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在感染HIV的个体中,开始基于依非韦伦的抗逆转录病毒治疗方案后高敏C反应蛋白水平的变化。

Change in high-sensitivity c-reactive protein levels following initiation of efavirenz-based antiretroviral regimens in HIV-infected individuals.

作者信息

Shikuma Cecilia M, Ribaudo Heather J, Zheng Yu, Gulick Roy M, Meyer William A, Tashima Karen T, Bastow Barbara, Kuritzkes Daniel R, Glesby Marshall J

机构信息

University of Hawaii , Honolulu, Hawaii, USA.

出版信息

AIDS Res Hum Retroviruses. 2011 May;27(5):461-8. doi: 10.1089/aid.2010.0154. Epub 2010 Nov 23.

Abstract

Elevations in C-reactive protein (CRP) are associated with increased cardiovascular disease (CVD) risk, increased HIV disease progression, and death in HIV-infected patients. Use of abacavir has been reported to increase CVD risk. We assessed the effect of virologically suppressive efavirenz (EFV)-based antiretroviral therapy on high sensitivity CRP (hsCRP) levels over a 96-week period with particular attention to the effect of gender and abacavir use. Banked sera from entry and week 96 visits of AIDS Clinical Trials Group A5095 participants were assayed for hsCRP, then analyzed by gender, abacavir randomization, and for correlation with changes in fasting metabolic parameters. Analyses of hsCRP were conducted in two phases and involved a total of 145 men and 51 women. hsCRP did not differ by gender at baseline but higher levels were seen at week 96 in women (median 6 mg/liter; Q1, Q3, 1.8, 13.8) compared to men (median 1.6 mg/liter; Q1, Q3, 0.9, 4.2, p < 0.001), with an estimated shift in hsCRP by gender of 2.5 mg/liter (95% CI 1.0, 5.1). There was no difference in hsCRP levels by abacavir use. Changes in hsCRP did not correlate with changes in insulin resistance or with changes in fasting lipids. Durably virologically suppressive therapy with EFV-based regimens did not decrease hsCRP levels over a 96-week period. hsCRP levels increased significantly only in women. Randomization to abacavir had no effect on changes in hsCRP levels. Changes in hsCRP levels did not correlate with changes in fasting metabolic parameters.

摘要

C反应蛋白(CRP)升高与心血管疾病(CVD)风险增加、HIV疾病进展加快以及HIV感染患者死亡相关。据报道,使用阿巴卡韦会增加CVD风险。我们评估了基于病毒学抑制的依非韦伦(EFV)抗逆转录病毒疗法在96周期间对高敏CRP(hsCRP)水平的影响,特别关注性别和阿巴卡韦使用的影响。对艾滋病临床试验组A5095参与者入组时和第96周访视时的储存血清进行hsCRP检测,然后按性别、阿巴卡韦随机分组情况进行分析,并分析其与空腹代谢参数变化的相关性。hsCRP分析分两个阶段进行,共涉及145名男性和51名女性。hsCRP在基线时无性别差异,但在第96周时,女性(中位数6毫克/升;四分位间距Q1、Q3分别为1.8、13.8)的hsCRP水平高于男性(中位数1.6毫克/升;Q1、Q3分别为0.9、4.2,p<0.001),估计性别导致的hsCRP水平变化为2.5毫克/升(95%置信区间1.0、5.1)。使用阿巴卡韦与否,hsCRP水平无差异。hsCRP的变化与胰岛素抵抗的变化或空腹血脂的变化无关。基于EFV的方案进行持久的病毒学抑制治疗在96周期间并未降低hsCRP水平。hsCRP水平仅在女性中显著升高。随机分组至阿巴卡韦对hsCRP水平变化无影响。hsCRP水平变化与空腹代谢参数变化无关。

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