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接受耐药性检测指导的高效抗逆转录病毒治疗(HAART)的多次病毒学治疗失败患者的血浆HIV RNA下降及耐药性突变的出现

Plasma HIV RNA decline and emergence of drug resistance mutations among patients with multiple virologic failures receiving resistance testing-guided HAART.

作者信息

Tozzi Valerio, Bellagamba Rita, Castiglione Filippo, Amendola Alessanda, Ivanovic Jelena, Nicastri Emanuele, Libertone Raffaella, D'Offizi Giampiero, Liuzzi Giuseppina, Gori Caterina, Forbici Federica, D'Arrigo Roberta, Bertoli Ada, Salvatori Maria Flora, Capobianchi Maria Rosaria, Antinori Andrea, Perno Carlo Federico, Narciso Pasquale

机构信息

National Institute for Infectious Diseases Lazzaro Spallanzani, 00149 Rome, Italy.

出版信息

AIDS Res Hum Retroviruses. 2008 Jun;24(6):787-96. doi: 10.1089/aid.2007.0236.

Abstract

Early recognition of virologic failure in patients with extensive drug resistance receiving salvage-HAART is essential to avoid exposure to subinhibitory regimens. We studied plasma viral load (PVL) decline and rates of drug-resistance mutation (DRM) accumulation in such patients. A prospective, 48 week study of 38 heavily pretreated patients receiving genotypic resistance testing (GRT)-guided HAART was conducted. The rate of PVL decline was studied by weekly PVL determinations. To assess DRM accumulation, serial GRTs were performed in all nonresponders (never reaching PVL <50 or two PVLs >50 copies/ml after suppression). Over 48 weeks, 10 patients (26%) were nonresponders. Receiving less then two fully active drugs and having an elevated number of PI and NRTI mutations at baseline were strongly associated with virologic failure. There was no evidence of a difference in the change from baseline PVL to week 1 and 2 between responders and nonresponders. By contrast, PVL reductions from week 2 to week 3 and thereafter were significantly greater for responders (p < 0.01). Among nonresponders, the incidence rates per patient-month (95% CI) of emergent DRM were 0.67 (0.13-1.20), 0.40 (0.00-0.74), and 0.37 (0.00-0.75) at weeks 4, 8, and 24, respectively. Having limited baseline resistance, receiving at least two fully active drugs, and showing constant PVL reductions from week 2 to week 3 and thereafter were predictive of virologic response. In contrast, early changes in PVL levels were not. Virologic failure was associated with detection of emergent DRMs. Virologic rebound in patients on salvage-HAART should be addressed aggressively.

摘要

对于接受挽救性高效抗逆转录病毒治疗(salvage-HAART)且具有广泛耐药性的患者,早期识别病毒学失败对于避免暴露于亚抑制性治疗方案至关重要。我们研究了此类患者的血浆病毒载量(PVL)下降情况以及耐药突变(DRM)积累率。对38例接受过大量治疗且接受基因型耐药性检测(GRT)指导的HAART的患者进行了一项为期48周的前瞻性研究。通过每周测定PVL来研究PVL下降率。为了评估DRM积累情况,对所有无反应者(在抑制后从未达到PVL<50或两次PVL>50拷贝/ml)进行了系列GRT。在48周内,10例患者(26%)无反应。接受少于两种完全有效的药物以及基线时蛋白酶抑制剂(PI)和核苷类逆转录酶抑制剂(NRTI)突变数量增加与病毒学失败密切相关。在反应者和无反应者之间,从基线PVL到第1周和第2周的变化没有差异的证据。相比之下,反应者从第2周到第3周及之后的PVL降低幅度显著更大(p<0.01)。在无反应者中,第4周、第8周和第24周时每位患者每月出现DRM的发生率(95%置信区间)分别为0.67(0.13 - 1.20)、0.40(0.00 - 0.74)和0.37(0.00 - 0.75)。基线耐药有限、接受至少两种完全有效的药物以及从第2周到第3周及之后显示PVL持续降低可预测病毒学反应。相比之下,PVL水平的早期变化则不然。病毒学失败与新出现的DRM检测相关。对于接受挽救性HAART的患者,病毒学反弹应积极处理。

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