来自患者的HIV-1分离株对齐多夫定和α-干扰素的体外耐药性：与治疗持续时间和反应的相关性。

In-vitro resistance to zidovudine and alpha-interferon in HIV-1 isolates from patients: correlations with treatment duration and response.

作者信息

Edlin B R, St Clair M H, Pitha P M, Whaling S M, King D M, Bitran J D, Weinstein R A

机构信息

Division of HIV/AIDS, Centers for Disease Control, Atlanta, GA 30333.

出版信息

Ann Intern Med. 1992 Sep 15;117(6):457-60. doi: 10.7326/0003-4819-117-6-457.

DOI:10.7326/0003-4819-117-6-457

PMID:1503348

Abstract

OBJECTIVE

To measure in-vitro antiviral drug susceptibilities of human immunodeficiency virus type 1 (HIV-1) isolates recovered from patients treated with alpha-interferon or zidovudine and patients not treated with these drugs and to examine the relation of these susceptibility measurements to duration of therapy, disease stage, and response to alpha-interferon therapy.

DESIGN

Cross-sectional study.

SETTING

Outpatient HIV clinic.

PATIENTS

Twenty-six ambulatory HIV-1-infected patients: Fifteen of these patients were receiving alpha-interferon therapy, and 11 had never received such therapy. Nine patients were participating in a clinical trial of combination therapy with zidovudine and alpha-interferon.

MEASUREMENTS

The 50% inhibitory concentration (IC50) of zidovudine and alpha-interferon was determined for HIV-1 isolates recovered from each patient. Plasma concentrations of HIV-1 p24 antigen in the nine patients in the clinical trial were measured monthly after alpha-interferon was added to zidovudine monotherapy.

RESULTS

Zidovudine IC50 (range, 0.01 to 4.87 microM) increased steadily with duration of zidovudine therapy (r = 0.57, P = 0.003). In contrast, alpha-interferon IC50 (range, 0.8 to 415 units/mL) was not related to duration of alpha-interferon treatment; in fact, high IC50s were found in isolates from patients who had never received exogenous alpha-interferon therapy. Resistance to alpha-interferon was greater in isolates from the 15 patients with the acquired immunodeficiency syndrome (AIDS) (median, 104 units/mL) than in those from the 10 patients without AIDS (median, 50 units/mL). Interferson activity was detected in plasma samples from 23 of 24 patients and was also at higher levels in patients with AIDS than in HIV-infected patients without AIDS. Reductions in plasma concentrations of HIV-1 p24 antigen in nine patients after beginning alpha-interferon therapy were greater in those with more susceptible isolates (r = -0.72, P = 0.03).

CONCLUSIONS

Interferon resistance, possibly due to endogenous interferon, is not related to duration of interferon therapy but may limit the effectiveness of interferon therapy. Determinations of interferon susceptibility may identify patients most likely to benefit from this agent.

摘要

目的

检测从接受α-干扰素或齐多夫定治疗的患者以及未接受这些药物治疗的患者中分离出的人类免疫缺陷病毒1型（HIV-1）毒株的体外抗病毒药物敏感性，并研究这些敏感性检测结果与治疗持续时间、疾病阶段以及对α-干扰素治疗反应之间的关系。

设计

横断面研究。

地点

门诊HIV诊所。

患者

26例门诊HIV-1感染患者：其中15例患者正在接受α-干扰素治疗，11例从未接受过此类治疗。9例患者参与了齐多夫定与α-干扰素联合治疗的临床试验。

测量指标

测定从每位患者分离出的HIV-1毒株对齐多夫定和α-干扰素的50%抑制浓度（IC50）。在临床试验的9例患者中，在齐多夫定单药治疗中添加α-干扰素后，每月测量血浆中HIV-1 p24抗原的浓度。

结果

齐多夫定IC50（范围为0.01至4.87μM）随着齐多夫定治疗持续时间的延长而稳步增加（r = 0.57，P = 0.003）。相比之下，α-干扰素IC50（范围为0.8至415单位/mL）与α-干扰素治疗持续时间无关；事实上，在从未接受过外源性α-干扰素治疗的患者分离出的毒株中发现了高IC50。来自15例获得性免疫缺陷综合征（AIDS）患者的分离株对α-干扰素的耐药性（中位数为104单位/mL）高于来自10例无AIDS患者的分离株（中位数为50单位/mL）。在24例患者中的23例血浆样本中检测到干扰素活性，且AIDS患者中的干扰素活性水平也高于未患AIDS的HIV感染患者。在开始α-干扰素治疗后，9例患者中，分离株更敏感的患者血浆中HIV-1 p24抗原浓度的降低幅度更大（r = -0.72，P = 0.03）。