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    58 research outputs found

    Bisphenol A at Low Nanomolar Doses Confers Chemoresistance in Estrogen Receptor-α–Positive and –Negative Breast Cancer Cells

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    National Institute of Environmental Health Sciences
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    PubMed Central

    Bisphenol A at Environmentally Relevant Doses Inhibits Adiponectin Release from Human Adipose Tissue Explants and Adipocytes

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    National Institute of Environmental Health Sciences
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    PubMed Central

    Selective Estrogen Receptor Down-Regulator and Selective Estrogen Receptor Modulators Differentially Regulate Lactotroph Proliferation

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    Public Library of Science
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    occupation, differentially modulates the biological outcome of anti-estrogens. expression and release, as well as ERE-mediated transcriptional activity. expression
    Public Library of Science (PLOS)
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    PubMed Central

    Dopamine receptor type 1 (D1R) in breast cancer: Expression, signaling and therapeutic applications

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    'OMICS Publishing Group'
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    Characterization of the Gonadotrophins Releasing Factors of the Rat and the Pig

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    155 p.Thesis (Ph.D.)--University of Illinois at Urbana-Champaign, 1972.U of I OnlyRestricted to the U of I community idenfinitely during batch ingest of legacy ETD
    Illinois Digital Environment for Access to Learning and Scholarship Repository

    Effects of bisphenol A on adipokine release from human adipose tissue: Implications for the metabolic syndrome

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    'Elsevier BV'
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    Activation of the cGMP/protein kinase G system in breast cancer by the dopamine receptor-1

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    'OAE Publishing Inc.'
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    Despite recent advances in the detection and treatment of breast cancer, many shortcomings remain, providing incentives to search for new therapeutic targets. This review provides information on the expression and actions of dopamine receptor-1 (D1R) in breast cancer. D1R is overexpressed in a significant number of primary breast tumors, characterized by having an aggressive phenotype and predicting a shorter survival time for patients. Activation of D1R in breast cancer cells by selective agonists caused suppression of cell viability, stimulation of apoptosis, inhibition of cell invasion, and an increase in chemosensitivity. Instead of being linked to the cAMP/PKA system as expected, D1R in breast cancer is linked to the activation of the cGMP/protein kinase G (PKG) pathway. Fenoldopam, a peripheral D1R agonist that does not penetrate the brain, dramatically suppressed the growth of breast cancer xenografts in immune-deficient mice. A new imaging system for detecting D1R-expressing tumors and metastases was also developed. The review offers a novel concept that D1R can serve as a biomarker for prognosis in advanced breast cancer and its agonists can be used as effective and personalized therapeutics in a subpopulation of patients with D1R-expressing breast tumors. Several drugs, some of which are FDA-approved, that bypass the D1R and directly activate the cGMP/PKG apoptotic system, are also identified
    OAE Publishing (via Crossref)
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