Abstract: University of Cantabria— Breast Cancer Therapy Based on Melatonin.

Avoid the Risks of Light-induced Suppression of Nocturnal Melatonin. Recent Pat Endocr Metab Immune Drug Discov. 2012 May 1;6(2):108-16.

Breast cancer therapy based on melatonin. Sanchez-Barcelo EJ, Mediavilla MD, Alonso-Gonzalez C, Rueda N. Source Department of Physiology and Pharmacology, School of Medicine, University of Cantabria, 39011 Santander, Spain. [email protected]. Abstract The usefulness of melatonin and melatoninergic drugs in breast cancer therapy is based on its Selective Estrogen Receptor Modulator (SERM) and Selective Estrogen Enzyme Modulator (SEEM) properties. Because of the oncostatic properties of melatonin, its nocturnal suppression by light-at-night (LAN) has been considered a risk-factor for breast cancer. Melatonin’s SERM actions include modulation of estrogen-regulated cell proliferation, invasiveness and expression of proteins, growth factors and proto-oncogenes (hTERT, p53, p21, TGFâ, E-cadherin, etc.). These actions are observable with physiologic doses of melatonin only in cells expressing ERá, and mediated by MT1 melatonin receptors. Melatonin acts like a SEEM, inhibiting expression and activity of P450 aromatase, estrogen sulfatase and type 1, 17â- hydroxysteroid dehydrogenase, but stimulating that of estrogen sulfotransferase. This double action mechanism (SERM and SEEM), and the specificity for ERá bestows melatonin with potential advantages for breast cancer treatments, associated with other antiestrogenic drugs, and idea already patented. LAN enhances the growth of rat mammary tumors by decreasing or suppressing melatonin production. Epidemiologic studies have also described increased breast cancer risk in women exposed to LAN. Since the strongest suppression of nocturnal melatonin occurs with wavelength light of the blue spectral region, optical and lightening devices filtering the blue light spectrum have been proposed to avoid the risks of light-induced suppression of nocturnal melatonin. PMID: 22369716

https://www.ncbi.nlm.nih.gov/pubmed/22369716