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苯并咪唑类化合物 SPR719 对非结核分枝杆菌具有浓度依赖性的活性和协同作用。

The Benzimidazole SPR719 Shows Promising Concentration-Dependent Activity and Synergy against Nontuberculous Mycobacteria.

机构信息

Radboudumc Center for Infectious Diseases, Department of Medical Microbiology, Radboud University Medical Center, Nijmegen, the Netherlands.

Radboudumc Center for Infectious Diseases, Department of Medical Microbiology, Radboud University Medical Center, Nijmegen, the Netherlands

出版信息

Antimicrob Agents Chemother. 2021 Mar 18;65(4). doi: 10.1128/AAC.02469-20.

Abstract

Nontuberculous mycobacterial pulmonary disease (NTM-PD) is emerging worldwide. Currently recommended multidrug treatment regimens yield poor outcomes, and new drugs and regimens are direly needed. SPR719, the active moiety of SPR720, is a new benzimidazole antibiotic with limited data on antimycobacterial activity. We determined MICs and MBCs against 138 clinical and reference strains of complex (MAC), , , , , and and determined synergy with antimycobacterial drugs by checkerboard titrations. To study pharmacodynamics, we performed time-kill kinetics assays of SPR719 alone and in combinations against , , and and assessed synergy by response surface analysis according to Bliss independence. SPR719 showed potent activity against MAC (MIC, 2 mg/liter) and (MIC, 0.125 mg/liter) and modest activity against (MIC, 8 mg/liter); its activity is bacteriostatic and concentration-dependent. We recorded a potential for combination therapy with ethambutol against and and synergy with clarithromycin against Ethambutol increased the SPR719 kill rate against but only prevented SPR719 resistance in SPR719 is active against NTM; its activity is strongest against , followed by MAC and SPR719 shows promise for combination therapy with ethambutol against MAC and and synergy with clarithromycin against The parent drug SPR720 could have a role especially in MAC pulmonary disease treatment. Further studies in dynamic models and trials are ongoing to advance clinical development.

摘要

非结核分枝杆菌肺病(NTM-PD)在全球范围内不断出现。目前推荐的多药治疗方案效果不佳,急需新的药物和治疗方案。SPR719 是 SPR720 的活性成分,是一种新型苯并咪唑类抗生素,其抗分枝杆菌活性的数据有限。我们测定了 SPR719 对 138 株临床和参考分枝杆菌复合群(MAC)、 、 、 、 和 菌株的 MIC 和 MBC,并通过棋盘滴定法测定了与抗分枝杆菌药物的协同作用。为了研究药效动力学,我们单独和联合使用 SPR719 对抗 、 、 和 进行了时间杀伤动力学试验,并根据 Bliss 独立性通过响应面分析评估协同作用。SPR719 对 MAC(MIC,2mg/L)和 (MIC,0.125mg/L)具有强大的活性,对 (MIC,8mg/L)具有中等活性;其活性呈抑菌和浓度依赖性。我们记录了与乙胺丁醇联合治疗 和 的潜在可能性,以及与克拉霉素联合治疗 的协同作用。乙胺丁醇提高了 SPR719 对 的杀伤率,但仅能防止 对 SPR719 的耐药性。SPR719 对 NTM 具有活性;其活性对 最强,其次是 MAC 和 。SPR719 与乙胺丁醇联合治疗 MAC 和 以及与克拉霉素联合治疗 具有协同作用,前景广阔。母药 SPR720 尤其在治疗 MAC 肺病方面可能具有作用。正在进行动态模型和试验的进一步研究,以推进临床开发。

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