, and higher levels of circulating inflammatory markers (PAMPs, DAMPs, and pro-inflammatory cytokines IL-6, IL-8, and TNFα) as well as denervation biomarkers (neural cell adhesion molecule 1 [NCAM1] and C-terminal Agrin fragment [CAF]), compared to controls. HIV-DNA levels positively correlated with activated, senescent, exhausted CD4 and CD8 T cells, circulating biomarkers levels, and inversely with regulatory T and B cells and telomere length. According to their viremia over time, PHIVAYA were subgrouped into 14 Not Suppressed (NS)-PHIVAYA and 41 Suppressed (S)-PHIVAYA, of whom 6 who initiated ART within one year of age and maintained sustained viral suppression overtime were defined as Early Suppressed (ES)-PHIVAYA and the other 35 as Late Suppressed (LS)-PHIVAYA. ES-PHIVAYA exhibited significantly lower HIV-DNA reservoir, decreased percentages of senescent and exhausted CD4 and CD8 T cells, reduced levels of circulating inflammatory and denervation biomarkers, but longer telomere compared to LS- and NS-PHIVAYA. They differed significantly from healthy controls only in a few markers, including higher percentages of regulatory T and B cells, and higher levels of DAMPs. Overall, these results underscore the importance of initiating ART early and maintaining viral suppression to limit the establishment of the viral reservoir and to counteract immune and cellular premature aging. These findings also suggest new approaches for minimally invasive monitoring of individuals at high risk of developing premature aging and age-related illnesses.
期刊介绍:
Bacteria, fungi, parasites, prions and viruses cause a plethora of diseases that have important medical, agricultural, and economic consequences. Moreover, the study of microbes continues to provide novel insights into such fundamental processes as the molecular basis of cellular and organismal function.