Development of Selective Inhibitors and Substrate of Matrix Metalloproteinase-12

Devel, Laurent; Rogakos, Vassilis; David, Arnaud; Makaritis, A.; Beau, Fabrice; Cuniasse, Philippe; Yiotakis, Athanasios; Dive, Vincent

doi:10.1074/jbc.m600222200

Cited by 140 publications

(165 citation statements)

References 53 publications

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“…Indeed, MMPs contributed to joint disease in other MPS models [44] while cathepsin S was upregulated in the brain of MPS I mice [45]. If the genetic cross that is in progress shows that deficiency of one or both of these elastase proteins can reduce aortic disease in MPS I, it might be possible to treat MPS I patients with inhibitors of MMP-12 [46] and/or cathepsin S [47]. Evaluation of transcription factor mRNA in aorta.…”

Section: Implications Of This Studymentioning

confidence: 99%

Upregulation of elastase proteins results in aortic dilatation in mucopolysaccharidosis I mice

Tittiger

Knutsen

et al. 2008

Molecular Genetics and Metabolism

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Mucopolysaccharidosis I (MPS I), known as Hurler syndrome in the severe form, is a lysosomal storage disease due to -L-iduronidase (IDUA) deficiency. It results in fragmentation of elastin fibers in the aorta and heart valves via mechanisms that are unclear, but may result from the accumulation of the glycosaminoglycans heparan and dermatan sulfate. Elastin fragmentation causes aortic dilatation and valvular insufficiency, which can result in cardiovascular disease. The pathophysiology of aortic disease was evaluated in MPS I mice. MPS I mice have normal elastic fiber structure and aortic compliance at early ages, which suggests that elastin assembly is normal. Elastin fragmentation and aortic dilatation are severe at 6 months, which is temporally associated with marked increases in mRNA and enzyme activity for two elastin-degrading proteins, matrix metalloproteinase-12 (MMP-12) and cathepsin S. Upregulation of these genes likely involves activation of STAT proteins, which may be induced by structural stress to smooth muscle cells from accumulation of glycosaminoglycans in lysosomes. Neonatal intravenous injection of a retroviral vector normalized MMP-12 and cathepsin S mRNA levels and prevented aortic disease. We conclude that aortic dilatation in MPS I mice is likely due to degradation of elastin by MMP-12 and/or cathepsin S. This aspect of disease might be ameliorated by inhibition of the signal transduction pathways that upregulate expression of elastase proteins, or by inhibition of elastase activity. This could result in a treatment for patients with MPS I, and might reduce aortic aneurism formation in other disorders.

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Section: Implications Of This Studymentioning

confidence: 99%

Upregulation of elastase proteins results in aortic dilatation in mucopolysaccharidosis I mice

Tittiger

Knutsen

et al. 2008

Molecular Genetics and Metabolism

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“…Several potent inhibitors for MMP-12, such as phospinic peptides, sulfonamides, and bisphosphonic derivatives, have already been designed and tested. 5−10 For some of them a high selectivity toward MMP-12 has been observed, 5,6,8,10 although the molecular basis of this specificity is still a matter of research. Here, based on the classical arylsulfonamide scaffold, new MMP inhibitors were designed by introducing an ethylene linker between the sulfonamide moiety and the P1′ aromatic portion and by replacing the glycine residue with a D-proline within the zinc-binding group (ZBG).…”

mentioning

confidence: 99%

Discovery of a New Class of Potent MMP Inhibitors by Structure-Based Optimization of the Arylsulfonamide Scaffold

Mori

Massaro

Calderone

et al. 2013

ACS Med. Chem. Lett.

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A new class of potent matrix metalloproteinase (MMP) inhibitors designed by structure-based optimization of the well-known arylsulfonamide scaffold is presented. Molecules show an ethylene linker connecting the sulfonamide group with the P1′ aromatic portion and a D-proline residue bearing the zinc-binding group. The affinity improvement provided by these modifications led us to discover a nanomolar MMP inhibitor bearing a carboxylate moiety as zinc-binding group, which might be a promising lead molecule. Notably, a significant selectivity for MMP-8, MMP-12, and MMP-13 was observed with respect to MMP-1 and MMP-7. KEYWORDS: MMP, X-ray, synthesis, desolvation, docking, free energy M atrix metalloproteinases (MMPs) are a family of extracellular zinc-and calcium-dependent endopeptidases involved in the degradation and remodeling of extracellular matrix components, cell movement, proliferation, and tissues remodeling. 1,2 Aberrant MMPs activities are involved in several pathological states, and the design of synthetic MMP inhibitors represents an opportunity to develop new drug candidates. Recently, we reported on the use of a MMP-9 inhibitor for the potential treatment of Dry Eye Syndrome. 3 Here, we present a new scaffold for potent MMP inhibitors that was discovered by means of an integrated medicinal chemistry study, composed of computer-aided design, synthesis, X-ray analysis, and fluorimetric measurement of the binding affinity toward MMPs. A new strategy to improve the inhibitory activity toward MMPs by increasing the interactions with the S1′ pocket and, especially, by increasing the ligand solvation free energy is further presented. The different contributions to the binding affinity were further investigated with computational methods. 4 Human macrophagic metalloelastase (MMP-12) was selected as target because of its pathological relevance and of the availability of detailed structural information. Several potent inhibitors for MMP-12, such as phospinic peptides, sulfonamides, and bisphosphonic derivatives, have already been designed and tested. 5−10 For some of them a high selectivity toward MMP-12 has been observed, 5,6,8,10 although the molecular basis of this specificity is still a matter of research. Here, based on the classical arylsulfonamide scaffold, new MMP inhibitors were designed by introducing an ethylene linker between the sulfonamide moiety and the P1′ aromatic portion and by replacing the glycine residue with a D-proline within the zinc-binding group (ZBG). 11,12 The flexible linker was introduced to increase van der Waals interactions with the deep S1′ lipophilic cavity of MMPs, 13 without affecting the overall ligand binding mode. At the same time, the hydroxamate derivative of the rigid D-proline was evaluated as ZBGs for its possible favorable contribution to the solvation free energy of the ligand. It is interesting to note that these chemical substitutions do not sizably affect the ligand logP values, that remain within the tolerance limits described by the rule of three and...

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“…15 N and 15 N, 13 C labelled proteins were expressed from a pGEMEX expression plasmid (Promega) in an E. coli BL21(DE3) RIL host using 15 NH 4 CI and 13 Cglucose-based M9 medium supplemented with Celtone (Spectral Stable Isotopes) at 20% (v/ v). The expressed protein is found in inclusion bodies.…”

Section: Mmp-12 Samplesmentioning

confidence: 99%

Solution Structure of Inhibitor-Free Human Metalloelastase (MMP-12) Indicates an Internal Conformational Adjustment

Bhaskaran

Palmier

Bagegni

et al. 2007

Journal of Molecular Biology

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Macrophage metalloelastase or MMP-12 appears to exacerbate atherosclerosis, emphysema, aortic aneurysm, rheumatoid arthritis, and inflammatory bowel disease. An inactivating E219A mutation, validated by crystallography and NMR spectra, prevents autolysis of MMP-12 and allowed us to determine its NMR structure without an inhibitor. The structural ensemble of the catalytic domain without inhibitor is based on 2813 NOEs and has an average RMSD to the mean of 0.25 Å for the backbone and 0.61 Å for all heavy atoms for residues Trp109 -Gly263. Compared to crystal structures of MMP-12, helix B (hB) at the active site is unexpectedly more deeply recessed under the betasheet. This opens a pocket between hB and β-strand sIV in the active site cleft. Both hB and an internal cavity are shifted toward β-strands sI and sIII and hA on the back side of the protease. About 25 internal NOE contacts distinguish the inhibitor-free solution structure and indicate hB's greater depth and proximity to the sheet and hA. Line broadening and multiplicity of amide proton NMR peaks from hB are consistent with hB undergoing slow conformational exchange among subtly different environments. Inhibitor binding-induced perturbations of NMR spectra of MMP-1 and -3 map to similar locations across MMP-12 and encompassing its internal conformational adjustments. Evolutionary trace analysis suggests a functionally important network of residues that encompasses most of the locations that adjust in conformation, including 18 residues with NOE contacts unique to inhibitor-free MMP-12. The conformational change, sequence analysis, and inhibitor perturbations of NMR spectra agree in the network they identify between structural scaffold and active site of MMPs.

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Development of Selective Inhibitors and Substrate of Matrix Metalloproteinase-12

Cited by 140 publications

References 53 publications

Upregulation of elastase proteins results in aortic dilatation in mucopolysaccharidosis I mice

Upregulation of elastase proteins results in aortic dilatation in mucopolysaccharidosis I mice

Discovery of a New Class of Potent MMP Inhibitors by Structure-Based Optimization of the Arylsulfonamide Scaffold

Solution Structure of Inhibitor-Free Human Metalloelastase (MMP-12) Indicates an Internal Conformational Adjustment

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