Literature DB >> 24100331

Conformational changes in human prolyl-tRNA synthetase upon binding of the substrates proline and ATP and the inhibitor halofuginone.

Jonghyeon Son1, Eun Hye Lee, Minyoung Park, Jong Hyun Kim, Junsoo Kim, Sunghoon Kim, Young Ho Jeon, Kwang Yeon Hwang.   

Abstract

Aminoacyl-tRNA synthetases recognize cognate amino acids and tRNAs from their noncognate counterparts and catalyze the formation of aminoacyl-tRNAs. Halofuginone (HF), a coccidiostat used in veterinary medicine, exerts its effects by acting as a high-affinity inhibitor of the enzyme glutamyl-prolyl-tRNA synthetase (EPRS). In order to elucidate the precise molecular basis of this inhibition mechanism of human EPRS, the crystal structures of the prolyl-tRNA synthetase domain of human EPRS (hPRS) at 2.4 Å resolution (hPRS-apo), of hPRS complexed with ATP and the substrate proline at 2.3 Å resolution (hPRS-sub) and of hPRS complexed with HF at 2.62 Å resolution (hPRS-HF) are presented. These structures show plainly that motif 1 functions as a cap in hPRS, which is loosely opened in hPRS-apo, tightly closed in hPRS-sub and incorrectly closed in hPRS-HF. In addition, the structural analyses are consistent with more effective binding of hPRS to HF with ATP. Mutagenesis and biochemical analysis confirmed the key roles of two residues, Phe1097 and Arg1152, in the HF inhibition mechanism. These structures will lead to the development of more potent and selective hPRS inhibitors for promoting inflammatory resolution.

Entities:  

Keywords:  drug design; glutamyl-prolyl-tRNA synthetase; herbal inhibitor; inflammation; multisynthetase complex

Mesh:

Substances:

Year:  2013        PMID: 24100331     DOI: 10.1107/S0907444913020556

Source DB:  PubMed          Journal:  Acta Crystallogr D Biol Crystallogr        ISSN: 0907-4449


  13 in total

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5.  Infection-specific phosphorylation of glutamyl-prolyl tRNA synthetase induces antiviral immunity.

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Journal:  Nat Immunol       Date:  2016-09-05       Impact factor: 25.606

6.  A binding hotspot in Trypanosoma cruzi histidyl-tRNA synthetase revealed by fragment-based crystallographic cocktail screens.

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Journal:  Acta Crystallogr D Biol Crystallogr       Date:  2015-07-31

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8.  Biochemical and Structural Characterization of Selective Allosteric Inhibitors of the Plasmodium falciparum Drug Target, Prolyl-tRNA-synthetase.

Authors:  Stephen Nakazawa Hewitt; David M Dranow; Benjamin G Horst; Jan A Abendroth; Barbara Forte; Irene Hallyburton; Chimed Jansen; Beatriz Baragaña; Ryan Choi; Kasey L Rivas; Matthew A Hulverson; Mitchell Dumais; Thomas E Edwards; Donald D Lorimer; Alan H Fairlamb; David W Gray; Kevin D Read; Adele M Lehane; Kiaran Kirk; Peter J Myler; Amy Wernimont; Chris Walpole; Robin Stacy; Lynn K Barrett; Ian H Gilbert; Wesley C Van Voorhis
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9.  Identification of Selective Novel Hits against Plasmodium falciparum Prolyl tRNA Synthetase Active Site and a Predicted Allosteric Site Using in silico Approaches.

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Review 10.  Structural analyses of the malaria parasite aminoacyl-tRNA synthetases provide new avenues for antimalarial drug discovery.

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Journal:  Protein Sci       Date:  2021-09       Impact factor: 6.993

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