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将先前接受治疗的HIV感染患者换用含马拉维若的无核苷类逆转录酶抑制剂双药治疗方案后内皮功能的改善

Improvement of endothelial function after switching previously treated HIV-infected patients to an NRTI-sparing bitherapy with maraviroc.

作者信息

Bernal Enrique, Verdú Jose Miguel Gomez, Vera Francisco, Martinez Onofre, Bravo Joaquin, Galera Carlos, Muñoz Angeles, Garcia Eva, Serrano Jose, Perez Ana, Vera Carmen, Marín Irene, Cano Alfredo

机构信息

Infectious Disease Unit, Reina Sofia Hospital, Murcia, Spain.

Infectious Disease Unit, Santa Lucia, Cartagena, Spain.

出版信息

J Int AIDS Soc. 2014 Nov 2;17(4 Suppl 3):19726. doi: 10.7448/IAS.17.4.19726. eCollection 2014.

Abstract

INTRODUCTION

Nucleoside reverse transcriptase inhibitor (NRTI) is associated with endothelial dysfunction and proinflammatory effects. Maraviroc (MVC) is an antagonist of CCR5 receptor. CCR5 is the receptor of RANTES (Regulated on Activation, Normal T Cell Expressed and Secreted), a mediator of chronic inflammation and endothelial function. Our aim was to evaluate the maintenance of viral suppression and improvement of endothelial function in virologically suppressed HIV-infected patients switched to an NRTI-sparing combined antiretroviral therapy (cART) with MVC.

MATERIALS AND METHODS

This observational, non-interventional, multicenter study was performed at the Infectious Diseases Service of Santa Lucia, Morales Meseguer, Virgen de la Arrixaca and Reina Sofía University Hospital (Murcia, Spain). The selection criteria were to be asymptomatic on a regimen with undetectable viral load (<50 HIV-RNA copies/mL) for at least six months, no previous treatment with R5 antagonists, no evidence of previous protease inhibitor (PI) failure and available R5 tropism test. Twenty-one HIV-infected patients were selected after the treatment regimen was changed to Maraviroc 150 mg/once daily plus ritonavir-boosted PI therapy. Endothelial function was prospectively evaluated through flow-mediated dilatation (FMD) of the brachial artery at baseline and at weeks 24.

RESULTS

We included 21 patients on treatment with PI in combination with 2 NRTI. The mean cART exposition was 133±68.9 months. Fourteen (66.6%) were males, aged 49±9 years, 15 (71.4%) smokers, 4 (19.04%) family history of coronary heart disease, 1 (5.76%) type 2 diabetes and 3 (14.28%) hypertensive, mean total cholesterol was 185.5±35 mg/dL, c-LDL 100.2±37 mg/dL, tryglicerides 170.42±92.03 mg/dL, cHDL 52.6±15.5 mg/dL, CD4 779,5±383.28 cells/mL, nadir CD4 187,96±96 cells/mL. After 24 weeks of follow-up of a switch to an NRTI-sparing regimen, 95.2% of HIV-patients on viral suppressive cART maintained viral suppression and CD4+ T cell count. This cART switch improve endothelial function in patients with lower baseline FMD levels after 24 weeks (baseline FMD -1.19±4.84 % to 24 weeks FMD 11.32±7.27%; p=0.002).

CONCLUSIONS

The results of our study show that a switch to an NRTI-sparing bi-therapy with MVC improves endothelial function and maintained the immune-virologic efficacy. This regimen emphasizes the needs for further clinical studies to associate these achievements with the incidence of non-AIDS-defining illnesses.

摘要

引言

核苷类逆转录酶抑制剂(NRTI)与内皮功能障碍和促炎作用相关。马拉维罗(MVC)是CCR5受体拮抗剂。CCR5是调节激活正常T细胞表达和分泌因子(RANTES)的受体,RANTES是慢性炎症和内皮功能的介质。我们的目的是评估转换为含MVC的无NRTI联合抗逆转录病毒疗法(cART)的病毒学抑制的HIV感染患者的病毒抑制维持情况和内皮功能改善情况。

材料与方法

本观察性、非干预性、多中心研究在西班牙穆尔西亚的圣卢西亚传染病科、莫拉莱斯·梅塞格尔、阿瑞萨卡圣母大学医院和雷纳·索菲亚大学医院进行。入选标准为在病毒载量不可检测(<50拷贝/mL HIV-RNA)的方案下无症状至少6个月,既往未接受过R5拮抗剂治疗,无既往蛋白酶抑制剂(PI)治疗失败的证据且有可用的R5嗜性检测。在治疗方案改为马拉维罗150 mg/每日一次加利托那韦增强的PI治疗后,选择了21例HIV感染患者。在基线和第24周通过肱动脉血流介导的血管舒张(FMD)前瞻性评估内皮功能。

结果

我们纳入了21例接受PI联合2种NRTI治疗的患者。cART平均治疗时间为133±68.9个月。14例(66.6%)为男性,年龄49±9岁,15例(71.4%)吸烟,4例(19.04%)有冠心病家族史,1例(5.76%)为2型糖尿病,3例(14.28%)高血压,平均总胆固醇为185.5±35 mg/dL,c-LDL为100.2±37 mg/dL,甘油三酯为170.42±92.03 mg/dL,cHDL为52.6±15.5 mg/dL,CD4为779.5±383.28细胞/mL,最低CD4为187.96±96细胞/mL。在转换为无NRTI方案的24周随访后,95.2%接受病毒抑制性cART的HIV患者维持了病毒抑制和CD4+T细胞计数。这种cART转换在24周后改善了基线FMD水平较低患者的内皮功能(基线FMD -1.19±4.84%至24周FMD 11.32±7.27%;p = 0.002)。

结论

我们的研究结果表明,转换为含MVC的无NRTI双药疗法可改善内皮功能并维持免疫病毒学疗效。该方案强调需要进一步的临床研究将这些成果与非艾滋病定义疾病的发生率联系起来。

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