首页> 外文期刊>Journal of Medicinal Chemistry >Structure-Activity Relationship Studies of Novel Benzophenones Leading to the Discovery of a Potent,Next Generation HIV Nonnucleoside Reverse Transcriptase Inhibitor
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Structure-Activity Relationship Studies of Novel Benzophenones Leading to the Discovery of a Potent,Next Generation HIV Nonnucleoside Reverse Transcriptase Inhibitor

机译:新型苯甲酮的结构-活性关系研究,导致发现有力的下一代HIV Nonnucleoside逆转录酶抑制剂

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摘要

Despite the progress of the past two decades,there is still considerable need for safe,efficacious drugs that target human immunodeficiency virus (HIV).This is particularly true for the growing number of patients infected with virus resistant to currently approved HIV drugs.Our high throughput screening effort identified a benzophenone template as a potential nonnucleoside reverse transcriptase inhibitor (NNRTI).This manuscript describes our extensive exploration of the benzophenone structure-activity relationships,which culminated in the identification of several compounds with very potent inhibition of both wild type and clinically relevant NNRTI-resistant mutant strains of HIV.These potent inhibitors include 70h (GW678248),which has in vitro antiviral assay IC_(50) values of 0.5 nM against wild-type HIV,1 nM against the K103N mutant associated with clinical resistance to efavirenz,and 0.7 nM against the Y181C mutant associated with clinical resistance to nevirapine.Compound 70h has also demonstrated relatively low clearance in intravenous pharmacokinetic studies in three species,and it is the active component of a drug candidate which has progressed to phase 2 clinical studies.
机译:尽管在过去的二十年中取得了进步,但仍存在对针对人类免疫缺陷病毒(HIV)的安全有效药物的需求。这对越来越多的患者感染了对目前批准的HIV药物具有抗药性的患者尤其如此。通量筛选工作确定了二苯甲酮模板是潜在的非核苷类逆转录酶抑制剂(NNRTI)。该手稿描述了我们对二苯甲酮结构-活性关系的广泛探索,最终鉴定出对野生型和临床都具有非常强抑制作用的几种化合物这些有效的抑制剂包括70h(GW678248),其对野生型HIV的体外抗病毒试验IC_(50)值为0.5 nM,对K103N突变体的IC_(50)值为1 nM,与依法韦仑的临床耐药性相关,和针对与奈韦拉平的临床耐药性相关的Y181C突变体的0.7 nM化合物70h具有在三种药物的静脉药代动力学研究中也显示出相对较低的清除率,并且它是候选药物的有效成分,该药物已进入第二阶段临床研究。

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