Repeat Dose Study of the Cancer Chemopreventive Agent Resveratrol in Healthy Volunteers: Safety, Pharmacokinetics, and Effect on the Insulin-like Growth Factor Axis

Brown, Victoria; Patel, Ketan; Viskaduraki, Maria; Crowell, James A.; Perloff, Marjorie; Booth, Tristan D.; Vasilinin, Grygoriy; Sen, Ananda; Schinas, Anna Maria; Piccirilli, Gianfranca; Brown, Karen; Steward, William P.; Gescher, Andreas J.; Brenner, Dean E.

doi:10.1158/0008-5472.can-10-2364

Cited by 547 publications

(530 citation statements)

References 32 publications

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“…Mechanisms responsible for the resveratrol chemopreventive and chemosensitization properties are poorly known in tumor cells, but evidence indicates that resveratrol uptake and the cancer microenvironment plasma membrane play a key role in these processes. Here, we show that resveratrol activates MAPK pathways to induce apoptosis both in colon carcinoma cell lines and in leukemic lymphoma cells but not in normal cells such as human normal monocytes or rat nontransformed intestinal cells in accordance with recent phase I/ II trials showing the absence of resveratrol toxicity (28). The inhibition of resveratrol-induced apoptosis by monensin in tumor cells suggests a clathrin-independent endocytosis of the compound.…”

Section: Discussionsupporting

confidence: 89%

Endocytosis of Resveratrol via Lipid Rafts and Activation of Downstream Signaling Pathways in Cancer Cells

Colin

Limagne²,

Jeanningros³

et al. 2011

Cancer Prevention Research

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trans-Resveratrol has been proposed to prevent tumor growth and to sensitize cancer cells to anticancer agents. Polyphenol entry into the cells has remained poorly understood. Here, we show that [ 3 H]-resveratrol enters colon cancer cells (SW480, SW620, HT29) and leukemia U937 cells through a monensin (5-20 mmol/L) -sensitive process that suggests clathrin-independent endocytosis. Uptake of the molecule can be prevented by methyl-b-cyclodextrin (2-12 mg/mL), nystatin (12 ng/mL), and filipin (1 mg/mL), which all disrupt plasma membrane lipid rafts. Accordingly, radiolabeled resveratrol accumulates in sphingomyelin-and cholesterol-enriched cell fractions. Interestingly, extracellular signalregulated kinases (ERK), c-Jun NH 2 -terminal kinases (JNK), and Akt also accumulate in lipid rafts on resveratrol exposure (IC 50 at 48 h % 30 mmol/L in SW480 and U937 cells). In these rafts also, resveratrol promotes the recruitment, by the integrin a V b 3 (revealed by coimmunoprecipitation with an anti-integrin a V b 3 antibody), of signaling molecules that include the FAK (focal adhesion kinase), Fyn, Grb2, Ras, and SOS proteins. Resveratrol-induced activation of downstream signaling pathways and caspase-dependent apoptosis is prevented by endocytosis inhibitors, lipid raft-disrupting molecules, and the integrin antagonist peptide arginine-glycine-aspartate (500 nmol/L). Altogether, these data show the role played by lipid rafts in resveratrol endocytosis and activation of downstream pathways leading to cell death.

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Section: Discussionsupporting

confidence: 89%

Endocytosis of Resveratrol via Lipid Rafts and Activation of Downstream Signaling Pathways in Cancer Cells

Colin

Limagne²,

Jeanningros³

et al. 2011

Cancer Prevention Research

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“…For example, oral administration of a single high dose of resveratrol (100 mg/kg) in mice with or without piperine (10 mg/kg) supplementation resulted in a dramatic increase in maximum plasma resveratrol concentration from 10 to 154 M (63). Furthermore, a repeated dose of resveratrol up to 5 g/day, which is equivalent to ϳ85 mg/kg for a 60-kg man, has been shown to be safe in humans (64). Because piceatannol is often compared with resveratrol due to their similar chemical structures, these studies underscore the importance of the development of a novel piceatannol formulation that would allow us to overcome its poor solubility and bioavailability in vivo, thereby achieving elevated plasma concentration of piceatannol for exerting its maximum health benefit.…”

Section: Discussionmentioning

confidence: 99%

Piceatannol, Natural Polyphenolic Stilbene, Inhibits Adipogenesis via Modulation of Mitotic Clonal Expansion and Insulin Receptor-dependent Insulin Signaling in Early Phase of Differentiation

Kwon

Seo

Heo

et al. 2012

Journal of Biological Chemistry

115

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Background: Adipogenesis contributes to the increase in adipose tissue mass. Results: Preadipocytes treated with piceatannol showed reduced adipogenesis with impairment of the early cell cycle progress and insulin-signaling pathway. Conclusion:The anti-adipogenic function of piceatannol is through inhibition of mitotic clonal expansion and insulin receptor activity in the early phase of adipogenesis. Significance: Piceatannol is a novel anti-adipogenic compound that could modulate development of adipose tissue.

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“…The greatest plasma trans-resveratrol concentrations have been reported by Boocock et al [29] and Brown et al [30], both of whom supplemented humans with up to 5 g trans-resveratrol. 5 g trans-resveratrol as a single dose resulted in a 24 h mean plasma concentration of 51.9 mg/L 24 h after administration, with a C max of 538.8 mg/ L attained 1.5 h after administration.…”

Section: Bioavailability From Resveratrol Supplementsmentioning

confidence: 94%

“…The CV for C max was large, similar to that reported by Boocock et al, ranging from 40 to 113%. Although C max was not reported following initial dose, data from Brown et al [30] demonstrate that this occurs at higher dosages as well. Following 29 days of 5 g trans-resveratrol administration, Brown et al [30] found plasma C max to be 958.6 mg/L.…”

Section: Bioavailability From Resveratrol Supplementsmentioning

confidence: 95%

Resveratrol and health – A comprehensive review of human clinical trials

Smoliga

Baur

Hausenblas

2011

Molecular Nutrition Food Res

487

301

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In the past decade, the small polyphenol resveratrol has received widespread attention as either a potential therapy or as a preventive agent for numerous diseases. Studies using purified enzymes, cultured cells, and laboratory animals have suggested that resveratrol has anti-aging, anti-carcinogenic, anti-inflammatory, and anti-oxidant properties that might be relevant to chronic diseases and/or longevity in humans. Although the supporting research in laboratory models is quite substantial, only recently data has emerged to describe the effects of resveratrol supplementation on physiological responses in humans. The limited number of human clinical trials that are available has largely described various aspects of resveratrol's safety and bioavailability, reaching a consensus that it is generally well-tolerated, but have poor bioavailability. Very few published human studies have explored the ability of resveratrol to achieve the physiological benefits that have been observed in laboratory models, although many clinical trials have recently been initiated. This review aims to examine the current state of knowledge on the effects of resveratrol on humans and to utilize this information to develop further guidelines for the implementation of human clinical trials.

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Repeat Dose Study of the Cancer Chemopreventive Agent Resveratrol in Healthy Volunteers: Safety, Pharmacokinetics, and Effect on the Insulin-like Growth Factor Axis

Cited by 547 publications

References 32 publications

Endocytosis of Resveratrol via Lipid Rafts and Activation of Downstream Signaling Pathways in Cancer Cells

Endocytosis of Resveratrol via Lipid Rafts and Activation of Downstream Signaling Pathways in Cancer Cells

Piceatannol, Natural Polyphenolic Stilbene, Inhibits Adipogenesis via Modulation of Mitotic Clonal Expansion and Insulin Receptor-dependent Insulin Signaling in Early Phase of Differentiation

Resveratrol and health – A comprehensive review of human clinical trials

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