利用新型高效液相色谱-串联质谱法和抗真菌唑类化合物作为化学探针对利什曼原虫的甾醇进行分析,揭示了一种支持支链麦角甾醇生物合成途径的关键中间体甾醇

Mei Feng , Yiru Jin , Sihyung Yang , Arline M. Joachim , Yu Ning , Luis M. Mori-Quiroz , Jacob Fromm , Chamani Perera , Kai Zhang , Karl A. Werbovetz , Michael Zhuo Wang
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引用次数: 4

摘要

人类利什曼病是一种由利什曼原虫寄生虫引起的传染病。目前针对这种致命疾病的化疗方案有很大的局限性。麦角甾醇生物合成途径已被确定为利什曼原虫的药物靶点。然而,抑制麦角甾醇生物合成的抗真菌唑类药物治疗利什曼病的疗效有显著差异。为了更好地了解利什曼原虫的甾醇生物合成途径,阐明抗真菌唑类药物疗效差异的机制,我们建立了一种新的LC-MS/MS方法,研究了3种利什曼原虫(L. donovani, L. major和L. tarentolae)原鞭毛体中的甾醇谱。使用新开发的LC-MS/MS方法,不同前体离子质量和LC保留时间的组合允许对羊毛甾醇和麦角甾醇之间的16种中间甾醇进行特异性检测。虽然泊沙康唑和氟康唑都是已知的真菌羊毛甾醇14α-去甲基化酶(CYP51)的抑制剂,但只有泊沙康唑导致了唑处理的L. donovani promastigotes羊毛甾醇的大量积累。通过高分辨质谱和核磁共振分析,分别测定了泊沙康唑和氟康唑处理后的一种关键中间体甾醇为4α、14α-二甲基酶甾醇,分别积累了40倍和7倍。4α,14α-二甲基化酶甾醇的鉴定支持利什曼原虫分支麦角甾醇生物合成途径,其中羊毛甾醇C4-和c14 -去甲基化反应平行而不是顺序发生。我们的研究结果表明,选择性抑制利什曼CYP51不足以有效地阻止寄生虫的生长,可能需要CYP51和未知的固醇c4 -去甲基化酶的双重抑制剂才能达到最佳的抗寄生虫效果。
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Sterol profiling of Leishmania parasites using a new HPLC-tandem mass spectrometry-based method and antifungal azoles as chemical probes reveals a key intermediate sterol that supports a branched ergosterol biosynthetic pathway

Human leishmaniasis is an infectious disease caused by Leishmania protozoan parasites. Current chemotherapeutic options against the deadly disease have significant limitations. The ergosterol biosynthetic pathway has been identified as a drug target in Leishmania. However, remarkable differences in the efficacy of antifungal azoles that inhibit ergosterol biosynthesis have been reported for the treatment of leishmaniasis. To better understand the sterol biosynthetic pathway in Leishmania and elucidate the mechanism underlying the differential efficacy of antifungal azoles, we developed a new LC-MS/MS method to study sterol profiles in promastigotes of three Leishmania species, including two L. donovani, one L. major and one L. tarentolae strains. A combination of distinct precursor ion masses and LC retention times allowed for specific detection of sixteen intermediate sterols between lanosterol and ergosterol using the newly developed LC-MS/MS method. Although both posaconazole and fluconazole are known inhibitors of fungal lanosterol 14α-demethylase (CYP51), only posaconazole led to a substantial accumulation of lanosterol in azole-treated L. donovani promastigotes. Furthermore, a key intermediate sterol accumulated by 40- and 7-fold when these parasites were treated with posaconazole and fluconazole, respectively, which was determined as 4α,14α-dimethylzymosterol by high resolution mass spectrometry and NMR spectroscopy. The identification of 4α,14α-dimethylzymosterol supports a branched ergosterol biosynthetic pathway in Leishmania, where lanosterol C4- and C14-demethylation reactions occur in parallel rather than sequentially. Our results suggest that selective inhibition of leishmanial CYP51 is insufficient to effectively prevent parasite growth and dual inhibitors of both CYP51 and the unknown sterol C4-demethylase may be required for optimal antiparasitic effect.

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来源期刊
CiteScore
7.90
自引率
7.50%
发文量
31
审稿时长
48 days
期刊介绍: The International Journal for Parasitology – Drugs and Drug Resistance is one of a series of specialist, open access journals launched by the International Journal for Parasitology. It publishes the results of original research in the area of anti-parasite drug identification, development and evaluation, and parasite drug resistance. The journal also covers research into natural products as anti-parasitic agents, and bioactive parasite products. Studies can be aimed at unicellular or multicellular parasites of human or veterinary importance.
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