NMR-Based Structural Characterization of a Two-Disulfide-Bonded Analogue of the FXIIIa Inhibitor Tridegin: New Insights into Structure–Activity Relationships

The saliva of blood-sucking leeches contains a plethora of anticoagulant substances. One of these compounds derived from Haementeria ghilianii, the 66mer three-disulfide-bonded peptide tridegin, specifically inhibits the blood coagulation factor FXIIIa. Tridegin represents a potential tool for antit...

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Autores principales: Schmitz, Thomas, Paul George, Ajay Abisheck, Nubbemeyer, Britta, Bäuml, Charlotte A., Steinmetzer, Torsten, Ohlenschläger, Oliver, Biswas, Arijit, Imhof, Diana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7830451/
https://www.ncbi.nlm.nih.gov/pubmed/33477282
http://dx.doi.org/10.3390/ijms22020880
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author Schmitz, Thomas
Paul George, Ajay Abisheck
Nubbemeyer, Britta
Bäuml, Charlotte A.
Steinmetzer, Torsten
Ohlenschläger, Oliver
Biswas, Arijit
Imhof, Diana
author_facet Schmitz, Thomas
Paul George, Ajay Abisheck
Nubbemeyer, Britta
Bäuml, Charlotte A.
Steinmetzer, Torsten
Ohlenschläger, Oliver
Biswas, Arijit
Imhof, Diana
author_sort Schmitz, Thomas
collection PubMed
description The saliva of blood-sucking leeches contains a plethora of anticoagulant substances. One of these compounds derived from Haementeria ghilianii, the 66mer three-disulfide-bonded peptide tridegin, specifically inhibits the blood coagulation factor FXIIIa. Tridegin represents a potential tool for antithrombotic and thrombolytic therapy. We recently synthesized two-disulfide-bonded tridegin variants, which retained their inhibitory potential. For further lead optimization, however, structure information is required. We thus analyzed the structure of a two-disulfide-bonded tridegin isomer by solution 2D NMR spectroscopy in a combinatory approach with subsequent MD simulations. The isomer was studied using two fragments, i.e., the disulfide-bonded N-terminal (Lys1–Cys37) and the flexible C-terminal part (Arg38–Glu66), which allowed for a simplified, label-free NMR-structure elucidation of the 66mer peptide. The structural information was subsequently used in molecular modeling and docking studies to provide insights into the structure–activity relationships. The present study will prospectively support the development of anticoagulant-therapy-relevant compounds targeting FXIIIa.
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spelling pubmed-78304512021-01-26 NMR-Based Structural Characterization of a Two-Disulfide-Bonded Analogue of the FXIIIa Inhibitor Tridegin: New Insights into Structure–Activity Relationships Schmitz, Thomas Paul George, Ajay Abisheck Nubbemeyer, Britta Bäuml, Charlotte A. Steinmetzer, Torsten Ohlenschläger, Oliver Biswas, Arijit Imhof, Diana Int J Mol Sci Article The saliva of blood-sucking leeches contains a plethora of anticoagulant substances. One of these compounds derived from Haementeria ghilianii, the 66mer three-disulfide-bonded peptide tridegin, specifically inhibits the blood coagulation factor FXIIIa. Tridegin represents a potential tool for antithrombotic and thrombolytic therapy. We recently synthesized two-disulfide-bonded tridegin variants, which retained their inhibitory potential. For further lead optimization, however, structure information is required. We thus analyzed the structure of a two-disulfide-bonded tridegin isomer by solution 2D NMR spectroscopy in a combinatory approach with subsequent MD simulations. The isomer was studied using two fragments, i.e., the disulfide-bonded N-terminal (Lys1–Cys37) and the flexible C-terminal part (Arg38–Glu66), which allowed for a simplified, label-free NMR-structure elucidation of the 66mer peptide. The structural information was subsequently used in molecular modeling and docking studies to provide insights into the structure–activity relationships. The present study will prospectively support the development of anticoagulant-therapy-relevant compounds targeting FXIIIa. MDPI 2021-01-17 /pmc/articles/PMC7830451/ /pubmed/33477282 http://dx.doi.org/10.3390/ijms22020880 Text en © 2021 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Schmitz, Thomas
Paul George, Ajay Abisheck
Nubbemeyer, Britta
Bäuml, Charlotte A.
Steinmetzer, Torsten
Ohlenschläger, Oliver
Biswas, Arijit
Imhof, Diana
NMR-Based Structural Characterization of a Two-Disulfide-Bonded Analogue of the FXIIIa Inhibitor Tridegin: New Insights into Structure–Activity Relationships
title NMR-Based Structural Characterization of a Two-Disulfide-Bonded Analogue of the FXIIIa Inhibitor Tridegin: New Insights into Structure–Activity Relationships
title_full NMR-Based Structural Characterization of a Two-Disulfide-Bonded Analogue of the FXIIIa Inhibitor Tridegin: New Insights into Structure–Activity Relationships
title_fullStr NMR-Based Structural Characterization of a Two-Disulfide-Bonded Analogue of the FXIIIa Inhibitor Tridegin: New Insights into Structure–Activity Relationships
title_full_unstemmed NMR-Based Structural Characterization of a Two-Disulfide-Bonded Analogue of the FXIIIa Inhibitor Tridegin: New Insights into Structure–Activity Relationships
title_short NMR-Based Structural Characterization of a Two-Disulfide-Bonded Analogue of the FXIIIa Inhibitor Tridegin: New Insights into Structure–Activity Relationships
title_sort nmr-based structural characterization of a two-disulfide-bonded analogue of the fxiiia inhibitor tridegin: new insights into structure–activity relationships
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7830451/
https://www.ncbi.nlm.nih.gov/pubmed/33477282
http://dx.doi.org/10.3390/ijms22020880
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