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两药与三药方案治疗 HIV-1:我们是否有足够的数据来进行转换?

Two-drug vs. three-drug combinations for HIV-1: Do we have enough data to make the switch?

机构信息

Department of Infectious Diseases, University Hospital Ramón y Cajal, Alcalá University, IRYCIS, Madrid, Spain.

Department of Laboratory Medicine, ASST Niguarda Hospital, University of Milan, Milan, Italy.

出版信息

HIV Med. 2019 Apr;20 Suppl 4:2-12. doi: 10.1111/hiv.12716.

Abstract

Three-drug combination antiretroviral therapy (ART) became available in 1996, dramatically improving the prognosis of people living with HIV. The clinical benefits of ART are due to the sustained viral load suppression and CD4 T cell gains. Major drawbacks of the first ART regimens were adverse events, and high pill burden, which led to the reduction of drug adherence resulting in frequent treatment discontinuations and the development of drug resistance. Due to increased viral potency of new antiretroviral drugs consideration of a two-drug combination therapy repositioning occurred in an effort to reduce adverse events, drug-drug interactions and cost, while maintaining a sustained antiviral effect. Various combinations of two-drug regimens have been studied, and non-inferiority compared to a three-drug regimen has been shown only for some of them. In addition, a two-drug combination regimen may not be suitable for every patient, especially those who are pregnant, those with tuberculosis or coexisting HBV infection. Furthermore no information has been generated concerning the secondary transmission of HIV from patients who have undetectable plasma viral load on two-drug regimens. Additional studies of two-drug combinations are also necessary to evaluate the debated existence of low viral replication in tissues and on immune activation. While there is no urgent need to routinely switch patients to two-drug combination therapy, due to the availability of drug combinations without significant toxicities, dual regimens represent a suitable option that deserve long-term evaluation before being introduced to clinical practice.

摘要

三药联合抗逆转录病毒疗法(ART)于 1996 年问世,极大地改善了 HIV 感染者的预后。ART 的临床获益归因于持续的病毒载量抑制和 CD4 T 细胞的增加。第一代 ART 方案的主要缺点是不良反应和高药物负担,这导致药物依从性降低,从而频繁中断治疗并产生耐药性。由于新抗逆转录病毒药物的病毒效力增加,考虑重新定位二药联合治疗以减少不良反应、药物相互作用和成本,同时保持持续的抗病毒效果。已经研究了各种二药联合方案,但只有其中一些方案与三药方案相比具有非劣效性。此外,二药联合方案可能并不适合每个患者,尤其是孕妇、结核病或合并乙型肝炎病毒感染的患者。此外,对于接受二药方案治疗且血浆病毒载量不可检测的患者,关于 HIV 二次传播的信息尚未生成。还需要对二药联合方案进行更多研究,以评估关于组织和免疫激活中低病毒复制的争议是否存在。虽然由于没有明显毒性的药物联合方案的可用性,目前没有必要常规将患者切换至二药联合治疗,但双药方案是一种合适的选择,在引入临床实践之前,值得进行长期评估。

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