Identification of Regulatory Molecular “Hot Spots” for LH/PLOD Collagen Glycosyltransferase Activity

Hydroxylysine glycosylations are post-translational modifications (PTMs) essential for the maturation and homeostasis of fibrillar and non-fibrillar collagen molecules. The multifunctional collagen lysyl hydroxylase 3 (LH3/PLOD3) and the collagen galactosyltransferase GLT25D1 are the human enzymes t...

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Autores principales: Mattoteia, Daiana, Chiapparino, Antonella, Fumagalli, Marco, De Marco, Matteo, De Giorgi, Francesca, Negro, Lisa, Pinnola, Alberta, Faravelli, Silvia, Roscioli, Tony, Scietti, Luigi, Forneris, Federico
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10342707/
https://www.ncbi.nlm.nih.gov/pubmed/37446392
http://dx.doi.org/10.3390/ijms241311213
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author Mattoteia, Daiana
Chiapparino, Antonella
Fumagalli, Marco
De Marco, Matteo
De Giorgi, Francesca
Negro, Lisa
Pinnola, Alberta
Faravelli, Silvia
Roscioli, Tony
Scietti, Luigi
Forneris, Federico
author_facet Mattoteia, Daiana
Chiapparino, Antonella
Fumagalli, Marco
De Marco, Matteo
De Giorgi, Francesca
Negro, Lisa
Pinnola, Alberta
Faravelli, Silvia
Roscioli, Tony
Scietti, Luigi
Forneris, Federico
author_sort Mattoteia, Daiana
collection PubMed
description Hydroxylysine glycosylations are post-translational modifications (PTMs) essential for the maturation and homeostasis of fibrillar and non-fibrillar collagen molecules. The multifunctional collagen lysyl hydroxylase 3 (LH3/PLOD3) and the collagen galactosyltransferase GLT25D1 are the human enzymes that have been identified as being responsible for the glycosylation of collagen lysines, although a precise description of the contribution of each enzyme to these essential PTMs has not yet been provided in the literature. LH3/PLOD3 is thought to be capable of performing two chemically distinct collagen glycosyltransferase reactions using the same catalytic site: an inverting beta-1,O-galactosylation of hydroxylysines (Gal-T) and a retaining alpha-1,2-glucosylation of galactosyl hydroxylysines (Glc-T). In this work, we have combined indirect luminescence-based assays with direct mass spectrometry-based assays and molecular structure studies to demonstrate that LH3/PLOD3 only has Glc-T activity and that GLT25D1 only has Gal-T activity. Structure-guided mutagenesis confirmed that the Glc-T activity is defined by key residues in the first-shell environment of the glycosyltransferase catalytic site as well as by long-range contributions from residues within the same glycosyltransferase (GT) domain. By solving the molecular structures and characterizing the interactions and solving the molecular structures of human LH3/PLOD3 in complex with different UDP-sugar analogs, we show how these studies could provide insights for LH3/PLOD3 glycosyltransferase inhibitor development. Collectively, our data provide new tools for the direct investigation of collagen hydroxylysine PTMs and a comprehensive overview of the complex network of shapes, charges, and interactions that enable LH3/PLOD3 glycosyltransferase activities, expanding the molecular framework and facilitating an improved understanding and manipulation of glycosyltransferase functions in biomedical applications.
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spelling pubmed-103427072023-07-14 Identification of Regulatory Molecular “Hot Spots” for LH/PLOD Collagen Glycosyltransferase Activity Mattoteia, Daiana Chiapparino, Antonella Fumagalli, Marco De Marco, Matteo De Giorgi, Francesca Negro, Lisa Pinnola, Alberta Faravelli, Silvia Roscioli, Tony Scietti, Luigi Forneris, Federico Int J Mol Sci Article Hydroxylysine glycosylations are post-translational modifications (PTMs) essential for the maturation and homeostasis of fibrillar and non-fibrillar collagen molecules. The multifunctional collagen lysyl hydroxylase 3 (LH3/PLOD3) and the collagen galactosyltransferase GLT25D1 are the human enzymes that have been identified as being responsible for the glycosylation of collagen lysines, although a precise description of the contribution of each enzyme to these essential PTMs has not yet been provided in the literature. LH3/PLOD3 is thought to be capable of performing two chemically distinct collagen glycosyltransferase reactions using the same catalytic site: an inverting beta-1,O-galactosylation of hydroxylysines (Gal-T) and a retaining alpha-1,2-glucosylation of galactosyl hydroxylysines (Glc-T). In this work, we have combined indirect luminescence-based assays with direct mass spectrometry-based assays and molecular structure studies to demonstrate that LH3/PLOD3 only has Glc-T activity and that GLT25D1 only has Gal-T activity. Structure-guided mutagenesis confirmed that the Glc-T activity is defined by key residues in the first-shell environment of the glycosyltransferase catalytic site as well as by long-range contributions from residues within the same glycosyltransferase (GT) domain. By solving the molecular structures and characterizing the interactions and solving the molecular structures of human LH3/PLOD3 in complex with different UDP-sugar analogs, we show how these studies could provide insights for LH3/PLOD3 glycosyltransferase inhibitor development. Collectively, our data provide new tools for the direct investigation of collagen hydroxylysine PTMs and a comprehensive overview of the complex network of shapes, charges, and interactions that enable LH3/PLOD3 glycosyltransferase activities, expanding the molecular framework and facilitating an improved understanding and manipulation of glycosyltransferase functions in biomedical applications. MDPI 2023-07-07 /pmc/articles/PMC10342707/ /pubmed/37446392 http://dx.doi.org/10.3390/ijms241311213 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/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 (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Mattoteia, Daiana
Chiapparino, Antonella
Fumagalli, Marco
De Marco, Matteo
De Giorgi, Francesca
Negro, Lisa
Pinnola, Alberta
Faravelli, Silvia
Roscioli, Tony
Scietti, Luigi
Forneris, Federico
Identification of Regulatory Molecular “Hot Spots” for LH/PLOD Collagen Glycosyltransferase Activity
title Identification of Regulatory Molecular “Hot Spots” for LH/PLOD Collagen Glycosyltransferase Activity
title_full Identification of Regulatory Molecular “Hot Spots” for LH/PLOD Collagen Glycosyltransferase Activity
title_fullStr Identification of Regulatory Molecular “Hot Spots” for LH/PLOD Collagen Glycosyltransferase Activity
title_full_unstemmed Identification of Regulatory Molecular “Hot Spots” for LH/PLOD Collagen Glycosyltransferase Activity
title_short Identification of Regulatory Molecular “Hot Spots” for LH/PLOD Collagen Glycosyltransferase Activity
title_sort identification of regulatory molecular “hot spots” for lh/plod collagen glycosyltransferase activity
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10342707/
https://www.ncbi.nlm.nih.gov/pubmed/37446392
http://dx.doi.org/10.3390/ijms241311213
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