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Long-Term Use of Atazanavir in the Treament of HIV-Infected Patients

机译:长期使用阿扎那韦治疗艾滋病毒感染者

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Atazanavir (ATV) is an HIV protease inhibitor (PI) that was approved as antiretroviral agent in year 2003. Ritonavir (RTV) enhances ATV plasma exposure and increases its barrier to resistance. Antiretroviral therapy with ATV plus RTV (ATV/r) has demonstrated high potency for achieving virological suppression in antiretroviral-na?ve patients and in simplification strategies. In rescue interventions, ATV/r-based combinations have shown to be equivalent in terms of viral response to other PI/r-containing regimens. In contrast with all other PIs, ATV has also demonstrated efficacy when given unboosted with RTV, an option attractive in special situations. Other benefits of the drug are its good metabolic and gastrointestinal profile. Its main adverse event is hyperbilirubinemia, since ATV inhibits the hepatic uridin-glucoronyl-transferase. A signature mutation at the protease gene, I50L, confers loss of susceptibility to the drug whereas it may confer hypersusceptibility to other PIs. Many ATV studies have provided data until or beyond week 96, supporting the efficacy and safety of the drug in the long-term.
机译:Atazanavir(ATV)是一种HIV蛋白酶抑制剂(PI),于2003年被批准用作抗逆转录病毒药物。Ritonavir(RTV)增强ATV血浆暴露并增加其耐药性屏障。 ATV加RTV(ATV / r)的抗逆转录病毒疗法已显示出对初次使用抗逆转录病毒疗法的患者和简化策略有效的病毒抑制作用。在救援干预中,基于ATV / r的组合在病毒应答方面已显示出与其他含PI / r的方案相当。与所有其他PI相比,ATV在不加RTV的情况下也表现出功效,这在特殊情况下很有吸引力。该药物的其他好处是其良好的代谢和胃肠道功能。它的主要不良事件是高胆红素血症,因为ATV抑制肝尿素-葡萄糖醛酸转移酶。蛋白酶基因I50L的特征性突变赋予了药物敏感性,而它可能赋予了其他PI高度敏感性。许多ATV研究都提供了直到第96周或以后的数据,从而长期支持了该药的有效性和安全性。

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