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Improving combination antiretroviral therapy by targeting HIV-1 gene transcription

机译:通过靶向HIV-1基因转录来改善联合抗逆转录病毒疗法

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Introduction: Combination Antiretroviral Therapy (cART) has not allowed the cure of HIV. The main obstacle to HIV eradication is the existence of quiescent reservoirs. Several other limitations of cART have been described, such as strict life-long treatment and high costs, restricting it to Western countries, as well as the development of multidrug resistance. Given these limitations and the impetus to find a cure, the development of new treatments is necessary.Areas covered: In this review, we discuss the current status of several efficient molecules able to suppress HIV gene transcription, including NF-kB and Tat inhibitors. We also assess the potential of new proteins belonging to the intriguing DING family, which have been reported to have potential anti-HIV-1 activity by inhibiting HIV gene transcription.Expert opinion: Targeting HIV-1 gene transcription is an alternative approach, which could overcome cART-related issues, such as the emergence of multidrug resistance. Improving cART will rely on the identification and characterization of new actors inhibiting HIV-1 transcription. Combining such efforts with the use of new technologies, the development of new models for preclinical studies, and improvement in drug delivery will considerably reduce drug toxicity and thus increase patient adherence.
机译:简介:联合抗逆转录病毒疗法(cART)不允许治愈HIV。消除艾滋病毒的主要障碍是静态水库的存在。已经描述了cART的其他一些局限性,例如严格的终身治疗和高昂的费用,将其限制在西方国家,以及对多药耐药性的发展。考虑到这些局限性和寻找治疗方法的动力,有必要开发新的治疗方法。涵盖的领域:在本综述中,我们讨论了能够抑制HIV基因转录的几种有效分子的当前状态,包括NF-kB和Tat抑制剂。我们还评估了有趣的DING家族新蛋白的潜力,据报道这些蛋白通过抑制HIV基因转录具有潜在的抗HIV-1活性。专家意见:靶向HIV-1基因转录是另一种方法,可以克服与cART相关的问题,例如出现多药耐药性。改善cART将依赖于抑制HIV-1转录的新参与者的鉴定和表征。将这些努力与新技术的使用相结合,开发用于临床前研究的新模型以及改善药物输送,将大大降低药物毒性并因此增加患者依从性。

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