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去铁胺与氟康唑联用对氟康唑耐药株的协同作用

Synergistic Effect of the Combination of Deferoxamine and Fluconazole and against Fluconazole-Resistant Spp.

机构信息

Department of Medical Mycology, Shanghai Skin Disease Hospital, Tongji University School of Medicine, Shanghai, People's Republic of China.

Institute for Biomedical Engineering & Nano Science, Tongji University School of Medicine, Shanghai, People's Republic of China.

出版信息

Antimicrob Agents Chemother. 2022 Nov 15;66(11):e0072522. doi: 10.1128/aac.00725-22. Epub 2022 Oct 26.

Abstract

The opportunistic fungal infections are an increasing threat to humans due to the increasing number of patients with immunodeficiency, in which the most popular fungal pathogen is Candida albicans. Fluconazole (FLC) is the common drug for treating C. albicans infections, but increasing drug resistance has limited its clinical use. Currently, combination therapy is being investigated as a treatment to overcome the resistance of C. albicans. This report investigated the synergistic properties of deferoxamine (DFO) and FLC combination therapy and against drug-resistant C. albicans. The results showed that the combination of DFO and FLC had a great synergistic antifungal effect against C. albicans, an FLC-resistant strain, with a fractional inhibition concentration index (FICI) of 0.25 by the broth microdilution checkerboard assay. Furthermore, the combination of DFO and FLC significantly inhibited the activity of C. glabrata cells (approximately 30% of C. glabrata cells are azole-resistant). The time-growth curves confirmed that the combination of DFO and FLC have a potent synergistic antifungal effect. Hyphal formation assays confirmed that DFO inhibited the hyphal induction of C. albicans. In addition, the combination of DFO and FLC significantly inhibited the expression of the adhesion gene (). experiments showed that the combination of DFO and FLC significantly reduced pustules, CFU counts and inflammatory cell infiltration in skin tissue. These results suggest that the combination of DFO and FLC inhibits yeast-hyphae transformation, reduces C. albicans infectivity and resistance and , and affects Cek1 MAPK signaling. This may offer a new option for the treatment of cutaneous candidiasis.

摘要

机会性真菌感染对人类构成的威胁日益增加,这是由于免疫功能低下患者人数不断增加所致,其中最常见的真菌病原体是白色念珠菌。氟康唑(FLC)是治疗白色念珠菌感染的常用药物,但耐药性的增加限制了其临床应用。目前,联合治疗作为一种治疗方法正在被研究,以克服白色念珠菌的耐药性。本报告研究了去铁胺(DFO)和 FLC 联合治疗对耐药性白色念珠菌的协同作用。结果表明,DFO 和 FLC 联合对耐氟康唑的白色念珠菌具有很强的协同抗真菌作用,通过肉汤微量稀释棋盘试验,其部分抑制浓度指数(FICI)为 0.25。此外,DFO 和 FLC 的联合显著抑制了光滑念珠菌细胞的活性(约 30%的光滑念珠菌细胞对唑类药物耐药)。时间生长曲线证实 DFO 和 FLC 的联合具有强大的协同抗真菌作用。菌丝形成试验证实 DFO 抑制了白色念珠菌的菌丝诱导。此外,DFO 和 FLC 的联合显著抑制了黏附基因()的表达。实验表明,DFO 和 FLC 的联合显著减少了皮肤组织中的脓疱、CFU 计数和炎症细胞浸润。这些结果表明,DFO 和 FLC 的联合抑制酵母-菌丝转化,降低白色念珠菌的感染性和耐药性,并影响 Cek1 MAPK 信号通路。这可能为治疗皮肤念珠菌病提供新的选择。

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