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Identification of antimalarial targets of chloroquine by a combined deconvolution strategy of ABPP and MS-CETSA.

Peng GaoYan-Qing LiuWei XiaoFei XiaJia-Yun ChenLi-Wei GuFan YangLiu-Hai ZhengJun-Zhe ZhangQian ZhangZhi-Jie LiYu-Qing MengYong-Ping ZhuHuan TangQiao-Li ShiQiu-Yan GuoYing ZhangCheng-Chao XuLing-Yun DaiJi-Gang Wang
Published in: Military Medical Research (2022)
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.
Keyphrases
  • plasmodium falciparum
  • label free
  • mass spectrometry
  • multiple sclerosis
  • ms ms
  • binding protein
  • bioinformatics analysis