Liu Yongge, Matsumoto Makoto, Ishida Hidekaza, Ohguro Kinue, Yoshitake Masuhiro, Gupta Rajesh, Geiter Lawrence, Hafkin Jeffrey
Otsuka Pharmaceutical Development & Commercialization, Inc., Rockville, MD, USA.
Pharmaceutical Business Division, Otsuka Pharmaceutical Co., Ltd., Tokyo, Japan.
Tuberculosis (Edinb). 2018 Jul;111:20-30. doi: 10.1016/j.tube.2018.04.008. Epub 2018 May 3.
Tuberculosis (TB), caused by Mycobacterium tuberculosis (MTB), is the leading cause of death from an infectious disease globally. The widespread and ever-increasing resistance to TB drugs is reducing the effectiveness of treatment and jeopardizing TB control. New effective drugs with acceptable safety profiles are needed to turn the tide. Since the early 1990s, Otsuka Pharmaceutical Co., Ltd. has had a TB drug development program that resulted in the selection and development of delamanid (OPC-67683, Deltyba), a first-in-class bicyclic nitroimidazole. Delamanid was initially approved by the European Medicines Agency (EMA) in 2014 for the treatment of adult pulmonary multi-drug resistant (MDR)-TB when an effective treatment regimen cannot otherwise be composed for reasons of resistance or tolerability. It has since been approved by several other countries/regions. In this review, we describe the history of delamanid's development, including the screening process, in vitro and in vivo characterization, as well as various clinical studies. Delamanid possesses potent activity against replicating, dormant, and intracellular MTB bacilli, and is bactericidal in mouse and guinea pig TB models. Delamanid resistance mechanisms have been attributed to genes in the F-dependent deazaflavin nitroreductase bio-activation pathway, found in mycobacterium species but not in common bacterial or mammalian cells. Published susceptibility testing results from 744 clinical isolates from delamanid-naïve patients indicate that the natural resistance rate to delamanid is very low (1.3%). Delamanid is largely metabolized by albumin in serum, and to a much less extent by cytochrome P enzymes. Furthermore, it neither inhibits nor induces P450 enzymes. In terms of efficacy, delamanid demonstrated activity in an early bactericidal activity trial in drug susceptible pulmonary TB patients and increased 2-month sputum culture conversion rates when added to an optimized background regimen in MDR-TB patients in a phase 2b global clinical trial. In addition, recent results outside clinical studies show favourable responses in highly resistant TB patients including extensively drug resistant (XDR)-TB when treated with delamanid-containing regimens in routine programmatic settings. The primary safety concern with delamanid is QTcF interval prolongation, although this observation has thus far not been associated with any clinical cardiac events. Overall, delamanid appears to be a well-tolerated and safe anti-TB drug when compared to other drugs used to treat MDR-TB.
结核病(TB)由结核分枝杆菌(MTB)引起,是全球传染病致死的主要原因。对结核病药物广泛且不断增加的耐药性正在降低治疗效果,并危及结核病防控。需要有安全性可接受的新型有效药物来扭转局面。自20世纪90年代初以来,大冢制药有限公司开展了一项结核病药物研发计划,最终筛选并开发出了地拉曼德(OPC - 67683,Deltyba),这是一种一流的双环硝基咪唑类药物。地拉曼德最初于2014年获欧洲药品管理局(EMA)批准,用于治疗成年耐多药(MDR)肺结核,前提是由于耐药性或耐受性原因无法组成有效的治疗方案。此后它又获得了其他几个国家/地区的批准。在本综述中,我们描述了地拉曼德的研发历程,包括筛选过程、体外和体内特性,以及各项临床研究。地拉曼德对正在复制、处于休眠状态和细胞内的MTB杆菌具有强大活性,并且在小鼠和豚鼠结核病模型中具有杀菌作用。地拉曼德的耐药机制归因于F - 依赖性脱氮黄素硝基还原酶生物激活途径中的基因,这种基因存在于分枝杆菌属中,但在常见细菌或哺乳动物细胞中不存在。来自未使用过地拉曼德的患者的744株临床分离株的已发表药敏试验结果表明,对地拉曼德的天然耐药率非常低(1.3%)。地拉曼德在血清中主要由白蛋白代谢,在很大程度上较少由细胞色素P酶代谢。此外,它既不抑制也不诱导P450酶。在疗效方面,地拉曼德在药物敏感肺结核患者的早期杀菌活性试验中显示出活性,并且在一项2b期全球临床试验中,当添加到MDR - TB患者的优化背景治疗方案中时,可提高2个月痰培养转阴率。此外,近期临床研究之外的结果表明,在常规项目环境中使用含地拉曼德的方案治疗包括广泛耐药(XDR)结核病在内的高度耐药结核病患者时,有良好反应。地拉曼德主要的安全问题是QTcF间期延长,尽管迄今为止这一观察结果尚未与任何临床心脏事件相关联。总体而言,与用于治疗MDR - TB的其他药物相比,地拉曼德似乎是一种耐受性良好且安全的抗结核药物。
