1. Selenoprotein K deficiency inhibits melanoma by reducing calcium flux required for tumor growth and metastasis
- Author
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Natalija Glibetic, Pietro Bertino, Michael P. Marciel, Katie Lee, Vedbar S. Khadka, FuKun W. Hoffmann, Suzie Chen, Michelle L. Matter, Andrew Pham, Youping Deng, Peter R. Hoffmann, and Pascal Kilicaslan
- Subjects
0301 basic medicine ,Genetically modified mouse ,Cell growth ,Chemistry ,Melanoma ,medicine.disease ,migration ,Metastasis ,Calcineurin ,03 medical and health sciences ,030104 developmental biology ,Oncology ,Cancer stem cell ,inositol 1,4,5-triphosphate receptor ,Calcium flux ,medicine ,Cancer research ,calcium channel ,palmitoylation ,Receptor ,selenium ,Research Paper - Abstract
Interest has emerged in the therapeutic potential of inhibiting store operated calcium (Ca2+) entry (SOCE) for melanoma and other cancers because malignant cells exhibit a strong dependence on Ca2+ flux for disease progression. We investigated the effects of deleting Selenoprotein K (SELENOK) in melanoma since previous work in immune cells showed SELENOK was required for efficient Ca2+ flux through the endoplasmic reticulum Ca2+ channel protein, inositol 1,4,5-trisphosphate receptor (IP3R), which is due to the role SELENOK plays in palmitoylating and stabilizing the expression of IP3R. CRISPR/Cas9 was used to generate SELENOK-deficiency in human melanoma cells and this led to reduced Ca2+ flux and impaired IP3R function, which inhibited cell proliferation, invasion, and migration. Ca2+-dependent signaling through calcineurin was inhibited with SELENOK-deficiency, and gene array analyses together with evaluation of transcript and protein levels showed altered transcriptional programs that ultimately disrupted stemness and pro-growth properties. In vivo investigations were conducted using the Grm1-Tg transgenic mouse strain that develops spontaneous metastatic melanoma, which was crossed with SELENOK-/- mice to generate the following littermates: Grm1-Tg/SELENOK-/-, Grm1-Tg/SELENOK-/+, Grm1-Tg/SELENOK+/+. SELENOK-deficiency in Grm1-Tg/SELENOK-/- male and female mice inhibited primary tumor growth on tails and ears and reduced metastasis to draining lymph nodes down to levels equivalent to non-tumor control mice. Cancer stem cell pools were also decreased in Grm1-Tg/SELENOK-/- mice compared to littermates. These results suggest that melanoma requires SELENOK expression for IP3R dependent maintenance of stemness, tumor growth and metastasic potential, thus revealing a new potential therapeutic target for treating melanoma and possibly other cancers.
- Published
- 2018