Candidate Genes and Mechanisms for 2-Methoxyestradiol–Mediated Vasoprotection

Barchiesi, Federica; Lucchinetti, Eliana; Zaugg, Michael; Ogunshola, Omolara O.; Wright, Matthew B.; Meyer, Markus; Rosselli, Marinella; Schaufelberger, Sara; Gillespie, Delbert G.; Jackson, Edwin K.; Dubey, Raghvendra K.

doi:10.1161/hypertensionaha.110.152298

Cited by 29 publications

(24 citation statements)

References 30 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Our previous studies using microarray analysis showed that 2-ME modulates multiple mechanisms that can affect tissue factor expression. Specifically, 2-ME induces COX2 expression, activates PPAR␣ and -␥, inhibits 3-hydroxyl-3-methylglutaryl coenzyme A (HMG-CoA), blocks squalene epoxidase and mevalonate (diphospho) decarboxylase (which convert mevalonic acid to isopentenyl-PP and squalene), and inhibits NF-B and phosphatidylinositol 3-kinase (6,7,23). Moreover, 2-ME inhibits MAPK, a known activator of tissue factor (21).…”

Section: Discussionmentioning

confidence: 99%

“…Taken together, these observations indicate that RhoA acts as a microtubuledependent signal in cytokinesis. It is known that 2-ME disrupts tubulin polymerization (4), and our previous microarray experiment shows a downregulation by 2-ME of genes necessary for mitotic spindle assembly (6). Thus, it is conceivable that 2-ME inhibits the activation of the RhoA/ROCK1 pathway via its microtubule disrupting action and thereby blocks cytokinesis (Fig.…”

mentioning

confidence: 87%

See 1 more Smart Citation

2-Methoxyestradiol blocks the RhoA/ROCK1 pathway in human aortic smooth muscle cells

Rigassi

Bozzolo

Lucchinetti

et al. 2015

American Journal of Physiology-Endocrinology and Metabolism

Self Cite

View full text Add to dashboard Cite

-2-Methoxyestradiol (2-ME), a metabolite of estradiol with little affinity for estrogen receptors, inhibits proliferation of vascular smooth muscle cells; however, the molecular mechanisms underlying this effect are incompletely understood. Our previous work shows that 2-ME inhibits initiation (blocks phosphorylation of ERK and Akt) and progression (reduces cyclin expression and increases expression of cyclin inhibitors) of the mitogenic pathway and interferes with mitosis (disrupts tubulin organization). Because the RhoA/ROCK1 pathway (RhoA ¡ ROCK1 ¡ myosin phosphatase targeting subunit ¡ myosin light chain) is involved in cytokinesis, herein we tested the concept that 2-ME also blocks the RhoA/ROCK1 pathway. Because of the potential importance of 2-ME for preventing/treating vascular diseases, experiments were conducted in female human aortic vascular smooth muscle cells. Microarray transcriptional profiling suggested an effect of 2-ME on the RhoA/ROCK1 pathway. Indeed, 2-ME blocked mitogen-induced GTP-bound RhoABC expression and membrane-bound RhoA, suggesting interference with the activation of RhoA. 2-ME also reduced ROCK1 expression, suggesting reduced production of the primary downstream signaling kinase of the RhoA pathway. Moreover, 2-ME inhibited RhoA/ROCK1 pathway downstream signaling, including phosphorylated myosin phosphatase targeting subunit and myosin light chain; the ROCK1 inhibitor H-1152 mimicked these effects of 2-ME; both 2-ME and H-1152 blocked cytokinesis. 2-ME also reduced the expression of tissue factor, yet another downstream signaling component of the RhoA/ROCK1 pathway. We conclude that 2-ME inhibits the pathway RhoA ¡ ROCK1 ¡ myosin phosphatase targeting subunit ¡ myosin light chain, and this likely contributes to the reduced cytokinesis in 2-ME treated HASMCs.2-methoxyestradiol; RhoA; ROCK1; myosin phosphatase targeting subunit; myosin light chain; cytokinesis 2-METHOXYESTRADIOL (2-ME) is an endogenous metabolite of estradiol that attenuates vascular smooth muscle cell (VSMC) proliferation, migration, and extracellular matrix synthesis (5,8,9) and reduces injury-induced neointima formation (4), cholesterol-induced atherosclerosis (9), monocrotaline-induced vascular thickening in pulmonary hypertension (9), and injuryinduced glomerosclerosis (9). Although 2-ME inhibits VSMC proliferation and is thus effective against multiple proliferative disorders (4, 9, 10), the mechanisms via which 2-ME mediates these actions remain incompletely understood.Our previously published work shows that in human aortic vascular smooth muscle cells (HASMCs) 2-ME inhibits cell proliferation in part by blocking initiation of the mitogenic pathway (4). Specifically, 2-ME inhibits phosphorylation of both ERK1/2 and Akt (Fig. 1), which turns off the mitogenic pathway by decreasing the expression and activity of cyclins. Indeed, we (4) found that 2-ME 1) blocks cell-cycle progression in both G0/G1 and in G2/M phases, 2) reduces cyclin D1 and cyclin B1 expression, 3) inhibits Cdk-1 and Cdk-2 activity, 4) reduc...

show abstract

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 87%

2-Methoxyestradiol blocks the RhoA/ROCK1 pathway in human aortic smooth muscle cells

Rigassi

Bozzolo

Lucchinetti

et al. 2015

American Journal of Physiology-Endocrinology and Metabolism

Self Cite

View full text Add to dashboard Cite

show abstract

“…Rosiglitazone used to treat type II diabetes also was suspended by the EMEA and restricted by the United States Federal Drug Administration because of increased cardiovascular risk (Hancox 2011). Rosiglitazone acts through peroxisome proliferator-activated receptor g (PPAR g), a receptor which is also modulated by metabolites of estrogen (Barchiesi et al 2010). Rosiglitazone may also inhibit estrogen synthesis in ovarian tissue which could indirectly as well as directly affect bone resorption (Harslof et al 2011;Seto-Young et al 2011).…”

Section: Discussionmentioning

confidence: 99%

Considerations of Sex and Gender Differences in Preclinical and Clinical Trials

Raz

Miller

2012

Sex and Gender Differences in Pharmacology

View full text Add to dashboard Cite

Women continue to be underrepresented in clinical trials, particularly in Phases I and II of experimental drug studies in spite of legislative guidelines in the USA, Canada, the European Union, Australia, and Japan requiring the inclusion of women in clinical trials. As such, women remain a vulnerable population subject to the adverse effects of pharmacological therapies. Thus, women experience higher rates of adverse drug reactions than do men and for women of reproductive age or who may be pregnant, therapeutic options may be limited. This chapter provides a brief history of inclusion of sex and gender as variables in clinical trials, summarizes governmental legislation for consideration of sex and gender in clinical trials and provides specific examples of drugs which have been withdrawn from the market because of side effects in women. Additional information related to sex and gender in preclinical testing, trial design, challenges to recruitment of women for clinical trials and statistical methods for analysis of data also is considered.

show abstract

“…We mainly use peripheral blood samples [45] in human and vascular smooth muscle cell (VSMC) [46,47] , adrenal [44] , heart [2,48,49] and kidney [2,44,[53][54][55][56]58] in animal models.…”

Section: Samplesmentioning

confidence: 99%

Differential Gene Expression Profile in Essential Hypertension

Yang¹

2012

Genetics and Pathophysiology of Essential Hypertension

View full text Add to dashboard Cite

Candidate Genes and Mechanisms for 2-Methoxyestradiol–Mediated Vasoprotection

Cited by 29 publications

References 30 publications

2-Methoxyestradiol blocks the RhoA/ROCK1 pathway in human aortic smooth muscle cells

2-Methoxyestradiol blocks the RhoA/ROCK1 pathway in human aortic smooth muscle cells

Considerations of Sex and Gender Differences in Preclinical and Clinical Trials

Differential Gene Expression Profile in Essential Hypertension

Contact Info

Product

Resources

About