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尼可霉素 Z 对持续释放给药的小鼠播散性球孢子菌病的作用。

Nikkomycin Z against Disseminated Coccidioidomycosis in a Murine Model of Sustained-Release Dosing.

机构信息

California Institute for Medical Researchgrid.413248.8, San Jose, California, USA.

Valley Fever Solutions, Tucson, Arizona, USA.

出版信息

Antimicrob Agents Chemother. 2021 Sep 17;65(10):e0028521. doi: 10.1128/AAC.00285-21. Epub 2021 Jul 12.

Abstract

Nikkomycin Z (nikZ) is a chitin synthase inhibitor. Efficacy against has been demonstrated in animal models of pulmonary or brain infection. Its short half-life in mice and in humans would necessitate divided daily dosing. We assayed nikZ efficacy in disseminated coccidioidomycosis (in a reduction of CFU design) and whether sustained release might be useful. Mice were challenged intravenously with low or high arthroconidial inocula. Fluconazole, clinically the most commonly used anticoccidioidal drug, was compared (gavage) at high dose to a dose range of nikZ administered intraperitoneally or, to mimic sustained release, administered continuously in drinking water. Therapy was given for 5 days. , both fluconazole and nikZ inhibited the isolate studied; nikZ was fungicidal. Oral nikZ therapy gave similar results to intraperitoneal nikZ and sterilized infection in most animals after low-inoculum challenge. In both challenges, oral nikZ produced greater reduction of CFU in organs (lung, liver, and spleen) than fluconazole. Oral nikZ doses of ≥200 mg/kg of body weight/day were particularly effective in all organs and were well tolerated. This efficacy occurred even though, after severe challenge, mice had reduced water intake, resulting in ingesting less than the desired dose, particularly initially after infection. This study shows, for the first time, efficacy of nikZ against disseminated coccidioidomycosis. Efficacy was shown after challenges producing different levels of severity of disease. This study also suggests the likely benefits of developing an extended release formulation supplying continuous systemic concentrations of nikZ.

摘要

尼可霉素 Z(nikZ)是一种几丁质合成酶抑制剂。在肺部或脑部感染的动物模型中已证明其对有疗效。其在小鼠和人体内的半衰期短,需要每日分剂量给药。我们检测了 nikZ 在播散性球孢子菌病(以 CFU 减少为指标)中的疗效,以及是否可以使用缓释。通过静脉内接种低或高的关节孢子接种物来挑战小鼠。氟康唑,是临床上最常用的抗球孢子菌药物,与腹腔内给予的不同剂量的 nikZ(以模拟缓释)或连续给予饮用水进行比较(灌胃)。治疗持续 5 天。结果显示,氟康唑和 nikZ 均抑制所研究的分离株;nikZ 具有杀菌作用。在低接种量挑战后,口服 nikZ 治疗与腹腔内 nikZ 治疗相似,并使大多数动物的感染得到了根治。在两种挑战中,与氟康唑相比,口服 nikZ 对器官(肺、肝和脾)中的 CFU 减少更有效果。口服 nikZ 剂量≥200mg/kg 体重/天对所有器官都特别有效,且耐受性良好。即使在严重挑战后,小鼠减少了饮水量,导致摄入的剂量低于预期,特别是在感染后最初几天,这种疗效仍然存在。这项研究首次表明 nikZ 对播散性球孢子菌病有效。在产生不同严重程度疾病的挑战中都显示出疗效。这项研究还表明,开发一种提供持续系统浓度的 nikZ 的缓释制剂可能会带来好处。

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本文引用的文献

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