Identification of Antimalarial Targets of Chloroquine by a Combined Deconvolution Strategy of ABPP and MS-CETSA

Overview

Journal Mil Med Res

Publisher Biomed Central

Specialty Emergency Medicine

Date 2022 Jun 13

PMID 35698214

Authors

Peng Gao

Yan-Qing Liu

Wei Xiao

Fei Xia

Jia-Yun Chen

Li-Wei Gu

Fan Yang

Liu-Hai Zheng

Jun-Zhe Zhang

Qian Zhang

Zhi-Jie Li

Yu-Qing Meng

Yong-Ping Zhu

Huan Tang

Qiao-Li Shi

Qiu-Yan Guo

Ying Zhang

Cheng-Chao Xu

Ling-Yun Dai

Ji-Gang Wang

Affiliations

Soon will be listed here.

Abstract

Background: Malaria is a devastating infectious disease that disproportionally threatens hundreds of millions of people in developing countries. In the history of anti-malaria campaign, chloroquine (CQ) has played an indispensable role, however, its mechanism of action (MoA) is not fully understood.

Methods: We used the principle of photo-affinity labeling and click chemistry-based functionalization in the design of a CQ probe and developed a combined deconvolution strategy of activity-based protein profiling (ABPP) and mass spectrometry-coupled cellular thermal shift assay (MS-CETSA) that identified the protein targets of CQ in an unbiased manner in this study. The interactions between CQ and these identified potential protein hits were confirmed by biophysical and enzymatic assays.

Results: We developed a novel clickable, photo-affinity chloroquine analog probe (CQP) which retains the antimalarial activity in the nanomole range, and identified a total of 40 proteins that specifically interacted and photo-crosslinked with CQP which was inhibited in the presence of excess CQ. Using MS-CETSA, we identified 83 candidate interacting proteins out of a total of 3375 measured parasite proteins. At the same time, we identified 8 proteins as the most potential hits which were commonly identified by both methods.

Conclusions: We found that CQ could disrupt glycolysis and energy metabolism of malarial parasites through direct binding with some of the key enzymes, a new mechanism that is different from its well-known inhibitory effect of hemozoin formation. This is the first report of identifying CQ antimalarial targets by a parallel usage of labeled (ABPP) and label-free (MS-CETSA) methods.

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