Use this URL to cite or link to this record in EThOS: https://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.754782
Title: Synthesis and biological evaluation of three novel antimalarial series
Author: Tunstall, Lucy Victoria
ISNI:       0000 0004 7427 8021
Awarding Body: Keele University
Current Institution: Keele University
Date of Award: 2018
Availability of Full Text:
Access from EThOS:
Access from Institution:
Abstract:
This research explored the optimisation of three novel antimalarial series based on the MMV compound leads shown below. Extensive research began to optimise these potent hits through exploration of multiple functional group substitutions on two or more sites of the core structure (shown above). The highest activity tetrahydro-β-carboline analogue discovered during this research was LVT30 (IC50=1μM) which possesses an absent C3 interaction and a p-trifluoromethyl R2 substitution. Meanwhile, of the spirocyclic subset of derivatives, a high nanomolar activity compound was generated LVT86 (IC50=960 nM), possessing a butyl R1 chain and a m-trifluoromethyl R2 group and future work will include optimisation of this analogues pharmacokinetic properties. The most fruitful subseries of this project was a catalogue of 2-iminobenzimidazole compounds. In an attempt to optimise activity and increase potency, exploration involved variation of all three R positions and as a result, generated the most potent derivative over all three series. Compound LVTa95 possesses an inhibitory concentration of 33.4 nM and exhibits: a pentane R1 group, 2,4-dichloro R2 substitution and a hydroxy R3 group. As this compound existed as enantiomers, they were subsequently separated, and it was found both stereoisomers had similar activity.
Supervisor: Phillips, Tess ; Edwards, Mike Sponsor: Not available
Qualification Name: Thesis (Ph.D.) Qualification Level: Doctoral
EThOS ID: uk.bl.ethos.754782  DOI: Not available
Keywords: Q Science (General)
Share: