Candida albicans is a common opportunistic fungal pathogen that may cause nosocomial fungal infections. The resistance of Candida albicans to traditional antifungal drugs has been increasing rapidly in recent years, and it brings a great challenge in clinical treatment. N-butylphthalide is originally extracted from the seed of Apium graveolens and is currently used for the treatment of ischemic stroke in the clinic. This study demonstrated that n-butylphthalide exhibited antifungal activity against Candida albicans with minimum inhibitory concentrations of 128 mu g/ml; moreover, n-butylphthalide combined with fluconazole showed synergistic antifungal effects against resistant Candida albicans, resulting in a decrease in the minimum inhibitory concentrations of fluconazole from >512 to 0.25-1 mu g/ml. Time-killing curves verified the antifungal activity in dynamic. Besides, n-butylphthalide exhibited antibiofilm activity against Candida albicans, biofilms preformed < 12 h with sessile minimum inhibitory concentrations of 128-256 mu g/ml and synergism was observed when n-butylphthalide combined with fluconazole against resistant Candida albicans biofilms preformed < 12 h, resulting in a decrease in the sessile minimum inhibitory concentrations of fluconazole from >1,024 to 0.5-8 mu g/ml. Furthermore, in vitro antifungal effects of n-butylphthalide were confirmed in vivo. N-butylphthalide prolonged survival rate of larvae infected by Candida albicans, reduced the fungal burden in larvae and caused less damage to larval tissues. Notably, n-butylphthalide inhibited hyphal growth and induced intracellular reactive oxygen species accumulation and a loss in mitochondrial membrane potential, which was a potential antifungal mechanism. Besides, the synergistic effects between n-butylphthalide and fluconazole potentially relied on the mechanism that n-butylphthalide significantly promoted drug uptake, and suppressed drug efflux via down-regulating the drug transporter encoding genes CDR1 and CDR2. These findings demonstrated the antifungal effects and mechanisms of n-butylphthalide against Candida albicans for the first time, which might provide broad prospects for the identification of new potential antifungal targets.
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Univ Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, IrelandUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
Higgins, J.
Pinjon, E.
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Univ Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, IrelandUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
Pinjon, E.
Oltean, H. N.
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Seattle Biomed Res Inst, Seattle, WA 98109 USAUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
Oltean, H. N.
White, T. C.
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Seattle Biomed Res Inst, Seattle, WA 98109 USAUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
White, T. C.
Kelly, S. L.
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Swansea Univ, Inst Life Sci, Swansea SA2 8PP, W Glam, Wales
Swansea Univ, Sch Med, Swansea SA2 8PP, W Glam, WalesUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
Kelly, S. L.
Martel, C. M.
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Swansea Univ, Inst Life Sci, Swansea SA2 8PP, W Glam, Wales
Swansea Univ, Sch Med, Swansea SA2 8PP, W Glam, WalesUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
Martel, C. M.
Sullivan, D. J.
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Univ Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, IrelandUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
Sullivan, D. J.
Coleman, D. C.
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Univ Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, IrelandUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
Coleman, D. C.
Moran, G. P.
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Univ Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, IrelandUniv Dublin Trinity Coll, Dublin Dent Univ Hosp, Div Oral Biosci, Microbiol Res Unit, Dublin 2, Ireland
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Kerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Norozipor, Sara
Bamorovat, Mehdi
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Kerman Univ Med Sci, Leishmaniasis Res Ctr, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Bamorovat, Mehdi
Mosavi, Seyyed Amin Ayatollahi
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Kerman Univ Med Sci, Med Mycol & Bacteriol Res Ctr, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Mosavi, Seyyed Amin Ayatollahi
Salarkia, Ehsan
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Kerman Univ Med Sci, Leishmaniasis Res Ctr, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Salarkia, Ehsan
Hadizadeh, Sanaz
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Kerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Hadizadeh, Sanaz
Shari, Fatemeh
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Kerman Univ Med Sci, Res Ctr Trop & Infect Dis, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Shari, Fatemeh
Karamoozian, Ali
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Kerman Univ Med Sci, Fac Hlth, Dept Biostat & Epidemiol, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Karamoozian, Ali
Ranjbar, Mehdi
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Kerman Univ Med Sci, Inst Neuropharmacol, Pharmaceut Res Ctr, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Ranjbar, Mehdi
Afshari, Setareh Agha Kuchak
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Kerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran
Kerman Univ Med Sci, Med Mycol & Bacteriol Res Ctr, Kerman, IranKerman Univ Med Sci, Afzalipour Fac Med, Dept Med Parasitol & Mycol, Kerman, Iran