Discovery of Leishmania Druggable Serine Proteases by Activity-Based Protein Profiling

蛋白酵素 可药性 利什曼原虫 丝氨酸 药物发现 生物 丝氨酸水解酶 墨西哥利什曼原虫 丝氨酸蛋白酶 蛋白质组学 丝氨酸蛋白酶抑制剂 生物化学 药理学 蛋白酶 计算生物学 万维网 基因 寄生虫寄主 计算机科学
作者
Exequiel O. J. Porta,Jaime Isern,Karunakaran Kalesh,Patrick G. Steel
出处
期刊:Frontiers in Pharmacology [Frontiers Media SA]
卷期号:13 被引量:7
标识
DOI:10.3389/fphar.2022.929493
摘要

Leishmaniasis are a group of diseases caused by parasitic protozoa of the genus Leishmania. Current treatments are limited by difficult administration, high cost, poor efficacy, toxicity, and growing resistance. New agents, with new mechanisms of action, are urgently needed to treat the disease. Although extensively studied in other organisms, serine proteases (SPs) have not been widely explored as antileishmanial drug targets. Herein, we report for the first time an activity-based protein profiling (ABPP) strategy to investigate new therapeutic targets within the SPs of the Leishmania parasites. Active-site directed fluorophosphonate probes (rhodamine and biotin-conjugated) were used for the detection and identification of active Leishmania serine hydrolases (SHs). Significant differences were observed in the SHs expression levels throughout the Leishmania life cycle and between different Leishmania species. Using iTRAQ-labelling-based quantitative proteomic mass spectrometry, we identified two targetable SPs in Leishmania mexicana: carboxypeptidase LmxM.18.0450 and prolyl oligopeptidase LmxM.36.6750. Druggability was ascertained by selective inhibition using the commercial serine protease inhibitors chymostatin, lactacystin and ZPP, which represent templates for future anti-leishmanial drug discovery programs. Collectively, the use of ABPP method complements existing genetic methods for target identification and validation in Leishmania.
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