论文信息 - Discovery of an enzyme and substrate selective inhibitor of ADAM10 using an exosite-binding glycosylated substrate - 字舞流文

Discovery of an enzyme and substrate selective inhibitor of ADAM10 using an exosite-binding glycosylated substrate

ADAM10 and ADAM17 have been shown to contribute to the acquired drug resistance of HER2-positive breast cancer in response to trastuzumab. The majority of ADAM10 and ADAM17 inhibitor development has been focused on the discovery of compounds that bind the active site zinc, however, in recent years, there has been a shift from active site to secondary substrate binding site (exosite) inhibitor discovery in order to identify non-zinc-binding molecules. In the present work a glycosylated, exosite-binding substrate of ADAM10 and ADAM17 was utilized to screen 370,276 compounds from the MLPCN collection. As a result of this uHTS effort, a selective, time-dependent, non-zinc-binding inhibitor of ADAM10 with Ki = 883 nM was discovered. This compound exhibited low cell toxicity and was able to selectively inhibit shedding of known ADAM10 substrates in several cell-based models. We hypothesize that differential glycosylation of these cognate substrates is the source of selectivity of our novel inhibitor. The data indicate that this novel inhibitor can be used as an in vitro and, potentially, in vivo, probe of ADAM10 activity. Additionally, results of the present and prior studies strongly suggest that glycosylated substrate are applicable as screening agents for discovery of selective ADAM probes and therapeutics.

Dmitriy Minond | Timothy P. Spicer | Franck Madoux | Radleigh Santos | Radleigh G. Santos | Gregg B. Fields | Thomas Bannister | T. Spicer | G. Fields | Franck Madoux | M. Cudic | A. Ludwig | L. Scampavia | Dmitriy Minond | T. Bannister | C. Becker-Pauly | Daniela Dreymuller | Jean-Phillipe Pettiloud | Andreas Ludwig | Christoph Becker-Pauly | Mare Cudic | Daniela Dreymuller | Jean-Phillipe Pettiloud | Louis D. Scampavia | D. Minond

[1] M. Sliwkowski,et al. Insights into ErbB signaling from the structure of the ErbB2-pertuzumab complex. , 2004, Cancer cell.

[2] L. Abrahmsén,et al. Structural basis for high-affinity HER2 receptor binding by an engineered protein , 2010, Proceedings of the National Academy of Sciences.

[3] B. Buwalda,et al. Synaptic plasticity in the dentate gyrus of aged rats is altered after chronic nimodipine application , 1992, Brain Research.

[4] C. Blobel,et al. ADAM17 is regulated by a rapid and reversible mechanism that controls access to its catalytic site , 2010, Journal of Cell Science.

[5] Jintao Zhang,et al. Characterizing the Diversity and Biological Relevance of the MLPCN Assay Manifold and Screening Set , 2011, J. Chem. Inf. Model..

[6] Thomas D. Y. Chung,et al. A Simple Statistical Parameter for Use in Evaluation and Validation of High Throughput Screening Assays , 1999, Journal of biomolecular screening.

[7] M. Lambert,et al. Metalloproteinase inhibitors for the disintegrin-like metalloproteinases ADAM10 and ADAM17 that differentially block constitutive and phorbol ester-inducible shedding of cell surface molecules. , 2005, Combinatorial chemistry & high throughput screening.

[8] Ji Zhang,et al. ADAM17 is overexpressed in non-small cell lung cancer and its expression correlates with poor patient survival , 2013, Tumor Biology.

[9] Jennifer A. Getz,et al. Identifi cation of protease exosite-interacting peptides that enhance substrate cleavage kinetics , 2012, Biological chemistry.

[10] G. Fields,et al. High throughput screening of potentially selective MMP-13 exosite inhibitors utilizing a triple-helical FRET substrate. , 2009, Bioorganic & medicinal chemistry.

[11] N. Schwarz,et al. Distinct role of the intracellular C-terminus for subcellular expression, shedding and function of the murine transmembrane chemokine CX3CL1. , 2010, Biochemical and biophysical research communications.

[12] G. Fields,et al. Characterization of an exosite binding inhibitor of matrix metalloproteinase 13 , 2007, Protein science : a publication of the Protein Society.

[13] J. Pfeilschifter,et al. CXCL16 is expressed in podocytes and acts as a scavenger receptor for oxidized low-density lipoprotein. , 2009, The American journal of pathology.

[14] S. Uhlig,et al. A Disintegrin and Metalloproteinase 17 (ADAM17) Mediates Inflammation-induced Shedding of Syndecan-1 and -4 by Lung Epithelial Cells* , 2009, The Journal of Biological Chemistry.

[15] V. Magdolen,et al. The α and β Subunits of the Metalloprotease Meprin Are Expressed in Separate Layers of Human Epidermis, Revealing Different Functions in Keratinocyte Proliferation and Differentiation , 2007 .

[16] M. Bissell,et al. Targeting TACE-dependent EGFR ligand shedding in breast cancer. , 2007, The Journal of clinical investigation.

[17] S. Rose-John,et al. The Transmembrane CXC-Chemokine Ligand 16 Is Induced by IFN-γ and TNF-α and Shed by the Activity of the Disintegrin-Like Metalloproteinase ADAM10 1 , 2004, The Journal of Immunology.

[18] A. Harris,et al. HER2 Phosphorylation Is Maintained by a PKB Negative Feedback Loop in Response to Anti-HER2 Herceptin in Breast Cancer , 2010, PLoS biology.

[19] D. Georgiadis,et al. Specific targeting of metzincin family members with small-molecule inhibitors: progress toward a multifarious challenge. , 2008, Bioorganic & medicinal chemistry.

[20] G. Sahni,et al. Multiple exosites distributed across the three domains of streptokinase co-operate to generate high catalytic rates in the streptokinase-plasmin activator complex. , 2013, Biochemistry.

[21] Franklin Peale,et al. Variants of the Antibody Herceptin That Interact with HER2 and VEGF at the Antigen Binding Site , 2009, Science.

[22] R. Rimokh,et al. The Disintegrin and Metalloprotease ADAM12 Is Associated with TGF-β-Induced Epithelial to Mesenchymal Transition , 2015, PloS one.

[23] A. Harris,et al. ADAM10 mediates trastuzumab resistance and is correlated with survival in HER2 positive breast cancer , 2014, Oncotarget.

[24] Y. You,et al. Effects of ADAM10 upregulation on progression, migration, and prognosis of nasopharyngeal carcinoma , 2015, Cancer science.

[25] T. Spicer,et al. Development of high throughput screening assays and pilot screen for inhibitors of metalloproteases meprin α and β , 2014, Biopolymers.

[26] T. Spicer,et al. Characterization of Selective Exosite-Binding Inhibitors of Matrix Metalloproteinase 13 That Prevent Articular Cartilage Degradation in Vitro , 2014, Journal of medicinal chemistry.

[27] Peter Hodder,et al. Application of Parallel Multiparametric Cell-Based FLIPR Detection Assays for the Identification of Modulators of the Muscarinic Acetylcholine Receptor 4 (M4) , 2015, Journal of biomolecular screening.

[28] P. Alzari,et al. Substrate-selective inhibition of protein kinase PDK1 by small compounds that bind to the PIF-pocket allosteric docking site. , 2012, Chemistry & biology.

[29] I. Wang,et al. Expression and protein chemistry yielding crystallization of the catalytic domain of ADAM17 complexed with a hydroxamate inhibitor. , 2007, Protein expression and purification.

[30] M. Giulianotti,et al. Activity of ADAM17 (a Disintegrin and Metalloprotease 17) Is Regulated by Its Noncatalytic Domains and Secondary Structure of its Substrates* , 2013, The Journal of Biological Chemistry.

[31] J. Minna,et al. Targeting ADAM-mediated ligand cleavage to inhibit HER3 and EGFR pathways in non-small cell lung cancer. , 2006, Cancer cell.

[32] U. Desai,et al. Designing allosteric regulators of thrombin. Exosite 2 features multiple subsites that can be targeted by sulfated small molecules for inducing inhibition. , 2013, Journal of medicinal chemistry.

[33] B. Roques,et al. Comparison of Fluorigenic Peptide Substrates PL50, SNAPtide, and BoTest A/E for BoNT/A Detection and Quantification , 2013, Journal of biomolecular screening.

[34] M. Giulianotti,et al. Discovery of Novel Inhibitors of a Disintegrin and Metalloprotease 17 (ADAM17) Using Glycosylated and Non-glycosylated Substrates* , 2012, The Journal of Biological Chemistry.

[35] M. Giulianotti,et al. SAR Studies of Exosite-Binding Substrate-Selective Inhibitors of A Disintegrin And Metalloprotease 17 (ADAM17) and Application as Selective in Vitro Probes. , 2015, Journal of medicinal chemistry.

[36] D. Soler,et al. Expression Cloning of the STRL33/BONZO/TYMSTR Ligand Reveals Elements of CC, CXC, and CX3C Chemokines , 2001, The Journal of Immunology.

[37] Jun Zou,et al. Crystal structure of the catalytic domain of human ADAM33. , 2004, Journal of molecular biology.

[38] J. Jiménez-Barbero,et al. Thermodynamic Switch in Binding of Adhesion/Growth Regulatory Human Galectin-3 to Tumor-Associated TF Antigen (CD176) and MUC1 Glycopeptides , 2015, Biochemistry.

[39] Patrick J. Curran,et al. The discovery of novel tartrate-based TNF-alpha converting enzyme (TACE) inhibitors. , 2010, Bioorganic & medicinal chemistry letters.

[40] P. Dempsey,et al. The ADAM10 Prodomain Is a Specific Inhibitor of ADAM10 Proteolytic Activity and Inhibits Cellular Shedding Events* , 2007, Journal of Biological Chemistry.

[41] V. Magdolen,et al. The alpha and beta subunits of the metalloprotease meprin are expressed in separate layers of human epidermis, revealing different functions in keratinocyte proliferation and differentiation. , 2007, Journal of Investigative Dermatology.

[42] Rommie E. Amaro,et al. POVME 2.0: An Enhanced Tool for Determining Pocket Shape and Volume Characteristics , 2014, Journal of chemical theory and computation.

[43] W. Ouwehand,et al. Cross-domain inhibition of TACE ectodomain , 2011, Proceedings of the National Academy of Sciences.

[44] V. Devita,et al. Trials and tribulations , 2008, Nature Clinical Practice Oncology.

[45] L. Marnett,et al. Substrate-selective COX-2 inhibition as a novel strategy for therapeutic endocannabinoid augmentation. , 2014, Trends in pharmacological sciences.

[46] N. Neff,et al. Purification of Her-2 extracellular domain and identification of its cleavage site. , 2003, Protein expression and purification.

[47] V. Dive,et al. Synthetic active site-directed inhibitors of metzincins: achievement and perspectives. , 2008, Molecular aspects of medicine.

[48] J. Spring,et al. Biology of the syndecans: a family of transmembrane heparan sulfate proteoglycans. , 1992, Annual review of cell biology.

[49] P. Saftig,et al. Leukocytes require ADAM10 but not ADAM17 for their migration and inflammatory recruitment into the alveolar space. , 2014, Blood.

[50] H. Jahr,et al. A transmembrane C-terminal fragment of syndecan-1 is generated by the metalloproteinase ADAM17 and promotes lung epithelial tumor cell migration and lung metastasis formation , 2015, Cellular and Molecular Life Sciences.

[51] T. Chou,et al. Quantitative analysis of dose-effect relationships: the combined effects of multiple drugs or enzyme inhibitors. , 1984, Advances in enzyme regulation.

[52] F. Echtermeyer,et al. Syndecan-4 core protein is sufficient for the assembly of focal adhesions and actin stress fibers. , 1999, Journal of cell science.

[53] Raphael Nudelman,et al. Drug Insight: tumor necrosis factor-converting enzyme as a pharmaceutical target for rheumatoid arthritis , 2008, Nature Clinical Practice Rheumatology.

[54] Robert A Copeland,et al. Evaluation of enzyme inhibitors in drug discovery. A guide for medicinal chemists and pharmacologists. , 2005, Methods of biochemical analysis.

[55] H. Krell,et al. Human meprin alpha and beta homo-oligomers: cleavage of basement membrane proteins and sensitivity to metalloprotease inhibitors. , 2004, The Biochemical journal.

[56] B. Fingleton,et al. Matrix Metalloproteinase Inhibitors and Cancer—Trials and Tribulations , 2002, Science.

[57] P. Murumkar,et al. Novel methods and strategies in the discovery of TACE inhibitors , 2013, Expert opinion on drug discovery.