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新型三氮杂吖庚因类药物 gepotidacin(GSK2140944)对耐多药淋病奈瑟菌的体外活性。

In vitro activity of the novel triazaacenaphthylene gepotidacin (GSK2140944) against MDR Neisseria gonorrhoeae.

机构信息

WHO Collaborating Centre for Gonorrhoea and Other Sexually Transmitted Infections, National Reference Laboratory for Sexually Transmitted Infections, Department of Laboratory Medicine, Faculty of Medicine and Health, Örebro University, Örebro, Sweden.

GlaxoSmithKline, Collegeville, PA, USA.

出版信息

J Antimicrob Chemother. 2018 Aug 1;73(8):2072-2077. doi: 10.1093/jac/dky162.

Abstract

OBJECTIVES

Increased antimicrobial resistance surveillance and new effective antimicrobials are crucial to maintain treatable gonorrhoea. We examined the in vitro activity of gepotidacin, a novel triazaacenaphthylene, and the effect of efflux pump inactivation on clinical Neisseria gonorrhoeae isolates and international reference strains (n = 252) and compared gepotidacin with antimicrobials currently or previously recommended for gonorrhoea treatment.

METHODS

MICs (mg/L) were determined by agar dilution (gepotidacin) or by Etest (seven other antimicrobials). The gyrA and parC genes were sequenced and the impact of inactivation of the MtrCDE, MacAB and NorM efflux pumps on gepotidacin MICs was examined.

RESULTS

Gepotidacin showed potent in vitro activity against all gonococcal isolates (n = 252; MIC ≤4 mg/L). The modal MIC, MIC50, MIC90 and MIC range of gepotidacin were 0.5, 0.5, 1 and 0.032-4 mg/L, respectively. Inactivation of the MtrCDE efflux pump, but not MacAB or NorM, decreased the gepotidacin MICs for most strains. No significant cross-resistance between gepotidacin and any other antimicrobials, including the fluoroquinolone ciprofloxacin, was identified. However, the ParC D86N mutation (possibly together with additional antimicrobial resistance mutation), which is associated with fluoroquinolone resistance, was associated with increased gepotidacin MICs.

CONCLUSIONS

Gepotidacin demonstrated high in vitro activity against gonococcal strains, indicating that gepotidacin could potentially be an effective option for gonorrhoea treatment, particularly in a dual antimicrobial therapy regimen and for patients with resistance or allergy to extended-spectrum cephalosporins. Nevertheless, elucidating in vitro and in vivo resistance emergence and mechanisms in detail, together with further gonorrhoea clinical studies, ideally also including chlamydia and Mycoplasma genitalium are essential.

摘要

目的

增加抗菌药物耐药性监测和新的有效抗菌药物对于维持可治疗淋病至关重要。我们检测了新型三氮杂萘并[1,2-d][1,3,5]三嗪酮 gepotidacin 的体外活性,以及外排泵失活对临床淋病奈瑟菌分离株和国际参考株(n=252)的影响,并将 gepotidacin 与目前或以前推荐用于淋病治疗的抗菌药物进行了比较。

方法

通过琼脂稀释法(gepotidacin)或 Etest 法(七种其他抗菌药物)测定 MIC(mg/L)。测序 gyrA 和 parC 基因,并检测 MtrCDE、MacAB 和 NorM 外排泵失活对 gepotidacin MIC 的影响。

结果

gepotidacin 对所有淋病分离株(n=252)均显示出强大的体外活性(MIC≤4mg/L)。gepotidacin 的模式 MIC、MIC50、MIC90 和 MIC 范围分别为 0.5、0.5、1 和 0.032-4mg/L。MtrCDE 外排泵的失活,但不是 MacAB 或 NorM,降低了大多数菌株的 gepotidacin MIC。未发现 gepotidacin 与任何其他抗菌药物(包括氟喹诺酮环丙沙星)之间存在显著的交叉耐药性。然而,与氟喹诺酮耐药相关的 ParC D86N 突变(可能与其他抗菌药物耐药突变一起)与 gepotidacin MIC 升高有关。

结论

gepotidacin 对淋病菌株显示出高体外活性,表明 gepotidacin 可能是淋病治疗的有效选择,特别是在双重抗菌治疗方案中,以及对头孢菌素类抗生素耐药或过敏的患者。然而,阐明体外和体内耐药性的出现和机制,以及进一步的淋病临床研究,理想情况下还包括衣原体和支原体,是必不可少的。

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