Antimalarials based on the arylpiperazine privileged substructure

Master Thesis

2005

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http://hdl.handle.net/11427/6342
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thesis_sci_2005_molyneaux_ca.pdf (7.83 MB)
Authors
Molyneaux, Carrie-Anne
Supervisors
Chibale, Kelly
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University of Cape Town

Department
Department of Chemistry
Faculty
Faculty of Science
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Abstract
Based on a previous study, arylpiperazines (2-chlorophenylpiperazine, 2-ethoxyphenylpiperazine and phenylpiperazine) were found to be significantly more potent against the chloroquine-resistant (K1) strain than against the chloroquine-sensitive(DIO) strain. In other studies, 8-hydroxy-2-(di-n-propylamino)tetralin (8-0H-DPAT) has been identified as a potential antimalarial agent for the inhibition of the 5-hydroxytryptamine type 1A receptor in Plasmodium falciparum. A number of arylpiperazines are also known to target this receptor in other systems. Coupled with the potential role of arylpiperazines as replacements for the antimalarial 8-OH-OPA T, these results prompted a further investigation into the antiplasmodial properties of a broader range of simple un substituted and substituted arylpiperazines against a broader range of chloroquine-sensitive and chloroquine-resistant strains of PlasmodiumJalciparum.
Description

Includes bibliographical references (leaves 118-124).

Keywords
Chemistry

Reference:

Molyneaux, C. 2005. Antimalarials based on the arylpiperazine privileged substructure. University of Cape Town.

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