通过复制终点浓度测定法确定的1型人类免疫缺陷病毒临床分离株中去羟肌苷和齐多夫定的耐药模式。
Didanosine and zidovudine resistance patterns in clinical isolates of human immunodeficiency virus type 1 as determined by a replication endpoint concentration assay.
作者信息
McLeod G X, McGrath J M, Ladd E A, Hammer S M
机构信息
Department of Medicine, New England Deaconess Hospital, Boston, Massachusetts.
出版信息
Antimicrob Agents Chemother. 1992 May;36(5):920-5. doi: 10.1128/AAC.36.5.920.
Reports of in vitro resistance of human immunodeficiency virus type 1 (HIV-1) to zidovudine (AZT) have raised concerns about the development of resistance to other dideoxynucleosides in clinical use. To address this, we have developed a screening assay which supports the growth of clinical isolates and have applied this to a series of paired isolates from patients entered into a phase I trial of didanosine (DDI). Thirteen patients (10 with AIDS, 3 with AIDS-related complex) who had been exposed to AZT for a mean of 6.5 months (range, 1 to 13 months) were treated with DDI at 750 mg/day. Paired isolates were obtained pretherapy and after a mean of 58 weeks (range, 21 to 90) of DDI therapy by coculture of peripheral blood mononuclear leukocytes (PBLs) with phytohemagglutinin-stimulated donor PBLs. Isolates were passaged only one additional time in PBLs and then tested in parallel in a microtiter assay with phytohemagglutinin-stimulated donor PBLs as targets. PBLs were infected with 10(5) 50% tissue culture infectious doses per 10(7) cells and exposed to DDI (1 to 50 microM) or AZT (0.01 to 100 microM), and supernatants were assayed for the HIV p24 antigen at 7 days postinfection. Control AZT-susceptible and resistant isolates were included. The median pre- and posttherapy DDI susceptibilities of the 13 pairs of isolates were 10.0 microM (range, 1 to 25 microM) and 17.5 microM (range, 2.5 to 50 microM), respectively (P = 0.036; Wilcoxon signed-rank test). These studies thus indicated that (i) the susceptibility to DDI tends to mildly decrease with drug exposure; (ii) the susceptibility to AZT improves with time off AZT; (iii) baseline susceptibilities to DDI have a wide range, and the CD4 response may correlate with the initial susceptibility; and (iv) a PBL-based microtiter assay is useful for screening clinical isolated for dideoxynucleoside susceptibility profiles.
有报告称人类免疫缺陷病毒1型(HIV-1)对齐多夫定(AZT)产生了体外耐药性,这引发了人们对临床使用的其他双脱氧核苷产生耐药性的担忧。为解决这一问题,我们开发了一种支持临床分离株生长的筛选试验,并将其应用于参加去羟肌苷(DDI)I期试验患者的一系列配对分离株。13名患者(10名艾滋病患者,3名艾滋病相关综合征患者)平均接受AZT治疗6.5个月(范围1至13个月),随后接受750毫克/天的DDI治疗。通过将外周血单个核白细胞(PBL)与植物血凝素刺激的供体PBL共培养,在治疗前和平均接受58周(范围21至90周)的DDI治疗后获得配对分离株。分离株仅在PBL中再传代一次,然后在微量滴定试验中与植物血凝素刺激的供体PBL作为靶标进行平行测试。用每10^7个细胞10^5个50%组织培养感染剂量感染PBL,并使其暴露于DDI(1至50微摩尔)或AZT(0.01至100微摩尔),感染后7天测定上清液中的HIV p24抗原。包括对照的AZT敏感和耐药分离株。13对分离株治疗前和治疗后DDI敏感性的中位数分别为10.0微摩尔(范围1至25微摩尔)和17.5微摩尔(范围2.5至50微摩尔)(P = 0.036;Wilcoxon符号秩检验)。因此,这些研究表明:(i)对DDI的敏感性倾向于随着药物暴露而轻度降低;(ii)停用AZT后对AZT的敏感性提高;(iii)对DDI的基线敏感性范围较宽,CD4反应可能与初始敏感性相关;(iv)基于PBL的微量滴定试验可用于筛选临床分离株的双脱氧核苷敏感性谱。
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