Farnesyl Pyrophosphate Inhibits Epithelialization and Wound Healing through the Glucocorticoid Receptor

Vukelic, S.; Stojadinović, Olivera; Pastar, Irena; Vouthounis, Constantinos; Krzyzanowska, Agata; Das, Sharmistha; Samuels, Herbert H.; Tomic‐Canic, Marjana

doi:10.1074/jbc.m109.016741

Cited by 58 publications

(93 citation statements)

References 39 publications

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“…This effect was due to the blockade of FPP's activation of the GR. 9 Taken together, this finding establishes a second, upstream mechanism whereby the stress hormone pathway can be activated in epidermis. The role of FPP in the pathogenesis of chronic wounds and their nonmigratory keratinocytes needs further investigation.…”

Section: Discussion Of Findings and Relevant Literaturementioning

confidence: 85%

“…9 However, studies have shown that enhanced keratinocyte migratory potential is not mediated through the inhibition of cholesterol synthesis despite the disrupted skin barrier. This effect was due to the blockade of FPP's activation of the GR.…”

Section: Discussion Of Findings and Relevant Literaturementioning

confidence: 99%

“…3 Similarly, topical mevastatin, an 3-hydroxy-3-methylglutaryl-CoA reductase inhibitor, reduces endogenous levels of FPP and increases epithelization in an ex vivo wound model. 9 Further, inclusion of a b2AR antagonist, timolol, reverses the inhibitory effects of epinephrine on keratinocyte migration and wound epithelization. 6 Systemic administration of a b2AR antagonist accelerates wound epithelization in an in vivo burn wound model.…”

Section: Discussion Of Findings and Relevant Literaturementioning

confidence: 99%

“…Two novel topical treatments, which are typically used to improve cardiovascular health, are proposed to improve wound healing: statins and beta-blockers. 5,9,19 Additionally, topical treatment with metyrapone, an inhibitor of CYP11B1, enhanced keratinocyte migration and wound epithelization.…”

Section: Innovationmentioning

confidence: 99%

“…A main branch point intermediate in the mevalonate pathway is FPP. 9 FPP can bind GR, thus causing many of the same deleterious effects as GCs during the wound healing process. Each is shown to inhibit keratinocyte migration and wound epithelization through a similar mechanism by targeting expression of the early wound healing markers, keratin 6 and 16.…”

Section: Relevant Basic Science Contextmentioning

confidence: 99%

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Stress-Induced Hormones Cortisol and Epinephrine Impair Wound Epithelization

Stojadinović

Gordon

Lebrun

et al. 2012

Advances in Wound Care

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Section: Discussion Of Findings and Relevant Literaturementioning

confidence: 85%

Section: Discussion Of Findings and Relevant Literaturementioning

confidence: 99%

Section: Discussion Of Findings and Relevant Literaturementioning

confidence: 99%

Section: Innovationmentioning

confidence: 99%

Section: Relevant Basic Science Contextmentioning

confidence: 99%

See 3 more Smart Citations

Stress-Induced Hormones Cortisol and Epinephrine Impair Wound Epithelization

Stojadinović

Gordon

Lebrun

et al. 2012

Advances in Wound Care

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Statins as anti‐tumor agents: A paradigm for repurposed drugs

Tripathi,

Gupta,

Galande

2024

Cancer Reports

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BackgroundStatins, frequently prescribed medications, work by inhibiting the rate‐limiting enzyme HMG‐CoA reductase (HMGCR) in the mevalonate pathway to reduce cholesterol levels. Due to their multifaceted benefits, statins are being adapted for use as cost‐efficient, safe and effective anti‐cancer treatments. Several studies have shown that specific types of cancer are responsive to statin medications since they rely on the mevalonate pathway for their growth and survival.Recent FindingsStatin are a class of drugs known for their potent inhibition of cholesterol production and are typically prescribed to treat high cholesterol levels. Nevertheless, there is growing interest in repurposing statins for the treatment of malignant neoplastic diseases, often in conjunction with chemotherapy and radiotherapy. The mechanism behind statin treatment includes targeting apoptosis through the BCL2 signaling pathway, regulating the cell cycle via the p53‐YAP axis, and imparting epigenetic modulations by altering methylation patterns on CpG islands and histone acetylation by downregulating DNMTs and HDACs respectively. Notably, some studies have suggested a potential chemo‐preventive effect, as decreased occurrence of tumor relapse and enhanced survival rate were reported in patients undergoing long‐term statin therapy. However, the definitive endorsement of statin usage in cancer therapy hinges on population based clinical studies with larger patient cohorts and extended follow‐up periods.ConclusionsThe potential of anti‐cancer properties of statins seems to reach beyond their influence on cholesterol production. Further investigations are necessary to uncover their effects on cancer promoting signaling pathways. Given their distinct attributes, statins might emerge as promising contenders in the fight against tumorigenesis, as they appear to enhance the efficacy and address the limitations of conventional cancer treatments.

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The effects of direct inhibition of geranylgeranyl pyrophosphate synthase on osteoblast differentiation

Weivoda

Hohl

2011

J. Cell. Biochem.

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Statins, drugs commonly used to lower serum cholesterol, have been shown to stimulate osteoblast differentiation and bone formation. These effects have been attributed to the depletion of geranylgeranyl pyrophosphate (GGPP). In this study, we tested whether specific inhibition of GGPP synthase (GGPPS) with digeranyl bisphosphonate (DGBP) would similarly lead to increased osteoblast differentiation. DGBP concentration dependently decreased intracellular GGPP levels in MC3T3-E1 pre-osteoblasts and primary rat calvarial osteoblasts, leading to impaired Rap1a geranylgeranylation. In contrast to our hypothesis, 1 µM DGBP inhibited matrix mineralization in the MC3T3-E1 pre-osteoblasts. Consistent with this, DGBP inhibited the expression of alkaline phosphatase and osteocalcin in primary osteoblasts. By inhibiting GGPPS, DGBP caused an accumulation of the GGPPS substrate farnesyl pyrophosphate (FPP). This effect was observed throughout the time course of MC3T3-E1 pre-osteoblast differentiation. Interestingly, DGBP treatment led to activation of the glucocorticoid receptor in MC3T3-E1 pre-osteoblast cells, consistent with recent findings that FPP activates nuclear hormone receptors. These findings demonstrate that direct inhibition of GGPPS, and the resulting specific depletion of GGPP, does not stimulate osteoblast differentiation. This suggests that in addition to depletion of GGPP, statin-stimulated osteoblast differentiation may depend on the depletion of upstream isoprenoids, including FPP.

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Farnesyl Pyrophosphate Inhibits Epithelialization and Wound Healing through the Glucocorticoid Receptor

Cited by 58 publications

References 39 publications

Stress-Induced Hormones Cortisol and Epinephrine Impair Wound Epithelization

Stress-Induced Hormones Cortisol and Epinephrine Impair Wound Epithelization

Statins as anti‐tumor agents: A paradigm for repurposed drugs

The effects of direct inhibition of geranylgeranyl pyrophosphate synthase on osteoblast differentiation

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