Literature DB >> 26740262

Determination of the substrate repertoire of ADAMTS2, 3, and 14 significantly broadens their functions and identifies extracellular matrix organization and TGF-β signaling as primary targets.

Mourad Bekhouche1, Cedric Leduc2, Laura Dupont2, Lauriane Janssen2, Frederic Delolme3, Sandrine Vadon-Le Goff4, Nicolas Smargiasso5, Dominique Baiwir6, Gabriel Mazzucchelli5, Isabelle Zanella-Cleon7, Johanne Dubail2, Edwin De Pauw5, Betty Nusgens2, David J S Hulmes4, Catherine Moali4, Alain Colige8.   

Abstract

A disintegrin and metalloproteinase with thrombospondin type I motif (ADAMTS)2, 3, and 14 are collectively named procollagen N-proteinases (pNPs) because of their specific ability to cleave the aminopropeptide of fibrillar procollagens. Several reports also indicate that they could be involved in other biological processes, such as blood coagulation, development, and male fertility, but the potential substrates associated with these activities remain unknown. Using the recently described N-terminal amine isotopic labeling of substrate approach, we analyzed the secretomes of human fibroblasts and identified 8, 17, and 22 candidate substrates for ADAMTS2, 3, and 14, respectively. Among these newly identified substrates, many are components of the extracellular matrix and/or proteins related to cell signaling such as latent TGF-β binding protein 1, TGF-β RIII, and dickkopf-related protein 3. Candidate substrates for the 3 ADAMTS have been biochemically validated in different contexts, and the implication of ADAMTS2 in the control of TGF-β activity has been further demonstrated in human fibroblasts. Finally, the cleavage site specificity was assessed showing a clear and unique preference for nonpolar or slightly hydrophobic amino acids. This work shows that the activities of the pNPs extend far beyond the classically reported processing of the aminopropeptide of fibrillar collagens and that they should now be considered as multilevel regulators of matrix deposition and remodeling.-Bekhouche, M., Leduc, C., Dupont, L., Janssen, L., Delolme, F., Vadon-Le Goff, S., Smargiasso, N., Baiwir, D., Mazzucchelli, G., Zanella-Cleon, I., Dubail, J., De Pauw, E., Nusgens, B., Hulmes, D. J. S., Moali, C., Colige, A. Determination of the substrate repertoire of ADAMTS2, 3, and 14 significantly broadens their functions and identifies extracellular matrix organization and TGF-β signaling as primary targets. © FASEB.

Entities:  

Keywords:  DKK3; LTBP1; N-TAILS; betaglycan

Mesh:

Substances:

Year:  2016        PMID: 26740262     DOI: 10.1096/fj.15-279869

Source DB:  PubMed          Journal:  FASEB J        ISSN: 0892-6638            Impact factor:   5.191


  30 in total

Review 1.  ADAMTS proteins in human disorders.

Authors:  Timothy J Mead; Suneel S Apte
Journal:  Matrix Biol       Date:  2018-06-06       Impact factor: 11.583

2.  C-terminal proteolysis of the collagen VI α3 chain by BMP-1 and proprotein convertase(s) releases endotrophin in fragments of different sizes.

Authors:  Stefanie Elisabeth Heumüller; Maya Talantikite; Manon Napoli; Jean Armengaud; Matthias Mörgelin; Ursula Hartmann; Gerhard Sengle; Mats Paulsson; Catherine Moali; Raimund Wagener
Journal:  J Biol Chem       Date:  2019-07-25       Impact factor: 5.157

3.  Differential cleavage of lysyl oxidase by the metalloproteinases BMP1 and ADAMTS2/14 regulates collagen binding through a tyrosine sulfate domain.

Authors:  Tamara Rosell-García; Alberto Paradela; Gema Bravo; Laura Dupont; Mourad Bekhouche; Alain Colige; Fernando Rodriguez-Pascual
Journal:  J Biol Chem       Date:  2019-05-31       Impact factor: 5.157

Review 4.  The "other" 15-40%: The Role of Non-Collagenous Extracellular Matrix Proteins and Minor Collagens in Tendon.

Authors:  Nandaraj Taye; Stylianos Z Karoulias; Dirk Hubmacher
Journal:  J Orthop Res       Date:  2019-08-26       Impact factor: 3.494

5.  A Selective Extracellular Matrix Proteomics Approach Identifies Fibronectin Proteolysis by A Disintegrin-like and Metalloprotease Domain with Thrombospondin Type 1 Motifs (ADAMTS16) and Its Impact on Spheroid Morphogenesis.

Authors:  Rahel Schnellmann; Ragna Sack; Daniel Hess; Douglas S Annis; Deane F Mosher; Suneel S Apte; Ruth Chiquet-Ehrismann
Journal:  Mol Cell Proteomics       Date:  2018-04-18       Impact factor: 5.911

Review 6.  Cardiac fibrosis in regenerative medicine: destroy to rebuild.

Authors:  Gianluca Lorenzo Perrucci; Erica Rurali; Giulio Pompilio
Journal:  J Thorac Dis       Date:  2018-07       Impact factor: 2.895

7.  A disintegrin-like and metalloproteinase domain with thrombospondin type 1 motif 9 (ADAMTS9) regulates fibronectin fibrillogenesis and turnover.

Authors:  Lauren W Wang; Sumeda Nandadasa; Douglas S Annis; Joanne Dubail; Deane F Mosher; Belinda B Willard; Suneel S Apte
Journal:  J Biol Chem       Date:  2019-05-13       Impact factor: 5.157

8.  Systems Genetics Approach Identifies Gene Pathways and Adamts2 as Drivers of Isoproterenol-Induced Cardiac Hypertrophy and Cardiomyopathy in Mice.

Authors:  Christoph D Rau; Milagros C Romay; Mary Tuteryan; Jessica J-C Wang; Marc Santolini; Shuxun Ren; Alain Karma; James N Weiss; Yibin Wang; Aldons J Lusis
Journal:  Cell Syst       Date:  2016-11-17       Impact factor: 10.304

Review 9.  Regulation of ADAMTS Proteases.

Authors:  Keron W J Rose; Nandaraj Taye; Stylianos Z Karoulias; Dirk Hubmacher
Journal:  Front Mol Biosci       Date:  2021-06-29

Review 10.  The quest for substrates and binding partners: A critical barrier for understanding the role of ADAMTS proteases in musculoskeletal development and disease.

Authors:  Brandon Satz-Jacobowitz; Dirk Hubmacher
Journal:  Dev Dyn       Date:  2020-09-17       Impact factor: 3.780
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