Distinct Roles of Catalytic Cysteine and Histidine in the Protease and Ligase Mechanisms of Human Legumain As Revealed by DFT-Based QM/MM Simulations

[Image: see text] The cysteine protease enzyme legumain hydrolyzes peptide bonds with high specificity after asparagine and under more acidic conditions after aspartic acid [ E. N. BakerJ. Mol. Biol.1980, 141, 441−4847003158; E. N. Baker; J. Mol. Biol.1977, 111, 207–210859183; J. Drenth; Biochemistr...

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Autores principales: Elsässer, Brigitta, Zauner, Florian B., Messner, Johann, Soh, Wai Tuck, Dall, Elfriede, Brandstetter, Hans
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2017
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5600538/
https://www.ncbi.nlm.nih.gov/pubmed/28932620
http://dx.doi.org/10.1021/acscatal.7b01505
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author Elsässer, Brigitta
Zauner, Florian B.
Messner, Johann
Soh, Wai Tuck
Dall, Elfriede
Brandstetter, Hans
author_facet Elsässer, Brigitta
Zauner, Florian B.
Messner, Johann
Soh, Wai Tuck
Dall, Elfriede
Brandstetter, Hans
author_sort Elsässer, Brigitta
collection PubMed
description [Image: see text] The cysteine protease enzyme legumain hydrolyzes peptide bonds with high specificity after asparagine and under more acidic conditions after aspartic acid [ E. N. BakerJ. Mol. Biol.1980, 141, 441−4847003158; E. N. Baker; J. Mol. Biol.1977, 111, 207–210859183; J. Drenth; Biochemistry1976, 15, 3731–3738952885; R. Menard; J. Cell. Biochem.1994, 137; L. PolgarEur. J. Biochem.1978, 88, 513–521689035; A. C. Storer; Methods Enzymol.1994, 244, 486–5007845227. Remarkably, legumain additionally exhibits ligase activity that prevails at pH > 5.5. The atomic reaction mechanisms including their pH dependence are only partly understood. Here we present a density functional theory (DFT)-based quantum mechanics/molecular mechanics (QM/MM) study of the detailed reaction mechanism of both activities for human legumain in solution. Contrasting the situation in other papain-like proteases, our calculations reveal that the active site Cys189 must be present in the protonated state for a productive nucleophilic attack and simultaneous rupture of the scissile peptide bond, consistent with the experimental pH profile of legumain-catalyzed cleavages. The resulting thioester intermediate (INT1) is converted by water attack on the thioester into a second intermediate, a diol (INT2), which is released by proton abstraction by Cys189. Surprisingly, we found that ligation is not the exact reverse of the proteolysis but can proceed via two distinct routes. Whereas the transpeptidation route involves aminolysis of the thioester (INT1), at pH 6 a cysteine-independent, histidine-assisted ligation route was found. Given legumain’s important roles in immunity, cancer, and neurodegenerative diseases, our findings open up possibilities for targeted drug design in these fields.
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spelling pubmed-56005382017-09-18 Distinct Roles of Catalytic Cysteine and Histidine in the Protease and Ligase Mechanisms of Human Legumain As Revealed by DFT-Based QM/MM Simulations Elsässer, Brigitta Zauner, Florian B. Messner, Johann Soh, Wai Tuck Dall, Elfriede Brandstetter, Hans ACS Catal [Image: see text] The cysteine protease enzyme legumain hydrolyzes peptide bonds with high specificity after asparagine and under more acidic conditions after aspartic acid [ E. N. BakerJ. Mol. Biol.1980, 141, 441−4847003158; E. N. Baker; J. Mol. Biol.1977, 111, 207–210859183; J. Drenth; Biochemistry1976, 15, 3731–3738952885; R. Menard; J. Cell. Biochem.1994, 137; L. PolgarEur. J. Biochem.1978, 88, 513–521689035; A. C. Storer; Methods Enzymol.1994, 244, 486–5007845227. Remarkably, legumain additionally exhibits ligase activity that prevails at pH > 5.5. The atomic reaction mechanisms including their pH dependence are only partly understood. Here we present a density functional theory (DFT)-based quantum mechanics/molecular mechanics (QM/MM) study of the detailed reaction mechanism of both activities for human legumain in solution. Contrasting the situation in other papain-like proteases, our calculations reveal that the active site Cys189 must be present in the protonated state for a productive nucleophilic attack and simultaneous rupture of the scissile peptide bond, consistent with the experimental pH profile of legumain-catalyzed cleavages. The resulting thioester intermediate (INT1) is converted by water attack on the thioester into a second intermediate, a diol (INT2), which is released by proton abstraction by Cys189. Surprisingly, we found that ligation is not the exact reverse of the proteolysis but can proceed via two distinct routes. Whereas the transpeptidation route involves aminolysis of the thioester (INT1), at pH 6 a cysteine-independent, histidine-assisted ligation route was found. Given legumain’s important roles in immunity, cancer, and neurodegenerative diseases, our findings open up possibilities for targeted drug design in these fields. American Chemical Society 2017-07-14 2017-09-01 /pmc/articles/PMC5600538/ /pubmed/28932620 http://dx.doi.org/10.1021/acscatal.7b01505 Text en Copyright © 2017 American Chemical Society This is an open access article published under a Creative Commons Attribution (CC-BY) License (http://pubs.acs.org/page/policy/authorchoice_ccby_termsofuse.html) , which permits unrestricted use, distribution and reproduction in any medium, provided the author and source are cited.
spellingShingle Elsässer, Brigitta
Zauner, Florian B.
Messner, Johann
Soh, Wai Tuck
Dall, Elfriede
Brandstetter, Hans
Distinct Roles of Catalytic Cysteine and Histidine in the Protease and Ligase Mechanisms of Human Legumain As Revealed by DFT-Based QM/MM Simulations
title Distinct Roles of Catalytic Cysteine and Histidine in the Protease and Ligase Mechanisms of Human Legumain As Revealed by DFT-Based QM/MM Simulations
title_full Distinct Roles of Catalytic Cysteine and Histidine in the Protease and Ligase Mechanisms of Human Legumain As Revealed by DFT-Based QM/MM Simulations
title_fullStr Distinct Roles of Catalytic Cysteine and Histidine in the Protease and Ligase Mechanisms of Human Legumain As Revealed by DFT-Based QM/MM Simulations
title_full_unstemmed Distinct Roles of Catalytic Cysteine and Histidine in the Protease and Ligase Mechanisms of Human Legumain As Revealed by DFT-Based QM/MM Simulations
title_short Distinct Roles of Catalytic Cysteine and Histidine in the Protease and Ligase Mechanisms of Human Legumain As Revealed by DFT-Based QM/MM Simulations
title_sort distinct roles of catalytic cysteine and histidine in the protease and ligase mechanisms of human legumain as revealed by dft-based qm/mm simulations
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5600538/
https://www.ncbi.nlm.nih.gov/pubmed/28932620
http://dx.doi.org/10.1021/acscatal.7b01505
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