艾滋病病毒感染者的亚临床心血管重塑:两个血清不一致的单卵双胞胎的多模式病例研究。

Pieter-Paul S Robbertse, Jan Steyn, Megan R Rajah, Anton F Doubell, Jean B Nachega, Philip G Herbst
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引用次数: 0

摘要

在新诊断出的艾滋病病毒感染者中,心血管异常被越来越多地发现,但亚临床病理诊断可能具有挑战性。我们对一对同卵双胞胎的心血管微妙变化进行了个案研究,这对双胞胎一个未感染 HIV,另一个最近被诊断出感染了 HIV(血清不一致)。我们假设,除非是非遗传(环境)因素在起作用,否则双胞胎之间的心血管参数应该是相似的。这些差异很可能是早期艾滋病病毒感染继发的隐性病变。一名 25 岁的女性偶然被诊断出感染了艾滋病毒,而她的未感染艾滋病毒的同卵双胞胎自出生起就与她生活在一起,她们接受了全面的心血管评估。与姐姐相比,HIV 阳性双胞胎的左心室(LV)呈球状,左心室容积较大,左心室应变、心房纵向应变峰值(PALS)降低,原生 T1 和 T2 映射值升高。感染艾滋病毒的双胞胎中,心脏生物标志物高敏心肌肌钙蛋白T和N-端proBNP以及纤维化和重塑的新型标志物galectin-3和可溶性-ST2的含量更高。鉴于这对双胞胎具有共同的环境和基因构成,这些差异很可能源于艾滋病病毒感染。我们的研究支持之前的发现,并提出了包括 PALS 在内的 HIV 相关心血管疾病的潜在筛查指标。我们有必要进一步研究 PALS 在这方面的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Subclinical cardiovascular remodelling in HIV-infection: A multimodal case study of 2 serodiscordant, monozygotic twins.

Cardiovascular abnormalities are increasingly recognised among people newly diagnosed with HIV, but subclinical pathology may be challenging to diagnose. We present a case study of subtle cardiovascular changes in identical twins, one without HIV-infection and the other recently diagnosed with HIV (serodiscordant). We hypothesise that cardiovascular parameters would be similar between the twins, unless non-genetic (environmental) factors are at play. These differences likely represent occult pathology secondary to the effects of early HIV-infection. A 25-year-old female incidentally diagnosed with HIV, and her HIV-uninfected identical twin, living with her since birth, underwent comprehensive cardiovascular assessments. The HIV-positive twin exhibited a globular left ventricle (LV), larger LV volumes, decreased LV strain, peak atrial longitudinal strain (PALS) and higher native T1 and T2 mapping values compared to her sister. Cardiac biomarkers high sensitivity cardiac troponin T and N-terminal proBNP, as well as the novel markers of fibrosis and remodelling, galectin-3 and soluble-ST2, were higher in the HIV-infected twin. Given the twins' shared environment and genetic makeup, these differences likely stem from HIV-infection. Our study supports previous findings and suggests potential screening markers for HIV-associated cardiovascular disease, including PALS. Further research is warranted to explore PALS' utility in this context.

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