Discovery of a highly selective chemical inhibitor of matrix metalloproteinase-9 (MMP-9) that allosterically inhibits zymogen activation

Scannevin, Robert H.; Alexander, Richard; Haarlander, Tara Mezzasalma; Burke, Sharon L.; Singer, Monica; Huo, Cuifen; Zhang, Yuemei; Maguire, Diane; Spurlino, John; Deckman, Ingrid C.; Carroll, Karen; Lewandowski, Frank; Devine, Eric; Dzordzorme, Keli C.; Tounge, Brett A.; Milligan, Cindy; Bayoumy, Shariff; Williams, Robyn; Schalk-Hihi, Céline; Leonard, Kristi; Jackson, Paul F.; Todd, Matthew J.; Kuo, Lawrence C.; Rhodes, Kenneth J.

doi:10.1074/jbc.m117.806075

Cited by 103 publications

(88 citation statements)

References 60 publications

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“…Although results from early animal studies utilizing broad spectrum inhibitors were compelling, it was determined that inhibiting such a broad scale inhibition of MMPs interfered with normal tissue function, which could support disease progression (66, 67). Moreover, MMP-9 active site inhibitors were prone to off target binding which induced unexpected malignancies including musculoskeletal toxicity (68).…”

Section: Discussionmentioning

confidence: 99%

Merkel Cell Polyomavirus Small Tumor Antigen Activates Matrix Metallopeptidase-9 Gene Expression for Cell Migration and Invasion

Nwogu

Ortiz

Whitehouse³

et al. 2020

Preprint

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46Merkel cell polyomavirus (MCV) small T antigen (sT) is the main oncoprotein for the 47 development of Merkel cell carcinoma (MCC). MCC is a rare, clinically aggressive 48 neuroendocrine tumor of the skin with a high propensity for local, regional, and distant 49 spread. The expression of matrix metalloproteinase (MMP)-9 has been implicated as 50 playing an important role in cell invasion and metastasis in many human cancers. 51Previously, MCV sT has been shown to increase the cell migration and invasiveness of 52 MCC cells through the transcriptional activation of the sheddase molecule, ADAM 10 (A 53 disintergrin and metalloprotease domain-containing protein 10). In this study, we show 54 that MCV sT protein stimulates epithelial-mesenchymal transition (EMT) gene 55 expression, including MMP-9. This effect is dependent on the presence of the large 56 stabilization domain (LSD), which is known to be responsible for cell transformation 57 through targeting of promiscuous E3 ligases, including FBW7, a known MMP-9 58 regulator. Chemical treatments of MMP-9 markedly inhibited sT-induced cell migration 59 and invasion. These results suggest that sT contributes to the activation of MMP-9 as a 60 result of FBW7 targeting, and increases the invasive potential of cells, which can be 61 used for a targeted therapeutic intervention. 62 63 IMPORTANCE 64Merkel cell carcinoma (MCC) is the most aggressive cutaneous tumor without clearly 65 defined treatment. Although MCC has high propensity for metastasis, little is known about 66 the underlying mechanisms that drive MCC invasion and metastatic progression. MMP-9 67 has shown to play a detrimental role in many metastatic human cancers, including 68 melanoma and other non-melanoma skin cancers. Our study discovers that MCV sT-69 mediated MMP-9 activation is driven through the LSD, a known E3 ligase targeting 70 domain, in MCC. MMP-9 may serve as the biochemical culprit to target and develop a 71 novel approach for the treatment of metastatic MCC. 72 5333. Kaae J, Hansen AV, Biggar RJ, Boyd HA, Moore PS, Wohlfahrt J, Melbye M. 534

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Section: Discussionmentioning

confidence: 99%

Merkel Cell Polyomavirus Small Tumor Antigen Activates Matrix Metallopeptidase-9 Gene Expression for Cell Migration and Invasion

Nwogu

Ortiz

Whitehouse³

et al. 2020

Preprint

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“…None of the 50some clinical trials with MMP inhibitors were successful, due to off-target toxicity or absence of efficacy. A recent study reports effective allosteric prevention of pro-MMP-9 activation in a mouse neuroinflammatory model by a small, highly selective heterocyclic chemical inhibitor [204]. This orally administered compound does not prevent activation of the structurally related pro-MMP-2, and does not inhibit catalytically active MMP-1, −2, −3, −9 or −14.…”

Section: Proteolysis-related Processes As Drug Targetsmentioning

confidence: 99%

“…Additional allosteric, exosite and effector-binding site interactions are expected to contribute significantly to exclusive selection of the target protease. Structural conservation of the specificity site throughout a protease family with diverse catalytic properties and biological targets may pose a problem in designing specific drugs, and a promising alternative was developed by targeting zymogen activation rather than the active protease [204]. A highly selective compound that allosterically inhibits MMP-9 activation by binding to a pocket near the zymogen cleavage site may be a first viable drug candidate.…”

Section: The Future Of Proteolysis-related Drug and Diagnostic Develomentioning

confidence: 99%

Proteases: Pivot Points in Functional Proteomics

Verhamme

Leonard

Perkins

2018

Functional Proteomics

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Proteases drive the life cycle of all proteins, ensuring the transportation and activation of newly minted, would-be proteins into their functional form while recycling spent or unneeded proteins. Far from their image as engines of protein digestion, proteases play fundamental roles in basic physiology and regulation at multiple levels of systems biology. Proteases are intimately associated with disease and modulation of proteolytic activity is the presumed target for successful therapeutics. “Proteases: Pivot Points in Functional Proteomics” examines the crucial roles of proteolysis across a wide range of physiological processes and diseases. The existing and potential impacts of proteolysis-related activity on drug and biomarker development are presented in detail. All told the decisive roles of proteases in four major categories comprising 23 separate sub-categories are addressed. Within this construct, 15 sets of subject-specific, tabulated data are presented that include identification of proteases, protease inhibitors, substrates and their actions. Said data are derived from and confirmed by over 300 references. Cross comparison of datasets indicates that proteases, their inhibitors/promoters and substrates intersect over a range of physiological processes and diseases, both chronic and pathogenic. Indeed, “Proteases: Pivot Points …” closes by dramatizing this very point through association of (pro)Thrombin and Fibrin(ogen) with: hemostasis, innate immunity, cardiovascular and metabolic disease, cancer, neurodegeneration and bacterial self-defense.

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“…C, the chemical structure of compound JNJ0966. D, a novel approach by Scannevin et al (9), in which the MMPI (green) targets the final activation point of the zymogen and prevents prodomain (blue) removal. This MMPI does not inhibit the mature MMP.…”

Section: Figure 1 Mechanisms Of Mmp Inhibitorsmentioning

confidence: 99%

“…As one role of MMPs in cancer is associated with excessive activity, blocking zymogen activation could provide a fairly targeted mechanism to disrupt cancer development. The conceptually simple but elegant working hypothesis, then, of Scannevin et al (9), is that repressing activation of the zymogen could be an alternate approach to preventing activity. Using high-throughput screening employing the ThermoFluor approach, which reports on protein stability variations due to ligand binding, the authors identified compound JNJ0966 (Fig.…”

mentioning

confidence: 99%

Third time lucky? Getting a grip on matrix metalloproteinases

Gomis‐Rüth

2017

Journal of Biological Chemistry

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Edited by Norma AllewellDrug candidates against matrix metalloproteinases (MMPs) failed in the clinic in the past because their strong zinc-targeting warheads led to a lack of specificity. More recently, significant selectivity among MMPs was achieved by blocking the enzymes' specificity pockets, nearby exosites, and downstream domains. Scannevin and colleagues now elegantly twist the plot and achieve ultimate selectivity: They target MMP-9 by allosterically preventing activation of its zymogen.The matrix metalloproteinases (MMPs) 2 are a family of zincdependent metallopeptidases belonging to the metzincin clan (1, 2). They are multidomain enzymes containing a prodomain that is proteolytically cleaved in one or more steps to activate the enzyme, a catalytic domain containing the reactive zinc ion, and several other structural and functional domains (1). MMPs were initially discovered 55 years ago as active factors in frog metamorphosis, in which they act as general degraders of extracellular matrix components (3). For decades, the few orthologs known in humans were also those that nonspecifically degraded extracellular matrix proteins, a process associated with metastasis and angiogenesis in cancer. As a result, these enzymes were viewed as promising anticancer targets, inspiring efforts to develop MMP inhibitors (MMPIs). The initial generations of MMPIs were small-molecule peptidomimetics equipped with a warhead that very strongly targeted the catalytic zinc ion (e.g. batimastat, ilomastat, marimastat, and prinomastat; Fig. 1 A), but these displayed low specificity. Discouragingly, they failed in clinical trials due to lack of efficacy (4); to date, the only approved MMPI is Periostat (doxycycline) for the treatment of chronic periodontitis, which displays only modest efficacy (5).Over the decades, the known palette of MMP orthologs in humans reached 23, and their physiological functions expanded well beyond indiscriminate protein degradation to sophisticated (in)activation or shedding of a plethora of proteins, including growth factors, chemokines and other cytokines. It is now well established that MMPs contribute to various inflammatory, immune, infectious, and repair processes. As we've learned more about these vast functions, the basis for the failure of the initial zinc-targeting and therefore nonspecific MMPIs has become clear: General MMP inhibition leads to off-target effects and is thus not a viable strategy (6).These clinical failures, combined with the increasing knowledge regarding the complexity of MMP biology, led to a period during which pharmaceutical companies discontinued their pipelines for the development of MMPIs. However, the field has gradually reemerged through the development of highly selective inhibitors for each of the biomedically relevant MMPs. This generation of small-molecule MMPIs does not possess strong zinc-binding groups; instead, they are designed to complement one of pockets within the active-site cleft, the specificity pocket, which diverges among MMPs. They also tackle...

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Discovery of a highly selective chemical inhibitor of matrix metalloproteinase-9 (MMP-9) that allosterically inhibits zymogen activation

Cited by 103 publications

References 60 publications

Merkel Cell Polyomavirus Small Tumor Antigen Activates Matrix Metallopeptidase-9 Gene Expression for Cell Migration and Invasion

Merkel Cell Polyomavirus Small Tumor Antigen Activates Matrix Metallopeptidase-9 Gene Expression for Cell Migration and Invasion

Proteases: Pivot Points in Functional Proteomics

Third time lucky? Getting a grip on matrix metalloproteinases

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