Candida albicans ergosterol disorders as a consequence of the new sulfone derivative action mode

IF 2.6 4区 医学 Q3 CHEMISTRY, MEDICINAL
Monika Staniszewska, Michalina Kazek, Marta Rogalska, Anna Wojewódzka, Łukasz Kuryk, Zbigniew Ochal
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Abstract

A series of novel sulfone derivatives were synthesized and screened in vitro for their cytotoxicity and antifungal activity with annotated primary mechanism of action (MOA). We prioritized sulfones with high (4-(bromodichloromethylsulfonyl)benzoic acid 4, 4-(difluoromethylsulfonyl)benzoic acid 12), little (3-[4-(bromodichloromethylsulfonyl)phenyl]propanoic acid 8, difluoromethyl 4-methylphenyl sulfone 11, 4-(difluoromethylsulfonyl)benzoic acid 12), or no cytotoxicity of 4-(4-(dichloromethylsulfonyl)benzoic acid 3) and 3-[4-(dichloromethylsulfonyl)phenyl]propanoic acid 7 against mammalian cell lines. 3 was found to be the most potent sulfone against Candida albicans (Rlog=7.25 at 128–256 µg/mL). The mutation in the CNB1 gene (1) increased the sensitivity of the C. albicans biofilm to 3; (2) reduced ergosterol production and therefore generated higher susceptibility to 4. Sulfone 4 at 128 µg/mL increased cellular RH-123 fluorescence in the wild-type cells of C. albicans, except CNB1/cnb1∆. Moreover, the uptake of sulfones into the cell was unaffected regardless of the presence or absence of RH-123, and the uptake of sulfones was strictly cell/strain dependent. Both RH123 and sulfones cumulatively competed with one another for access to transporters. Calcineurin played a role in this mechanism.

Abstract Image

新型砜衍生物作用模式导致白色念珠菌麦角固醇紊乱
我们合成了一系列新型砜衍生物,并对其细胞毒性和抗真菌活性进行了体外筛选,同时注释了主要作用机制(MOA)。我们优先选择了毒性高(4-(溴二氯甲基砜基)苯甲酸 4、4-(二氟甲基砜基)苯甲酸 12)、毒性低(3-[4-(溴二氯甲基砜基)苯基]丙酸 8、二氟甲基 4-甲基苯砜 11)的砜类衍生物、4-(4-(二氯甲基磺酰基)苯甲酸 3)和 3-[4-(二氯甲基磺酰基)苯基]丙酸 7 对哺乳动物细胞株无细胞毒性。结果发现,3 是对白色念珠菌最有效的砜类化合物(在 128-256 微克/毫升浓度下,Rlog=7.25)。CNB1 基因突变(1)增加了白念珠菌生物膜对 3 的敏感性;(2)减少了麦角固醇的产生,因此对 4 产生了更高的敏感性。除了 CNB1/cnb1∆,128 µg/mL 的砜 4 增加了白念珠菌野生型细胞的细胞 RH-123 荧光。此外,无论是否存在 RH-123,细胞对砜类化合物的吸收都不受影响,而且砜类化合物的吸收严格依赖于细胞/菌株。RH123 和砜类在进入转运体时相互累积竞争。降钙素在这一机制中发挥了作用。
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来源期刊
Medicinal Chemistry Research
Medicinal Chemistry Research 医学-医药化学
CiteScore
4.70
自引率
3.80%
发文量
162
审稿时长
5.0 months
期刊介绍: Medicinal Chemistry Research (MCRE) publishes papers on a wide range of topics, favoring research with significant, new, and up-to-date information. Although the journal has a demanding peer review process, MCRE still boasts rapid publication, due in part, to the length of the submissions. The journal publishes significant research on various topics, many of which emphasize the structure-activity relationships of molecular biology.
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