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HIV Med. 2013 Apr;14(4):217-25. doi: 10.1111/j.1468-1293.2012.01054.x. Epub 2012 Oct 4.
2
Toxicity associated with stavudine dose reduction from 40 to 30 mg in first-line antiretroviral therapy.与一线抗逆转录病毒治疗中从 40 毫克减少至 30 毫克司他夫定剂量相关的毒性。
PLoS One. 2011;6(11):e28112. doi: 10.1371/journal.pone.0028112. Epub 2011 Nov 21.
3
HIV neuropathy in South Africans: frequency, characteristics, and risk factors.南非的 HIV 神经病变:频率、特征和危险因素。
Muscle Nerve. 2010 May;41(5):599-606. doi: 10.1002/mus.21535.
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Symptomatic hyperlactataemia in adults on antiretroviral therapy: a single-centre experience.接受抗逆转录病毒治疗的成人患者出现症状性高乳酸血症:单中心经验
S Afr Med J. 2008 Oct;98(10):795-800.
5
Safety of stavudine in the treatment of HIV infection with a special focus on resource-limited settings.司他夫定治疗HIV感染的安全性,特别关注资源有限的环境。
Expert Opin Drug Saf. 2008 May;7(3):283-93. doi: 10.1517/14740338.7.3.283.
6
Effect of reducing the dose of stavudine on body composition, bone density, and markers of mitochondrial toxicity in HIV-infected subjects: a randomized, controlled study.降低司他夫定剂量对HIV感染受试者身体成分、骨密度及线粒体毒性标志物的影响:一项随机对照研究
Clin Infect Dis. 2008 Apr 15;46(8):1290-6. doi: 10.1086/529384.
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Changes in lipid profile over 24 months among adults on first-line highly active antiretroviral therapy in the home-based AIDS care program in rural Uganda.乌干达农村家庭艾滋病护理项目中接受一线高效抗逆转录病毒治疗的成年人在24个月内的血脂变化情况。
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Incidence and risk factors for new-onset diabetes in HIV-infected patients: the Data Collection on Adverse Events of Anti-HIV Drugs (D:A:D) study.HIV感染患者新发糖尿病的发病率及危险因素:抗HIV药物不良事件数据收集(D:A:D)研究
Diabetes Care. 2008 Jun;31(6):1224-9. doi: 10.2337/dc07-2013. Epub 2008 Feb 11.
9
The impact of reducing stavudine dose versus switching to tenofovir on plasma lipids, body composition and mitochondrial function in HIV-infected patients.在HIV感染患者中,与换用替诺福韦相比,降低司他夫定剂量对血脂、身体成分和线粒体功能的影响。
Antivir Ther. 2007;12(3):407-15.
10
Systematic review of clinical trials evaluating low doses of stavudine as part of antiretroviral treatment.评估低剂量司他夫定作为抗逆转录病毒治疗一部分的临床试验的系统评价。
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低剂量与高剂量司他夫定治疗HIV感染患者的比较。

Low dose versus high dose stavudine for treating people with HIV infection.

作者信息

Magula Nombulelo, Dedicoat Martin

机构信息

Nelson R Mandela School of Medicine, Durban, KwaZulu-Natal, South Africa.

出版信息

Cochrane Database Syst Rev. 2015 Jan 28;1(1):CD007497. doi: 10.1002/14651858.CD007497.pub2.

DOI:10.1002/14651858.CD007497.pub2
PMID:25627012
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10862382/
Abstract

BACKGROUND

Stavudine remains a component of combination antiretroviral therapy (ART) in resource-constrained countries due to its relatively low cost despite the WHO recommendation for its phasing out as a strategy to reduce stavudine associated toxicities. Where stavudine is still in use, it is recommended at a dose lower than the standard dose in order to reduce stavudine related toxicity.

OBJECTIVES

To compare the safety and virologic efficacy of low dose versus high dose stavudine for treating HIV-1 infection.

SEARCH METHODS

The comprehensive search strategy developed by the Cochrane HIV/AIDS Review Group was used to identify randomised controlled trials that compared the use of low dose versus high dose stavudine. The last search was conducted in February 2014 and the searches covered the period 1996 to 2014.

SELECTION CRITERIA

Randomised controlled trials comparing the use of low dose and high dose stavudine as part of ART combination therapy for treating adults.

DATA COLLECTION AND ANALYSIS

Two reviewers independently selected eligible trials, assessed methodological quality of the included studies and completed data extraction and analysis.

MAIN RESULTS

The search identified 3952 abstracts which were scanned for relevance. Three trials met the inclusion criteria (Milinkovic 2007; McComsey 2008; Sanchez-Conde 2005). All three trials were conducted in developed countries, participants were ART experienced and all had sustained virologic suppression at baseline. A total of 157 participants were recruited to the trials. Sample sizes ranged from 24 to 92 and more than 79% of participants were male.The studies were at a high risk of selection, performance/detection and selective outcome reporting biases. Some baseline characteristics differed among the groups, including triglyceride levels in two studies and body mass index in one study. In light of variation in the design and follow-up of the study results, no meta-analysis was performed and the results of single studies are presented. There was no significant difference in virologic suppression in the included studies (Milinkovic 2007; McComsey 2008; Sanchez-Conde 2005); Risk Ratio (RR) 1.09 (95% CI: 0.93 to 1.28), 0.94 (95% CI:0.59 to 1.50) and 1.03 (95% CI: 0.90 to 1.18) respectively. Symptomatic hyperlactatemia was seen in the high dose arm of the Milinkovic 2007 study; RR 0.21 (95% CI: 0.01 to 4.66), in no participants in the McComsey 2008 trial and not reported on in the Sanchez-Conde 2005 trial. McComsey 2008 and Milinkovic 2007 demonstrated a reduction in bone mineral density (BMD), reduction in limb fat and an increase in triglycerides in the high dose arms. The studies did not indicate that any participants discontinued treatment due to adverse events.

AUTHORS' CONCLUSIONS: This systematic review identified only three small trials that evaluated virologic efficacy and safety of high dose versus low dose stavudine. All three trials were conducted in developed countries and none reported from developing countries yet stavudine remains a component of ART combination therapy in many developing countries. It was not possible to perform a meta-analysis on these trails. Individual results from the trials were imprecise and have not identified a clear advantage in virologic efficacy or safety between low and high dose stavudine. Furthermore, enrolled participants were treatment experienced with sustained virologic suppression and so existing data cannot be generalized to settings where stavudine is currently used in ART naive patients with high viral loads. Stavudine dose reduction trials in ART naive patients, in developing countries where stavudine is still being used are warranted as the phasing out of stavudine that is recommended by WHO may not be immediately universally feasible.

摘要

背景

司他夫定仍是资源有限国家抗逆转录病毒联合治疗(ART)方案的组成部分,因其成本相对较低,尽管世界卫生组织建议逐步淘汰司他夫定,以减少与司他夫定相关的毒性。在仍使用司他夫定的地方,建议使用低于标准剂量的司他夫定,以降低与司他夫定相关的毒性。

目的

比较低剂量与高剂量司他夫定治疗HIV-1感染的安全性和病毒学疗效。

检索方法

采用Cochrane HIV/AIDS综述小组制定的综合检索策略,以识别比较低剂量与高剂量司他夫定使用情况的随机对照试验。最近一次检索于2014年2月进行,检索涵盖1996年至2014年期间。

入选标准

比较低剂量和高剂量司他夫定作为ART联合治疗一部分用于治疗成人的随机对照试验。

数据收集与分析

两名综述作者独立选择符合条件的试验,评估纳入研究的方法学质量,并完成数据提取和分析。

主要结果

检索识别出3952篇摘要,并对其相关性进行了筛选。三项试验符合纳入标准(米林科维奇2007年;麦科姆西2008年;桑切斯-孔德2005年)。所有三项试验均在发达国家进行,参与者都有ART治疗经验,且基线时均有持续的病毒学抑制。试验共招募了157名参与者。样本量从24至92不等,超过79%的参与者为男性。这些研究存在较高的选择、实施/检测和选择性结果报告偏倚风险。各研究组之间的一些基线特征存在差异,包括两项研究中的甘油三酯水平和一项研究中的体重指数。鉴于研究结果在设计和随访方面存在差异,未进行荟萃分析,仅呈现了单项研究的结果。纳入研究中病毒学抑制方面无显著差异(米林科维奇2007年;麦科姆西2008年;桑切斯-孔德2005年);风险比(RR)分别为1.09(95%CI:0.93至1.28)、0.94(95%CI:0.59至1.50)和1.03(95%CI:0.90至1.18)。在米林科维奇2007年研究的高剂量组中观察到有症状的高乳酸血症;RR为0.21(95%CI:0.01至4.66),麦科姆西2008年试验中无参与者出现该情况,桑切斯-孔德2005年试验未报告该情况。麦科姆西2008年和米林科维奇2007年的研究表明,高剂量组骨矿物质密度(BMD)降低、肢体脂肪减少且甘油三酯升高。这些研究未表明有任何参与者因不良事件而停药。

作者结论

本系统评价仅识别出三项评估高剂量与低剂量司他夫定病毒学疗效和安全性的小型试验。所有三项试验均在发达国家进行,尚无来自发展中国家的报告,但司他夫定仍是许多发展中国家ART联合治疗的组成部分。无法对这些试验进行荟萃分析。试验的个体结果不精确,未明确低剂量与高剂量司他夫定在病毒学疗效或安全性方面的明显优势。此外,纳入的参与者都有治疗经验且有持续的病毒学抑制,因此现有数据不能推广到目前在病毒载量高的初治患者中使用司他夫定的情况。鉴于世界卫生组织建议逐步淘汰司他夫定可能并非立即在全球范围内都可行,在司他夫定仍在使用的发展中国家,对初治患者进行司他夫定剂量降低试验是必要的。