Inhibition of
            <i>Plasmodium falciparum</i>
            Choline Kinase by Hexadecyltrimethylammonium Bromide: a Possible Antimalarial Mechanism

Choubey, Vinay; Maity, Pallab; Guha, Mithu; Kumar, Sanjeev; Srivastava, Kumkum; Puri, Sunil K.; Bandyopadhyay, Uday

doi:10.1128/aac.00919-06

Cited by 64 publications

(54 citation statements)

References 42 publications

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“…Once the proof-of-principle that ChoKa is a validated target in oncology has been set up, a very intensive activity has been developed for the identification of novel ChoKa inhibitors with potential use as antitumoral drugs (15)(16)(17)(18)(19)(20)(28)(29)(30)(31) and also as antiparasitic compounds (32,33).…”

Section: Introductionmentioning

confidence: 99%

Preclinical Characterization of RSM-932A, a Novel Anticancer Drug Targeting the Human Choline Kinase Alpha, an Enzyme Involved in Increased Lipid Metabolism of Cancer Cells

Lacal

Campos

2015

Molecular Cancer Therapeutics

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Choline kinase a (CHKA; here designated as ChoKa) is the first enzyme in the CDP-choline pathway, implicated in phospholipids metabolism. It is overexpressed in several human tumors such as breast, lung, bladder, colorectal, prostate, ovary, and liver. The overexpression of ChoKa has oncogenic potential and synergizes with other known oncogenes. It has been proposed as a novel cancer drug target with a distinct mechanism of action. We have generated a set of ChoKa inhibitors with potent in vitro antiproliferative and in vivo antitumoral activity against human xenografts in mice, showing high efficacy with low toxicity profiles. Among these inhibitors, RSM-932A has been chosen for further clinical development due to its potent antiproliferative activity in vitro against a large variety of tumorderived cell lines, a potent in vivo anticancer activity, and lack of toxicity at the effective doses. Here, we provide the preclinical evidence to support the use of RSM-932A as a good candidate to be tested in clinical trials as the "first in humans" drug targeting ChoKa.

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Section: Introductionmentioning

confidence: 99%

Preclinical Characterization of RSM-932A, a Novel Anticancer Drug Targeting the Human Choline Kinase Alpha, an Enzyme Involved in Increased Lipid Metabolism of Cancer Cells

Lacal

Campos

2015

Molecular Cancer Therapeutics

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“…The primary sequence of the catalytic site (12) and the tertiary structure (PDB 3FI8; www.pdb.org) of p.f.-ChoK are conserved with respect to other ChoKs. Furthermore, p.f.-ChoK is more highly expressed in growth phases of P. falciparum (12), and inhibition of ChoK affects the parasite's viability in in vitro and mouse models of malaria (13). HC-3 has been shown to inhibit recombinant p.f.-ChoK (14) and to be lethal against the parasite (15).…”

mentioning

confidence: 99%

Antiplasmodial Activity and Mechanism of Action of RSM-932A, a Promising Synergistic Inhibitor of Plasmodium falciparum Choline Kinase

Zimmerman

Moneriz

Díez

et al. 2013

Antimicrob Agents Chemother

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“…The mode of action of miltefosine against Leishmania parasites involves the interaction with membrane phospholipids and sterols, and the drug interferes with the functionality of a number of enzymes involved in phospholipid metabolism such as protein kinase C and the phospholipases A, C and D, finally leading to apoptosis (Barratt et al 2009). Hexadecyltrimethylammonium bromide, a compound structurally similar to miltefosine, was demonstrated to exhibit potent in vitro activity against Plasmodium falciparum (Walochnik et al 2002;Schuster et al 2006;Choubey et al 2007).…”

Section: Introductionmentioning

confidence: 99%

Effects of miltefosine treatment in fibroblast cell cultures and in mice experimentally infected withNeospora caninumtachyzoites

Debache

Hemphill

2012

Parasitology

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SUMMARYMiltefosine was investigated for its activity againstNeospora caninumtachyzoitesin vitro,and was shown to inhibit the proliferation ofN. caninumtachyzoites cultured in human foreskin fibroblasts (HFF) with an IC50of 5·2μM. Treatment of infected cells with 25μM miltefosine for a period of 10 h had only a parasitostatic effect, while after 20 h of treatment parasiticidal effects were observed. This was confirmed by transmission electron microscopy ofN. caninum-infected and miltefosine-treated HFF. Administration of miltefosine toN. caninum-infected Balb/c female mice at 40 mg/kg/day for 14 days resulted in 6 out of 10 mice exhibiting weight loss, ruffled coat and apathy between days 7 and 13 post-infection. In the group that received placebo, only 2 out of 8 mice succumbed to infection, but the cerebral burden was significantly higher compared to the miltefosine treatment group. In a second experiment, the time-span of treatment was reduced to 5 days, and mice were maintained without further treatment for 4 weeks. Only 2 out of 9 mice in the miltefosine treatment group exhibited signs of disease, while 8 out of 10 mice succumbed to infection in the placebo group. These results showed that miltefosine hampered the dissemination of parasites into the CNS during experimentalN. caninuminfection in mice.

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Inhibition of Plasmodium falciparum Choline Kinase by Hexadecyltrimethylammonium Bromide: a Possible Antimalarial Mechanism

Cited by 64 publications

References 42 publications

Preclinical Characterization of RSM-932A, a Novel Anticancer Drug Targeting the Human Choline Kinase Alpha, an Enzyme Involved in Increased Lipid Metabolism of Cancer Cells

Preclinical Characterization of RSM-932A, a Novel Anticancer Drug Targeting the Human Choline Kinase Alpha, an Enzyme Involved in Increased Lipid Metabolism of Cancer Cells

Antiplasmodial Activity and Mechanism of Action of RSM-932A, a Promising Synergistic Inhibitor of Plasmodium falciparum Choline Kinase

Effects of miltefosine treatment in fibroblast cell cultures and in mice experimentally infected withNeospora caninumtachyzoites

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