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  5. Understanding the structural basis of species selective, stereospecific inhibition for <i>Cryptosporidium</i> and human thymidylate synthase

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Article
English
2019

Understanding the structural basis of species selective, stereospecific inhibition for <i>Cryptosporidium</i> and human thymidylate synthase

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English
2019
FEBS Letters
Vol 593 (15)
DOI: 10.1002/1873-3468.13474

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William L. Jorgensen
William L. Jorgensen

Yale University

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Daniel J. Czyzyk
Margarita Valhondo
William L. Jorgensen
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Abstract

Thymidylate synthase (TS), found in all organisms, is an essential enzyme responsible for the de novo synthesis of deoxythymidine monophosphate. The TS active sites of the protozoal parasite Cryptosporidium hominis and human are relatively conserved. Evaluation of antifolate compound 1 and its R-enantiomer 2 against both enzymes reveals divergent inhibitor selectivity and enzyme stereospecificity. To establish how C. hominis and human TS (ChTS and hTS) selectively discriminate 1 and 2, respectively, we determined crystal structures of ChTS complexed with 2 and hTS complexed with 1 or 2. Coupled with the previously determined structure of ChTS complexed with 1, we discuss a possible mechanism for enzyme stereospecificity and inhibitor selectivity.

How to cite this publication

Daniel J. Czyzyk, Margarita Valhondo, William L. Jorgensen, Karen S. Anderson (2019). Understanding the structural basis of species selective, stereospecific inhibition for <i>Cryptosporidium</i> and human thymidylate synthase. FEBS Letters, 593(15), pp. 2069-2078, DOI: 10.1002/1873-3468.13474.

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Publication Details

Type

Article

Year

2019

Authors

4

Datasets

0

Total Files

0

Language

English

Journal

FEBS Letters

DOI

10.1002/1873-3468.13474

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