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Pharmacological properties of a new antimalarial bisthiazolium salt, T3, and a corresponding prodrug, TE3.

Identifieur interne : 000337 ( France/Analysis ); précédent : 000336; suivant : 000338

Pharmacological properties of a new antimalarial bisthiazolium salt, T3, and a corresponding prodrug, TE3.

Auteurs : Olivier Nicolas [France] ; Delphine Margout [France] ; Nicolas Taudon [France] ; Sharon Wein [France] ; Michèle Calas [France] ; Henri J. Vial [France] ; Françoise M M. Bressolle [France]

Source :

RBID : Hal:hal-00116879

Abstract

A new approach to malarial chemotherapy based on quaternary ammonium that targets membrane biogenesis during intraerythrocytic Plasmodium falciparum development has recently been developed. To increase the bioavailability, nonionic chemically modified prodrugs were synthesized. In this paper, the pharmacological properties of a bisthiazolium salt (T3) and its bioprecursor (TE3) were studied. Their antimalarial activities were determined in vitro against the growth of P. falciparum and in vivo against the growth of P. vinckei in mice. Pharmacokinetic evaluations were performed after T3 (1.3 and 3 mg/kg of body weight administered intravenously; 6.4 mg/kg administered intraperitoneally) and TE3 (1.5 and 3 mg/kg administered intravenously; 12 mg/kg administered orally) administrations to rats. After intraperitoneal administration, very low doses offer protection in a murine model of malaria (50% efficient dose [ED50] of 0.2 to 0.25 mg/kg). After oral administration, the ED50 values were 13 and 5 mg/kg for T3 and TE3, respectively. Both compounds exerted antimalarial activity in the low nanomolar range. After TE3 administration, rapid prodrug-drug conversion occurred; the mean values of the pharmacokinetic parameters for T3 were as follows: total clearance, 1 liter/h/kg; steady-state volume of distribution, 14.8 liters/kg; and elimination half-life, 12 h. After intravenous administration, T3 plasma concentrations increased in proportion to the dose. The absolute bioavailability was 72% after intraperitoneal administration (T3); it was 15% after oral administration (TE3). T3 plasma concentrations (8 nM) 24 h following oral administration of TE3 were higher than the 50% inhibitory concentrations for the most chloroquine-resistant strains of P. falciparum (6.3 nM).


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DOI: 10.1128/AAC.49.9.3631-3639.2005


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<author>
<name sortKey="Bressolle, Francoise M M" sort="Bressolle, Francoise M M" uniqKey="Bressolle F" first="Françoise M M" last="Bressolle">Françoise M M. Bressolle</name>
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<hal:affiliation type="laboratory" xml:id="struct-150387" status="OLD">
<orgName>Laboratoire de Chimie des Biomolécules et de l'Environnement</orgName>
<orgName type="acronym">LCBE</orgName>
<desc>
<address>
<addrLine>Via Domitia, UPVD, 52 avenue Paul Alduy, 66860 Perpignan Cedex 9</addrLine>
<country key="FR"></country>
</address>
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<orgName>Université de Perpignan Via Domitia</orgName>
<orgName type="acronym">UPVD</orgName>
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<address>
<addrLine>52 avenue Paul Alduy - 66860 Perpignan Cedex 9</addrLine>
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<orgName>Université Montpellier 1</orgName>
<orgName type="acronym">UM1</orgName>
<date type="end">2014-12-31</date>
<desc>
<address>
<addrLine>5, boulevard Henri IV - CS 19044 - 34967 Montpellier cedex</addrLine>
<country key="FR"></country>
</address>
<ref type="url">http://www.univ-montp1.fr/</ref>
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</hal:affiliation>
<country>France</country>
<placeName>
<settlement type="city">Montpellier</settlement>
<region type="region" nuts="2">Occitanie (région administrative)</region>
<region type="old region" nuts="2">Languedoc-Roussillon</region>
</placeName>
<orgName type="university">Université de Perpignan</orgName>
<orgName type="institution" wicri:auto="newGroup">PRES Sud de France</orgName>
<placeName>
<settlement type="city">Montpellier</settlement>
<region type="region" nuts="2">Occitanie (région administrative)</region>
<region type="old region" nuts="2">Languedoc-Roussillon</region>
</placeName>
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<idno type="DOI">10.1128/AAC.49.9.3631-3639.2005</idno>
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<front>
<div type="abstract" xml:lang="en">
<p>A new approach to malarial chemotherapy based on quaternary ammonium that targets membrane biogenesis during intraerythrocytic Plasmodium falciparum development has recently been developed. To increase the bioavailability, nonionic chemically modified prodrugs were synthesized. In this paper, the pharmacological properties of a bisthiazolium salt (T3) and its bioprecursor (TE3) were studied. Their antimalarial activities were determined in vitro against the growth of P. falciparum and in vivo against the growth of P. vinckei in mice. Pharmacokinetic evaluations were performed after T3 (1.3 and 3 mg/kg of body weight administered intravenously; 6.4 mg/kg administered intraperitoneally) and TE3 (1.5 and 3 mg/kg administered intravenously; 12 mg/kg administered orally) administrations to rats. After intraperitoneal administration, very low doses offer protection in a murine model of malaria (50% efficient dose [ED50] of 0.2 to 0.25 mg/kg). After oral administration, the ED50 values were 13 and 5 mg/kg for T3 and TE3, respectively. Both compounds exerted antimalarial activity in the low nanomolar range. After TE3 administration, rapid prodrug-drug conversion occurred; the mean values of the pharmacokinetic parameters for T3 were as follows: total clearance, 1 liter/h/kg; steady-state volume of distribution, 14.8 liters/kg; and elimination half-life, 12 h. After intravenous administration, T3 plasma concentrations increased in proportion to the dose. The absolute bioavailability was 72% after intraperitoneal administration (T3); it was 15% after oral administration (TE3). T3 plasma concentrations (8 nM) 24 h following oral administration of TE3 were higher than the 50% inhibitory concentrations for the most chloroquine-resistant strains of P. falciparum (6.3 nM).</p>
</div>
</front>
</TEI>
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<li>France</li>
</country>
<region>
<li>Languedoc-Roussillon</li>
<li>Occitanie (région administrative)</li>
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<region name="Occitanie (région administrative)">
<name sortKey="Nicolas, Olivier" sort="Nicolas, Olivier" uniqKey="Nicolas O" first="Olivier" last="Nicolas">Olivier Nicolas</name>
</region>
<name sortKey="Bressolle, Francoise M M" sort="Bressolle, Francoise M M" uniqKey="Bressolle F" first="Françoise M M" last="Bressolle">Françoise M M. Bressolle</name>
<name sortKey="Calas, Michele" sort="Calas, Michele" uniqKey="Calas M" first="Michèle" last="Calas">Michèle Calas</name>
<name sortKey="Margout, Delphine" sort="Margout, Delphine" uniqKey="Margout D" first="Delphine" last="Margout">Delphine Margout</name>
<name sortKey="Taudon, Nicolas" sort="Taudon, Nicolas" uniqKey="Taudon N" first="Nicolas" last="Taudon">Nicolas Taudon</name>
<name sortKey="Vial, Henri J" sort="Vial, Henri J" uniqKey="Vial H" first="Henri J" last="Vial">Henri J. Vial</name>
<name sortKey="Wein, Sharon" sort="Wein, Sharon" uniqKey="Wein S" first="Sharon" last="Wein">Sharon Wein</name>
</country>
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</affiliations>
</record>

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