Antifungal activity of selective serotonin reuptake inhibitors against Cryptococcus spp. and their possible mechanism of action

IF 2.2 4区 医学 Q3 MYCOLOGY Journal de mycologie medicale Pub Date : 2023-08-30 DOI:10.1016/j.mycmed.2023.101431
Cecília Rocha da Silva , Livia Gurgel do Amaral Valente Sá , Thais Lima Ferreira , Amanda Cavalcante Leitão , Vitória Pessoa de Farias Cabral , Daniel Sampaio Rodrigues , Amanda Dias Barbosa , Lara Elloyse Almeida Moreira , Hugo Leonardo Pereira Filho , João Batista de Andrade Neto , Maria Erivanda França Rios , Bruno Coêlho Cavalcanti , Hemerson Iury Ferreira Magalhães , Manoel Odorico de Moraes , Hélio Vitoriano Nobre
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Abstract

Fungal infections caused by Cryptococcus spp. pose a threat to health, especially in immunocompromised individuals. The available arsenal of drugs against cryptococcosis is limited, due to their toxicity and/or lack of accessibility in low-income countries, requiring more therapeutic alternatives. Selective serotonin reuptake inhibitors (SSRIs), through drug repositioning, are a promising alternative to broaden the range of new antifungals against Cryptococcus spp. This study evaluates the antifungal activity of three SSRIs, sertraline, paroxetine, and fluoxetine, against Cryptococcus spp. strains, as well as assesses their possible mechanism of action. Seven strains of Cryptococcus spp. were used. Sensitivity to SSRIs, fluconazole, and itraconazole was evaluated using the broth microdilution assay. The interactions resulting from combinations of SSRIs and azoles were investigated using the checkerboard assay. The possible action mechanism of SSRIs against Cryptococcus spp. was evaluated through flow cytometry assays. The SSRIs exhibited in vitro antifungal activity against Cryptococcus spp. strains, with minimum inhibitory concentrations ranging from 2 to 32 μg/mL, and had synergistic and additive interactions with azoles. The mechanism of action of SSRIs against Cryptococcus spp. involved damage to the mitochondrial membrane and increasing the production of reactive oxygen species, resulting in loss of cellular viability and apoptotic cell death. Fluoxetine also was able to cause significant damage to yeast DNA. These findings demonstrate the in vitro antifungal potential of SSRIs against Cryptococcus spp. strains.

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选择性5 -羟色胺再摄取抑制剂对隐球菌的抗真菌活性及其可能的作用机制
由隐球菌引起的真菌感染对健康构成威胁,特别是在免疫功能低下的个体中。由于隐球菌病的毒性和/或在低收入国家难以获得,现有的抗隐球菌病药物有限,需要更多的治疗选择。选择性5 -羟色胺再摄取抑制剂(SSRIs)通过药物重新定位,有望拓宽新型抗隐球菌药物的范围。本研究评价了舍曲林、帕罗西汀和氟西汀三种SSRIs对隐球菌菌株的抗真菌活性,并对其可能的作用机制进行了评估。使用7株隐球菌。采用肉汤微量稀释法评价对SSRIs、氟康唑和伊曲康唑的敏感性。使用棋盘法研究了SSRIs和唑类药物联合使用的相互作用。通过流式细胞术分析SSRIs对隐球菌可能的作用机制。SSRIs对隐球菌具有较强的体外抑菌活性,最低抑菌浓度在2 ~ 32 μg/mL之间,与唑类具有协同和加性作用。SSRIs对隐球菌的作用机制涉及损伤线粒体膜,增加活性氧的产生,导致细胞活力丧失和凋亡细胞死亡。氟西汀也能对酵母DNA造成严重损害。这些发现证明了SSRIs对隐球菌的体外抗真菌潜力。
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来源期刊
CiteScore
5.10
自引率
2.80%
发文量
68
审稿时长
6-12 weeks
期刊介绍: The Journal de Mycologie Medicale / Journal of Medical Mycology (JMM) publishes in English works dealing with human and animal mycology. The subjects treated are focused in particular on clinical, diagnostic, epidemiological, immunological, medical, pathological, preventive or therapeutic aspects of mycoses. Also covered are basic aspects linked primarily with morphology (electronic and photonic microscopy), physiology, biochemistry, cellular and molecular biology, immunochemistry, genetics, taxonomy or phylogeny of pathogenic or opportunistic fungi and actinomycetes in humans or animals. Studies of natural products showing inhibitory activity against pathogenic fungi cannot be considered without chemical characterization and identification of the compounds responsible for the inhibitory activity. JMM publishes (guest) editorials, original articles, reviews (and minireviews), case reports, technical notes, letters to the editor and information. Only clinical cases with real originality (new species, new clinical present action, new geographical localization, etc.), and fully documented (identification methods, results, etc.), will be considered. Under no circumstances does the journal guarantee publication before the editorial board makes its final decision. The journal is indexed in the main international databases and is accessible worldwide through the ScienceDirect and ClinicalKey platforms.
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