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Soluble CD14 is independently associated with coronary calcification and extent of subclinical vascular disease in treated HIV infection

机译:在治疗的HIV感染中,可溶性CD14与冠状动脉钙化和亚临床血管疾病的程度独立相关

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Objective: To use multimodality imaging to explore the relationship of biomarkers of inflammation, T-cell activation and monocyte activation with coronary calcification and subclinical vascular disease in a population of HIV-infected patients on antiretroviral therapy (ART). Design: Cross-sectional. Methods: A panel of soluble and cellular biomarkers of inflammation and immune activation was measured in 147 HIV-infected adults on ART with HIV RNA less than 1000 copies/ml and low-density lipoprotein cholesterol (LDL-C) 130 mg/dl or less. We examined the relationship of biomarkers to coronary calcium (CAC) score and multiple ultrasound measures of subclinical vascular disease. Results: Overall, median (interquartile range, IQR) age was 46 (40-53) years; threequarters of participants were male and two-thirds African-American. Median 10-year Framingham risk score was 6%. Participants with CAC more than 0 were older, less likely to be African-American and had higher current and lower nadir CD4+ T-cell counts. Most biomarkers were similar between those with and without CAC; however, soluble CD14 was independently associated with CAC after adjustment for traditional risk factors. Among those with a CAC score of zero, T-cell activation and systemic inflammation correlated with carotid intima-media thickness and brachial hyperemic velocity, respectively. Compared with normal participants and those with CAC only, participants with increasing degrees of subclinical vascular disease had higher levels of sCD14, hs-CRP and fibrinogen (all P0.05). Conclusion: Soluble CD14 is independently associated with coronary artery calcification, and, among those with detectable calcium, predicts the extent of subclinical disease in other vascular beds. Future studies should investigate the utility of multimodality imaging to characterize vascular disease phenotypes in this population.
机译:目的:利用多模式成像技术,探讨接受抗逆转录病毒治疗(ART)的一批HIV感染患者的炎症,T细胞活化和单核细胞活化的生物标志物与冠状动脉钙化和亚临床血管疾病的关系。设计:横截面。方法:在147名HIV感染的成年人中,对HIV RNA低于1000拷贝/ ml和低密度脂蛋白胆固醇(LDL-C)130 mg / dl或以下的成年人中的一组可溶性炎症和免疫活化的生物标志物进行了测量。我们检查了生物标志物与冠状动脉钙(CAC)评分和亚临床血管疾病的多种超声测量结果之间的关系。结果:总体而言,中位(四分位间距,IQR)年龄为46(40-53)岁;四分之三的参与者是男性,三分之二的非洲裔美国人。 Framingham的10年风险中位数为6%。 CAC大于0的参与者年龄较大,非裔美国人的可能性较小,并且当前CD4 ++ T细胞计数最低且最低。有或没有CAC的大多数生物标志物相似。然而,在调整传统危险因素后,可溶性CD14与CAC独立相关。在CAC评分为零的患者中,T细胞活化和全身性炎症分别与颈动脉内膜中层厚度和肱充血速度相关。与正常参与者和仅具有CAC的参与者相比,亚临床血管疾病程度增加的参与者的sCD14,hs-CRP和纤维蛋白原水平更高(均P0.05)。结论:可溶性CD14与冠状动脉钙化独立相关,并且在可检出钙的人群中,可预测其他血管床的亚临床疾病程度。未来的研究应调查多模态成像在该人群中表征血管疾病表型的实用性。

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