Reyes-Terán G, Sierra-Madero J G, Martínez del Cerro V, Arroyo-Figueroa H, Pasquetti A, Calva J J, Ruiz-Palacios G M
Department of Infectious Diseases, Instituto Nacional de la Nutrición Salvador Zubirán, Tlalpan, México, D.F., México.
AIDS. 1996 Nov;10(13):1501-7. doi: 10.1097/00002030-199611000-00007.
To evaluate the efficacy of thalidomide in treating wasting syndrome in patients with advanced HIV disease, and to assess the effects of thalidomide on circulating CD4+ T cells, and on HIV viral burden in peripheral blood mononuclear cells (PBMC).
Randomized, double-blind placebo-controlled clinical trial.
Public tertiary care hospital in Mexico City.
Twenty-eight adults with advanced HIV disease being treated with antiretroviral therapy, and who had received antiretrovirals for at least 6 months, who did not have an active opportunistic infection, and who had 10% weight loss in the previous 6 months.
Patients received thalidomide (100 mg by mouth, four times daily) or a matching placebo for the duration of the study (12 weeks).
The main clinical endpoint for efficacy of thalidomide was weight gain or no progression of wasting. Secondary endpoints were Karnofsky performance status, CD4+ cell counts, and HIV viral burden in PBMC.
Both groups were comparable in their baseline status. Therapeutic failure occurred in 10 out of 14 patients from the placebo group and in three out of 14 from the thalidomide group (P = 0.021). Weight gain occurred in one patient on placebo and in eight given thalidomide. The Karnofsky index was significantly higher by the end of the study in the thalidomide group (P = 0.003). Mild and transient somnolence and erythematous macular skin lesions were significantly more common in the thalidomide group. CD4+ T cell counts and HIV viral burden in PBMC did not change in either group.
Results suggest that thalidomide not only impeded but also reverted the wasting syndrome, preserving the Karnofsky index in patients with advanced HIV disease. Thalidomide, at the dosage used in this study, had no effect on peripheral CD4+ T cells nor on HIV viral burden in PBMC.
评估沙利度胺治疗晚期HIV疾病患者消瘦综合征的疗效,并评估沙利度胺对循环CD4 + T细胞以及外周血单核细胞(PBMC)中HIV病毒载量的影响。
随机、双盲、安慰剂对照临床试验。
墨西哥城的公立三级护理医院。
28名接受抗逆转录病毒治疗的晚期HIV疾病成人患者,他们接受抗逆转录病毒药物治疗至少6个月,没有活动性机会性感染,且在过去6个月内体重减轻了10%。
患者在研究期间(12周)接受沙利度胺(口服100毫克,每日4次)或匹配的安慰剂。
沙利度胺疗效的主要临床终点是体重增加或消瘦无进展。次要终点是卡诺夫斯基表现状态、CD4 +细胞计数以及PBMC中的HIV病毒载量。
两组的基线状态具有可比性。安慰剂组14名患者中有10名治疗失败,沙利度胺组14名患者中有3名治疗失败(P = 0.021)。安慰剂组有1名患者体重增加,沙利度胺组有8名患者体重增加。研究结束时,沙利度胺组的卡诺夫斯基指数显著更高(P = 0.003)。沙利度胺组轻度和短暂的嗜睡以及红斑性黄斑皮肤病变明显更常见。两组的CD4 + T细胞计数和PBMC中的HIV病毒载量均未改变。
结果表明,沙利度胺不仅能阻止而且能逆转消瘦综合征,维持晚期HIV疾病患者的卡诺夫斯基指数。本研究中使用的剂量的沙利度胺对外周CD4 + T细胞和PBMC中的HIV病毒载量没有影响。
