Inhibition of human prostate cancer growth, osteolysis and angiogenesis in a bone metastasis model by a novel mechanism‐based selective gelatinase inhibitor

Bonfil, R. Daniel; Sabbota, Aaron; Nabha, Sanaa; Bernardo, M. Margarida; Dong, Zhong; Meng, Hong; Yamamoto, Hamilto Akihissa; Chinni, Sreenivasa R.; Lim, Int Taek; Chang, Mayland; Filetti, Lusia C.; Mobashery, Shahriar; Cher, Michael L.; Fridman, Rafael

doi:10.1002/ijc.21645

Cited by 90 publications

(94 citation statements)

References 35 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…To block MMP-9, we used the specific inhibitor, SB-3CT. SB-3CT is a highly selective mechanism-based gelatinase inhibitor with particular specificity for MMP-9 and has previously been shown to specifically inhibit MMP-9-driven pathways in disease models in vivo (Gu et al, 2005;Bonfil et al, 2006). We verified this selectivity in vitro; SB-3CT inhibited MMP-9-but not MMP-2-mediated gelatinase activity in medium from IL-1␤-treated glial cells.…”

Section: Methodssupporting

confidence: 52%

Systemic Inflammation Alters the Kinetics of Cerebrovascular Tight Junction Disruption after Experimental Stroke in Mice

McColl¹,

Rothwell²,

Allan³

2008

J. Neurosci.

282

262

View full text Add to dashboard Cite

Systemic inflammatory events, such as infection, increase the risk of stroke and are associated with worse outcome, but the mediators of this clinically important effect are unknown. Our aim here was to elucidate mechanisms contributing to the detrimental effects of systemic inflammation on mild ischemic brain injury in mice. Systemic inflammation was induced in mice by peripheral interleukin-1␤ (IL-1␤) challenge and focal cerebral ischemia by transient middle cerebral artery occlusion (MCAo). Systemic inflammation caused an alteration in the kinetics of blood-brain barrier (BBB) disruption through conversion of a transient to a sustained disruption of the tight junction protein, claudin-5, and also markedly exacerbated disruption to the cerebrovascular basal lamina protein, collagen-IV. These alterations were associated with a systemic inflammation-induced increase in neurovascular gelatinolytic activity that was mediated by a fivefold increase in neutrophil-derived matrix metalloproteinase-9 (MMP-9) in the brains of IL-1␤-challenged mice after MCAo. Specific inhibition of MMP-9 abrogated the effects of systemic inflammation on the sustained but not the acute disruption of claudin-5, which was associated with phosphorylation of cerebrovascular myosin light chain. MMP-9 inhibition also attenuated the deleterious impact of systemic inflammation on brain damage, edema, neurological deficit, and incidence of hemorrhagic transformation. These data indicate that a transformation from transient to sustained BBB disruption caused by enhanced neutrophil-derived neurovascular MMP-9 activity is a critical mechanism underlying the exacerbation of ischemic brain injury by systemic inflammation. These mechanisms may contribute to the poor clinical outcome in stroke patients presenting with antecedent infection.

show abstract

Section: Methodssupporting

confidence: 52%

Systemic Inflammation Alters the Kinetics of Cerebrovascular Tight Junction Disruption after Experimental Stroke in Mice

McColl¹,

Rothwell²,

Allan³

2008

J. Neurosci.

282

262

View full text Add to dashboard Cite

show abstract

“…The efficacy of SB3-CT was demonstrated in several distinct models where the functional activity of gelatinases was relevant to the disease. Thus, intraperitoneal treatment with SB-3CT (50 mg/kg) inhibited intraosseous growth of human PC3 cells within the marrow of human fetal femur fragments previously implanted in SCID mice (21). In a transient focal cerebral ischemia model of stroke in mice, MMP-9 contributes directly to neuron apoptosis and brain damage (22) by degrading the extracellular matrix laminin.…”

Section: Invasion-promoting Mt1-mmp In Cancermentioning

confidence: 96%

Defining the roles of T cell membrane proteinase and CD44 in type 1 diabetes

Savinov

Strongin

2007

IUBMB Life

View full text Add to dashboard Cite

SummaryMembrane type-1 matrix metalloproteinase (MT1-MMP) shedding of the signaling and adhesion CD44 receptor plays a significant role in stimulating cancer cells locomotion. Similarly, and unexpectedly, MT1-MMP-dependent shedding of CD44 plays an equally significant role in regulating the adhesion to the pancreatic vasculature and also in the concomitant transendothelial migration and intra-islet homing of the diabetogenic, cytotoxic, T cells. Inactivation of the T cell MT1-MMP functionality by clinically tested, synthetic inhibitors leads to an extended immobilization of the T killer cells on the pancreatic vasculature and, subsequently, to immunosuppression because of the cessation of the T cell transmigration and homing. Injections of insulin jointly with an MT1-MMP inhibitor stimulated the regeneration of functional, insulin-producing, b-cells in acutely diseased non-obese diabetic (NOD) mice. After insulin injections were suspended and inhibitor injections continued, diabetic NOD mice maintained mild hyperglycemia and did not require further insulin injections for survival. Overall, these data provide a substantive mechanistic rationale for clinical trials of the inhibitors of MT1-MMP in human type 1 diabetes. IUBMB Life, 59: 6-13, 2007

show abstract

“…These MMPIs contain a specific group that coordinate the Zn 2+ in the active site, resulting in a conformational change and a covalent attachment that prevent MMP dissociation. 25 The first mechanism-based inhibitor of MMPs was SB3CT, a selective inhibitor toward MMP-2 and MMP-9, that, in preclinical studies, has shown anticancer properties, 26 as well …”

Section: Exogenous Synthetic Mmp Inhibitorsmentioning

confidence: 99%

Metalloproteinases and their inhibitors as therapeutic targets for multiple sclerosis: current evidence and future perspectives

Latronico¹,

Liuzzi²

2017

MNM

View full text Add to dashboard Cite

Abstract:The treatment of multiple sclerosis (MS) has seen important changes in the last two decades with the introduction of several drugs able to modify the evolution of this disease. Current MS therapies primarily target the peripheral immune response, although it has been suggested that their efficacy could be in part the result of the beneficial effect on other nonspecific targets, such as matrix metalloproteinases (MMPs). Numerous experimental studies have suggested that MMPs may be involved in MS pathogenesis by contributing to blood-brain barrier disruption, migration of leukocytes into the central nervous system, demyelination and axonal damage. Therefore, MMPs have been considered important therapeutic targets in the course of MS. In this respect, different attempts have been made to develop synthetic, low-molecular-weight inhibitors of MMPs for the potential treatment of diseases in which MMPs play a major role. However, technical difficulties, side effects and reduced patient compliance because of parenteral administration have greatly limited the development in the clinical practice of specific anti-MMP drugs. By contrast, interesting results have been obtained with compounds that are already used in the clinical practice, such as MS drugs and natural compounds with anti-inflammatory and antioxidant activity. Here, we discuss the evidence and potential mechanisms for altered MMP function in MS. Furthermore, we outline the possible medical implications for the use of compounds that target MMP activity and we propose that together with anti-MS drugs, other compounds with anti-inflammatory and antioxidant properties, such as natural ω3 fatty acids, polyphenols and tetracyclines, which inhibit MMP functions, might represent potential therapeutic approaches to mitigate MMP-related damage during MS.

show abstract

Inhibition of human prostate cancer growth, osteolysis and angiogenesis in a bone metastasis model by a novel mechanism‐based selective gelatinase inhibitor

Cited by 90 publications

References 35 publications

Systemic Inflammation Alters the Kinetics of Cerebrovascular Tight Junction Disruption after Experimental Stroke in Mice

Systemic Inflammation Alters the Kinetics of Cerebrovascular Tight Junction Disruption after Experimental Stroke in Mice

Defining the roles of T cell membrane proteinase and CD44 in type 1 diabetes

Metalloproteinases and their inhibitors as therapeutic targets for multiple sclerosis: current evidence and future perspectives

Contact Info

Product

Resources

About