N-Myristoyltransferase inhibition as a tool for antileishmanial drug discovery: Use in high-throughput, de novo, and piggyback strategies for drug development

Kavouris, John (2014) N-Myristoyltransferase inhibition as a tool for antileishmanial drug discovery: Use in high-throughput, de novo, and piggyback strategies for drug development. Master's Thesis, University of Pittsburgh. (Unpublished)

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Abstract

Leishmaniasis is a disease caused by the Leishmania genus of protozoan parasites, and spread by the phlebotomine genus of sandfly. The disease is caused by at least 20 different species of Leishmania parasites, and manifests itself in three forms: cutaneous, mucocutaneous, and most severely, visceral leishmaniasis. Current chemotherapeutic treatments for leishmaniasis are limited by parasite resistance to existing drugs, highly toxic side effects, and high cost of treatment. As a neglected tropical disease, there has been relatively little research toward new drugs, despite a large need, comprising 1.3m new cases and 20,000-50,000 deaths annually. Fortunately, although there is a wide variety in species causing the disease, visceral leishmaniasis is largely caused by a single species of parasite, Leishmania donovani, greatly simplifying the search for drugs against the most dangerous form of the disease. The whole genome of the species has been sequenced, and many crystal structures of key proteins have been elucidated. Specifically, N-myristoyltransferase (NMT) has emerged as a promising enzyme for target-based antileishmanial drug development, with a wide array of tools available for any level of drug discovery: in silico modeling and docking, enzyme specific assays for protozoan and human isoforms, high throughput in vitro assays against both the parasite itself and infected host cells, and animal models of the disease. However, with L. donovani NMT as a newer target, research has yet to utilize all of these individual elements synergistically with themselves, or with related studies in different parasite species. Combined analysis of these methods can yield a more efficient search for antileishmanials, regardless of screening type.

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Details

Item Type:	University of Pittsburgh ETD
Status:	Unpublished
Creators/Authors:	Creators Email Pitt Username ORCID Kavouris, John jak208@pitt.edu JAK208
ETD Committee:	Title Member Email Address Pitt Username ORCID Committee Chair Nelson, Scott G. sgnelson@pitt.edu SGNELSON Committee Member Gold, Barry I. goldbi@pitt.edu GOLDBI Committee Member Horne, W. Seth horne@pitt.edu HORNE
Date:	15 September 2014
Date Type:	Publication
Defense Date:	25 April 2014
Approval Date:	15 September 2014
Submission Date:	6 June 2014
Access Restriction:	No restriction; Release the ETD for access worldwide immediately.
Number of Pages:	62
Institution:	University of Pittsburgh
Schools and Programs:	Dietrich School of Arts and Sciences > Chemistry
Degree:	MS - Master of Science
Thesis Type:	Master's Thesis
Refereed:	Yes
Uncontrolled Keywords:	Leishmaniasis, leishmania donovani, visceral leishmaniasis, neglected tropical diseases, N-myristoyltransferase
Date Deposited:	15 Sep 2014 17:40
Last Modified:	15 Nov 2016 14:23
URI:	http://d-scholarship.pitt.edu/id/eprint/22670

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• N-Myristoyltransferase inhibition as a tool for antileishmanial drug discovery: Use in high-throughput, de novo, and piggyback strategies for drug development. (deposited 15 Sep 2014 17:40) [Currently Displayed]

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