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Literature DB >> 30916990

Tethering soluble meprin α in an enzyme complex to the cell surface affects IBD-associated genes.

Florian Peters¹, Franka Scharfenberg¹, Cynthia Colmorgen¹, Fred Armbrust¹, Rielana Wichert¹, Philipp Arnold², Barbara Potempa³, Jan Potempa³, Claus U Pietrzik⁴, Robert Häsler⁵, Philip Rosenstiel⁵, Christoph Becker-Pauly¹.

Abstract

Biologic activity of proteases is mainly characterized by the substrate specificity, tissue distribution, and cellular localization. The human metalloproteases meprin α and meprin β share 41% sequence identity and exhibit a similar cleavage specificity with a preference for negatively charged amino acids. However, shedding of meprin α by furin on the secretory pathway makes it a secreted enzyme in comparison with the membrane-bound meprin β. In this study, we identified human meprin α and meprin β as forming covalently linked membrane-tethered heterodimers in the early endoplasmic reticulum, thereby preventing furin-mediated secretion of meprin α. Within this newly formed enzyme complex, meprin α was able to be activated on the cell surface and detected by cleavage of a novel specific fluorogenic peptide substrate. However, the known meprin β substrates amyloid precursor protein and CD99 were not shed by membrane-tethered meprin α. On the other hand, being linked to meprin α, activation of or substrate cleavage by meprin β on the cell surface was not altered. Interestingly, proteolytic activity of both proteases was increased in the heteromeric complex, indicating an increased proteolytic potential at the plasma membrane. Because meprins are susceptibility genes for inflammatory bowel disease (IBD), and to investigate the physiologic impact of the enzyme complex, we performed transcriptome analyses of intestinal mucosa from meprin-knockout mice. Comparison of the transcriptional gene analysis data with gene analyses of IBD patients revealed that different gene subsets were dysregulated if meprin α was expressed alone or in the enzyme complex, demonstrating the physiologic and pathophysiological relevance of the meprin heterodimer formation.-Peters, F., Scharfenberg, F., Colmorgen, C., Armbrust, F., Wichert, R., Arnold, P., Potempa, B., Potempa, J., Pietrzik, C. U., Häsler, R., Rosenstiel, P., Becker-Pauly, C. Tethering soluble meprin α in an enzyme complex to the cell surface affects IBD-associated genes.

Entities: Chemical Disease Gene Species

Keywords: chronic intestinal inflammation; meprin β; protease; quaternary structure

Mesh：

Substances：

Year: 2019 PMID： 30916990 PMCID： PMC6529335 DOI： 10.1096/fj.201802391R

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

40 in total

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3. Analyzing the protease web in skin: meprin metalloproteases are activated specifically by KLK4, 5 and 8 vice versa leading to processing of proKLK7 thereby triggering its activation.

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Journal: J Biol Chem Date: 2014-03-24 Impact factor: 5.157

7. Generation of aggregation prone N-terminally truncated amyloid β peptides by meprin β depends on the sequence specificity at the cleavage site.

Authors: Caroline Schönherr; Jessica Bien; Simone Isbert; Rielana Wichert; Johannes Prox; Hermann Altmeppen; Sathish Kumar; Jochen Walter; Stefan F Lichtenthaler; Sascha Weggen; Markus Glatzel; Christoph Becker-Pauly; Claus U Pietrzik
Journal: Mol Neurodegener Date: 2016-02-19 Impact factor: 14.195

8. MicroRNA interactome analysis predicts post-transcriptional regulation of ADRB2 and PPP3R1 in the hypercholesterolemic myocardium.

Authors: Bence Ágg; Tamás Baranyai; András Makkos; Borbála Vető; Nóra Faragó; Ágnes Zvara; Zoltán Giricz; Dániel V Veres; Péter Csermely; Tamás Arányi; László G Puskás; Zoltán V Varga; Péter Ferdinandy
Journal: Sci Rep Date: 2018-07-04 Impact factor: 4.379

9. SWISS-MODEL: homology modelling of protein structures and complexes.

Authors: Andrew Waterhouse; Martino Bertoni; Stefan Bienert; Gabriel Studer; Gerardo Tauriello; Rafal Gumienny; Florian T Heer; Tjaart A P de Beer; Christine Rempfer; Lorenza Bordoli; Rosalba Lepore; Torsten Schwede
Journal: Nucleic Acids Res Date: 2018-07-02 Impact factor: 16.971

10. Uncoupling of mucosal gene regulation, mRNA splicing and adherent microbiota signatures in inflammatory bowel disease.

Authors: Robert Häsler; Raheleh Sheibani-Tezerji; Anupam Sinha; Matthias Barann; Ateequr Rehman; Daniela Esser; Konrad Aden; Carolin Knecht; Berenice Brandt; Susanna Nikolaus; Sascha Schäuble; Christoph Kaleta; Andre Franke; Christoph Fretter; Werner Müller; Marc-Thorsten Hütt; Michael Krawczak; Stefan Schreiber; Philip Rosenstiel
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4 in total

1. Degradome of soluble ADAM10 and ADAM17 metalloproteases.

Authors: Franka Scharfenberg; Andreas Helbig; Martin Sammel; Julia Benzel; Uwe Schlomann; Florian Peters; Rielana Wichert; Maximilian Bettendorff; Dirk Schmidt-Arras; Stefan Rose-John; Catherine Moali; Stefan F Lichtenthaler; Claus U Pietrzik; Jörg W Bartsch; Andreas Tholey; Christoph Becker-Pauly
Journal: Cell Mol Life Sci Date: 2019-06-17 Impact factor: 9.261

Review 2. Regulation of the alternative β-secretase meprin β by ADAM-mediated shedding.

Authors: Franka Scharfenberg; Fred Armbrust; Liana Marengo; Claus Pietrzik; Christoph Becker-Pauly
Journal: Cell Mol Life Sci Date: 2019-06-14 Impact factor: 9.261

3. Helical ultrastructure of the metalloprotease meprin α in complex with a small molecule inhibitor.

Authors: Charles Bayly-Jones; Christopher J Lupton; Claudia Fritz; Hariprasad Venugopal; Daniel Ramsbeck; Michael Wermann; Christian Jäger; Alex de Marco; Stephan Schilling; Dagmar Schlenzig; James C Whisstock
Journal: Nat Commun Date: 2022-10-19 Impact factor: 17.694

4. Structure and Dynamics of Meprin β in Complex with a Hydroxamate-Based Inhibitor.

Authors: Miriam Linnert; Claudia Fritz; Christian Jäger; Dagmar Schlenzig; Daniel Ramsbeck; Martin Kleinschmidt; Michael Wermann; Hans-Ulrich Demuth; Christoph Parthier; Stephan Schilling
Journal: Int J Mol Sci Date: 2021-05-26 Impact factor: 5.923

4 in total