4.7 Article

Inhibition of Human Melanoma Growth by a Non-Cardioselective β-Blocker

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JOURNAL OF INVESTIGATIVE DERMATOLOGY
卷 135, 期 2, 页码 525-531

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ELSEVIER SCIENCE INC
DOI: 10.1038/jid.2014.373

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  1. Ligue Genevoise Contre le Cancer
  2. foundation Francis et Marie-France Minkoff

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Recently, retrospective studies provided conflicting results on the benefit of beta-adrenoceptor-blockers (beta-blockers) on melanoma progression. Most of these studies did not define the beta-blocker used, making it difficult to understand the source of discrepancies between results. Therefore, we investigated the effect of non-cardioselective and cardioselective beta-blockers on melanoma progression at the cellular, molecular, and tumor levels. Here we show that the non-cardioselective beta-blocker propranolol hydrochloride (propranolol) inhibits proliferation and induces apoptosis in primary cell cultures derived from a primary and a metastasis of human melanoma and in melanoma cell lines. In contrast, the cardioselective beta-blocker metoprolol tartrate hardly affects melanoma cell survival or proliferation. We further highlight that a daily treatment with propranolol slows down tumor development in immunodeficient mice transplanted with human melanoma cells. RNA microarrays, quantitative PCR, and histochemistry analyses showed that propranolol regulates the expression of different genes involved in tumor angiogenesis, cell death, or proliferation. Thus, our results suggest that non-cardioselective beta-blockers affect melanoma progression, and bring first clues about the pathways involved in this antitumor effect.

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