A novel multistage antiplasmodial inhibitor targeting Plasmodium falciparum histone deacetylase 1

Huang, Zhenghui; Li, Ruoxi; Tang, Tongke; Ling, Dazheng; Wang, Manjiong; Xu, Dandan; Sun, Maoxin; Zheng, Lulu; Zhu, Feng; Min, Hui; Boonhok, Rachasak; Ding, Yan; Wen, Yang; Chen, Zhong; Li, Xiaokang; Chen, Yuxi; Liu, Taiping; Han, Jiping; Miao, Jun; Fang, Qiang; Cao, Yaming; Tang, Yun; Cui, Jie; Xu, Wei; Cui, Liwang; Zhu, Jin; Wong, Gary; Li, Jian; Jiang, Lubin

doi:10.1038/s41421-020-00215-4

Cited by 27 publications

(37 citation statements)

References 72 publications

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“…Targeting pfEMP1 or factors regulating var variants is expected to be applied as potential antimalarial therapy and as adjuvant therapy in ACTs. The observed changes in the transcriptome and the membrane proteome strongly support this notion, and recent studies have also suggested exploiting chromatin and/or epigenetic regulators as drug targets in malarial diseases ( 37 – 39 ), providing evidence for our hypothesis of targeting pfEMP1 or factors regulating var variants in new antimalarial drug development.…”

Section: Discussionsupporting

confidence: 60%

Combined Transcriptome and Proteome Profiling for Role of pfEMP1 in Antimalarial Mechanism of Action of Dihydroartemisinin

et al. 2021

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Malaria parasites induce morphological and biochemical changes in the membranes of parasite-infected red blood cells (iRBCs) for propagation, with artemisinin combination therapies as the first-line treatments. To understand whether artemisinin targets or interacts with iRBC membrane proteins, this study investigated the molecular changes caused by dihydroartemisinin (DHA), an artemisinin derivative, in Plasmodium falciparum 3D7 using a combined transcriptomic and membrane proteomic profiling approach.

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Section: Discussionsupporting

confidence: 60%

Combined Transcriptome and Proteome Profiling for Role of pfEMP1 in Antimalarial Mechanism of Action of Dihydroartemisinin

et al. 2021

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“…These results indicated that the artemisinin resistance marker Pfk13 mutations are very complex and exhibited an increasing trend. Our study provides a strong theoretical basis for subsequent ACTs, but new mutant loci that are directly related to developing resistance by in vitro parasites require to be studied further using allelic exchange genetic modification methods, such as CRISPR/Cas9 genomic editing, combined with in vitro drug screening tests ( Xiao et al., 2019 ; Huang et al., 2020 ). The mechanism of action of artemisinin remains controversial, and our study provides some evidence of artemisinin drug resistance.…”

Section: Discussionmentioning

confidence: 99%

Ten-Year Molecular Surveillance of Drug-Resistant Plasmodium spp. Isolated From the China–Myanmar Border

Tang

Cao

et al. 2021

Front. Cell. Infect. Microbiol.

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Antimalarial drug resistance has emerged as a major threat to global malaria control efforts, particularly in the Greater Mekong Subregion (GMS). In this study, we analyzed the polymorphism and prevalence of molecular markers associated with resistance to first-line antimalarial drugs, such as artemisinin, chloroquine, and pyrimethamine, using blood samples collected from malaria patients in the China–Myanmar border region of the GMS from 2008 to 2017, including 225 cases of Plasmodium falciparum and 194 cases of Plasmodium vivax. In artemisinin resistance, only the C580Y mutation with low frequency was detected in pfk13, and no highly frequent stable mutation was found in pvk12. In chloroquine resistance, the frequency of K76T mutation in pfcrt was always high, and the frequency of double mutations in pvmdr1 of P. vivax has been steadily increasing every year. In pyrimidine resistance, pfdhfr and pvdhfr had relatively more complex mutant types associated with drug resistance sites, and the overall mutation rate was still high. Therefore, artemisinin-based combination therapies are still suitable for use as the first choice of antimalarial strategy in the China–Myanmar border region in the future.

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“…Although PfHDAC1 has been described as a target of multiple highly potent inhibitors, a thorough genetic and biological characterization of PfHDAC1 function is lacking in P. falciparum [19, 34-36]. To characterize its enzymatic activity, we cloned, expressed, and purified histidine- and GST-tagged PfHDAC1 (Figure 1A and 1B).…”

Section: Resultsmentioning

confidence: 99%

PfHDAC1 is an essential regulator of parasite asexual growth with its altered genomic occupancy and activity associated with artemisinin drug resistance in Plasmodium falciparum

Kanyal

Davies

Deshmukh

et al. 2022

Preprint

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Plasmodium falciparum is a deadly protozoan parasite and the causative agent of malaria, which accounts for close to 200 million cases and 400,000 deaths every year. It has been identified to possess a tightly regulated gene expression profile that is integrally linked to its timely development during the intraerythrocytic stage. Epigenetic modifiers of the histone acetylation code have been identified as key regulators of the parasite transcriptome. In this study, we characterize the solitary class I histone deacetylase PfHDAC1 and demonstrate that phosphorylation is required for its catalytic activity. PfHDAC1 binds to and regulates parasite genes responsible for housekeeping and stress-responsive functions. We show that PfHDAC1 activity in parasites is crucial for normal intraerythrocytic development and that its cellular abundance is correlated with parasitemia progression. We further show that PfHDAC1 has differential abundance and genomic occupancy in artemisinin drug-resistant vs sensitive parasites and that inhibition of its deacetylase activity can modulate the sensitivity of parasites to the drug. We also identify that artemisinin exposure can interfere with PfHDAC1 phosphorylation and its genomic occupancy. Collectively, our results demonstrate PfHDAC1 to be an important regulator of basic biological functions in parasites while also deterministic of responses to environmental stresses such as antimalarial drugs.

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A novel multistage antiplasmodial inhibitor targeting Plasmodium falciparum histone deacetylase 1

Cited by 27 publications

References 72 publications

Combined Transcriptome and Proteome Profiling for Role of pfEMP1 in Antimalarial Mechanism of Action of Dihydroartemisinin

Combined Transcriptome and Proteome Profiling for Role of pfEMP1 in Antimalarial Mechanism of Action of Dihydroartemisinin

Ten-Year Molecular Surveillance of Drug-Resistant Plasmodium spp. Isolated From the China–Myanmar Border

PfHDAC1 is an essential regulator of parasite asexual growth with its altered genomic occupancy and activity associated with artemisinin drug resistance in Plasmodium falciparum

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