Selective Inhibitors of Medium-Size S1′ Pocket Matrix Metalloproteinases: A Stepping Stone of Future Drug Discovery

Baidya, Sandip Kumar; Banerjee, S.; Adhikari, Nilanjan; Jha, Tarun

doi:10.1021/acs.jmedchem.1c01855

Cited by 20 publications

(9 citation statements)

References 209 publications

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“…Beside their poor pharmacokinetics and low oral availability/inability, this major failure has been mainly attributed to their lack of specificity within the MMP family and towards other metalloenzymes. Benefiting from a better understanding of MMP biology that emphasizes the necessity to selectively target one single MMP in a given pathological context, a new generation of selective MMPi has emerged recently ( 131 ). To achieve a better selectivity, several strategies have been deployed.…”

Section: Mmps Adams and Cd95l Regulationmentioning

confidence: 99%

“…To achieve a better selectivity, several strategies have been deployed. Regarding the small-molecule inhibitors they mainly consist in either replacing the hydroxamic acid group found in most of broad spectrum MMPis by a weaker Zn 2+ chelating moiety ( 132 , 133 ) or targeting exclusively the S1’ pocket which significantly differ between the MMPs ( 131 , 132 ). Alternatively, the development of surrogates of MMPs endogenous inhibitors such as TIMP analogs or targeting MMP gene expression using mRNAs have also been explored.…”

Section: Mmps Adams and Cd95l Regulationmentioning

confidence: 99%

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Role of metalloproteases in the CD95 signaling pathways

et al. 2022

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CD95L (also known as FasL or CD178) is a member of the tumor necrosis family (TNF) superfamily. Although this transmembrane ligand has been mainly considered as a potent apoptotic inducer in CD95 (Fas)-expressing cells, more recent studies pointed out its role in the implementation of non-apoptotic signals. Accordingly, this ligand has been associated with the aggravation of inflammation in different auto-immune disorders and in the metastatic occurrence in different cancers. Although it remains to decipher all key factors involved in the ambivalent role of this ligand, accumulating clues suggest that while the membrane bound CD95L triggers apoptosis, its soluble counterpart generated by metalloprotease-driven cleavage is responsible for its non-apoptotic functions. Nonetheless, the metalloproteases (MMPs and ADAMs) involved in the CD95L shedding, the cleavage sites and the different stoichiometries and functions of the soluble CD95L remain to be elucidated. To better understand how soluble CD95L triggers signaling pathways from apoptosis to inflammation or cell migration, we propose herein to summarize the different metalloproteases that have been described to be able to shed CD95L, their cleavage sites and the biological functions associated with the released ligands. Based on these new findings, the development of CD95/CD95L-targeting therapeutics is also discussed.

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Section: Mmps Adams and Cd95l Regulationmentioning

confidence: 99%

Section: Mmps Adams and Cd95l Regulationmentioning

confidence: 99%

Role of metalloproteases in the CD95 signaling pathways

et al. 2022

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“…Indeed, the small-molecule MMP inhibitors tested in clinical trials have shown uncertain efficacy and various side effects due to their poor selectivity. For this reason, selective MMP inhibitors have been actively investigated in recent years. − Because the depth of the S1′ pocket differs among MMP subtypes, suitable S1′ pocket-binding groups for each subtype have been explored for MMP selectivity. − …”

Section: Introductionmentioning

confidence: 99%

Discovery of TP0597850: A Selective, Chemically Stable, and Slow Tight-Binding Matrix Metalloproteinase-2 Inhibitor with a Phenylbenzamide–Pentapeptide Hybrid Scaffold

et al. 2023

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Matrix metalloproteinase-2 (MMP2) is a zinc-dependent endopeptidase and a promising target for various diseases, including cancer and fibrosis. Herein, we report the discovery of a novel MMP2selective inhibitor with high chemical stability and slow tight-binding features. Based on the degradation mechanism of our small-molecule− peptide hybrid 1, the tripeptide linker {5-aminopentanoic acid [Ape(5)]−Glu−Asp} of 1 was replaced by a shorter linker (γ-D-Glu). Phenylbenzamide was suitable for the new generation of MMP2 inhibitors as an S1′ pocket-binding group. The introduction of (4S)aminoproline dramatically increased the chemical stability while maintaining high subtype selectivity because of its interaction with Glu130. TP0597850 (18) exhibited high stability over a wide range of pH values as well as potent MMP2 inhibition (K i = 0.034 nM) and ≥2000-fold selectivity determined using the inhibition constants. A kinetic analysis revealed that it possesses slow tight-binding nature with a long MMP2 dissociative half-life (t 1/2 = 265 min).

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“…The study of the metalloenzymes in normal and pathophysiological conditions has elucidated several crucial involvements of these enzymes in a wide range of disease states, including cancer, neurodegenerative disorders, inflammation, osteoarthritis, cardiovascular diseases, viral and parasitic infections, as well as in epigenetic abnormalities. [1][2][3][4][5][6][7] Although several attempts were made to develop potential and selective inhibitors of such metalloenzymes, a few novel molecules have been approved to date for targeting such metalloenzyme-related pathophysiology and associated disease conditions. 8 Among these metalloenzymes, the Zn 2+ -dependent metalloenzyme meprin b is one of the metzincin superfamily proteases that modulates several substrates such as procollagen I, collagen IV, triggered receptor expressed on myeloid cells 2 (TREM 2), interleukin (IL)-6R, cluster of differentiation (CD) 109, CD99, MUC-2, amyloid precursor protein (APP), E-cadherin, and IL-1b.…”

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%