Startseite Metalloprotease inhibitor profiles of human ADAM8 in vitro and in cell-based assays
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Metalloprotease inhibitor profiles of human ADAM8 in vitro and in cell-based assays

  • Uwe Schlomann , Kristina Dorzweiler , Elisa Nuti , Tiziano Tuccinardi , Armando Rossello und Jörg W. Bartsch ORCID logo EMAIL logo
Veröffentlicht/Copyright: 4. März 2019
Biological Chemistry
Aus der Zeitschrift Biological Chemistry Band 400 Heft 6

Abstract

ADAM8 as a membrane-anchored metalloproteinase-disintegrin is upregulated under pathological conditions such as inflammation and cancer. As active sheddase, ADAM8 can cleave several membrane proteins, among them the low-affinity receptor FcεRII CD23. Hydroxamate-based inhibitors are routinely used to define relevant proteinases involved in ectodomain shedding of membrane proteins. However, for ADAM proteinases, common hydroxamates have variable profiles in their inhibition properties, commonly known for ADAM proteinases 9, 10 and 17. Here, we determined the inhibitor profile of human ADAM8 for eight ADAM/MMP inhibitors by in vitro assays using recombinant ADAM8 as well as the in vivo inhibition in cell-based assays using HEK293 cells to monitor the release of soluble CD23 by ADAM8. ADAM8 activity is inhibited by BB94 (Batimastat), GW280264, FC387 and FC143 (two ADAM17 inhibitors), made weaker by GM6001, TAPI2 and BB2516 (Marimastat), while no inhibition was observed for GI254023, an ADAM10 specific inhibitor. Modeling of inhibitor FC143 bound to the catalytic sites of ADAM8 and ADAM17 reveals similar geometries in the pharmacophoric regions of both proteinases, which is different in ADAM10 due to replacement in the S1 position of T300 (ADAM8) and T347 (ADAM17) by V327 (ADAM10). We conclude that ADAM8 inhibitors require maximum selectivity over ADAM17 to achieve specific ADAM8 inhibition.

Keywords: ADAM8; cell-based assay; ectodomain cleavage; hydroxamates; low-affinity IgE receptor FcεRII (CD23); recombinant protein

Funding source: Deutsche Forschungsgemeinschaft

Award Identifier / Grant number: BA1606/3-1

Funding statement: This work was supported by the Deutsche Forschungsgemeinschaft (Funder Id: 10.13039/501100001659, BA1606/3-1 to J.W.B. and U.S.) and by the University of Pisa (PRA_2018_20). We thank Sarah Koch (Marburg) for help with enzyme assays, Luciana Marinelli and Valeria La Pietra (Naples) for providing us with the docking model ADAM17/FC143, Muriel Bartsch for help with IC50 calculations, and Vincent Dive (Gif-sur-Yvette, France) for helpful discussions on the ADAM8 structure.

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Supplementary Material

The online version of this article offers supplementary material (https://doi.org/10.1515/hsz-2018-0396).

Received: 2018-10-10
Accepted: 2018-12-19
Published Online: 2019-03-04
Published in Print: 2019-06-26

©2019 Walter de Gruyter GmbH, Berlin/Boston

Artikel in diesem Heft

  1. Frontmatter
  2. Reviews
  3. Unforgettable force – crosstalk and memory of mechanosensitive structures
  4. Differential expression of DLG1 as a common trait in different human diseases: an encouraging issue in molecular pathology
  5. The effects of oxidative stress on the development of atherosclerosis
  6. Research Articles/Short Communications
  7. Protein Structure and Function
  8. Kinetically selective and potent inhibitors of HDAC8
  9. Assay of β-glucosidase 2 (GBA2) activity using lithocholic acid β-3-O-glucoside substrate for cultured fibroblasts and glucosylceramide for brain tissue
  10. Cell Biology and Signaling
  11. Changqin NO. 1 inhibits neuronal apoptosis via suppressing GAS5 expression in a traumatic brain injury mice model
  12. Nm23-H1 inhibits hypoxia induced epithelial-mesenchymal transition and stemness in non-small cell lung cancer cells
  13. Nodal promotes the malignancy of non-small cell lung cancer (NSCLC) cells via activation of NF-κB/IL-6 signals
  14. MCT1, MCT4 and CD147 expression and 3-bromopyruvate toxicity in colorectal cancer cells are modulated by the extracellular conditions
  15. Proteolysis
  16. Metalloprotease inhibitor profiles of human ADAM8 in vitro and in cell-based assays
https://doi.org/10.1515/hsz-2018-0396
Schlagwörter für diesen Artikel
ADAM8; cell-based assay; ectodomain cleavage; hydroxamates; low-affinity IgE receptor FcεRII (CD23); recombinant protein

Artikel in diesem Heft

  1. Frontmatter
  2. Reviews
  3. Unforgettable force – crosstalk and memory of mechanosensitive structures
  4. Differential expression of DLG1 as a common trait in different human diseases: an encouraging issue in molecular pathology
  5. The effects of oxidative stress on the development of atherosclerosis
  6. Research Articles/Short Communications
  7. Protein Structure and Function
  8. Kinetically selective and potent inhibitors of HDAC8
  9. Assay of β-glucosidase 2 (GBA2) activity using lithocholic acid β-3-O-glucoside substrate for cultured fibroblasts and glucosylceramide for brain tissue
  10. Cell Biology and Signaling
  11. Changqin NO. 1 inhibits neuronal apoptosis via suppressing GAS5 expression in a traumatic brain injury mice model
  12. Nm23-H1 inhibits hypoxia induced epithelial-mesenchymal transition and stemness in non-small cell lung cancer cells
  13. Nodal promotes the malignancy of non-small cell lung cancer (NSCLC) cells via activation of NF-κB/IL-6 signals
  14. MCT1, MCT4 and CD147 expression and 3-bromopyruvate toxicity in colorectal cancer cells are modulated by the extracellular conditions
  15. Proteolysis
  16. Metalloprotease inhibitor profiles of human ADAM8 in vitro and in cell-based assays
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