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beta-Adrenergic modulation of cancer cell proliferation: available evidence and clinical perspectives

Title
beta-Adrenergic modulation of cancer cell proliferation: available evidence and clinical perspectives
Type
Another Publication in an International Scientific Journal
Year
2017
Authors
Coelho, M
(Author)
Other
The person does not belong to the institution. The person does not belong to the institution. The person does not belong to the institution. Without AUTHENTICUS Without ORCID
Soares Silva, C
(Author)
Other
The person does not belong to the institution. The person does not belong to the institution. The person does not belong to the institution. Without AUTHENTICUS Without ORCID
Brandao, D
(Author)
Other
The person does not belong to the institution. The person does not belong to the institution. The person does not belong to the institution. Without AUTHENTICUS Without ORCID
Marino, F
(Author)
Other
The person does not belong to the institution. The person does not belong to the institution. The person does not belong to the institution. Without AUTHENTICUS Without ORCID
Cosentino, M
(Author)
Other
The person does not belong to the institution. The person does not belong to the institution. The person does not belong to the institution. Without AUTHENTICUS Without ORCID
Journal
Vol. 143
Pages: 275-291
ISSN: 0171-5216
Publisher: Springer Nature
Other information
Authenticus ID: P-00M-4J2
Abstract (EN): In this review, we aimed to present and discuss the available preclinical and epidemiological evidences regarding the modulation of cancer cell proliferation by beta-adrenoceptors (beta-AR), with a specific focus on the putative effects of beta-blockers according to their pharmacological properties. A comprehensive review of the published literature was conducted, and the evidences concerning the involvement of beta-AR in cancer as well as the possible role of beta-blockers were selected and discussed. The majority of reviewed studies show that: (1) All the cancer types express both beta 1- and beta 2-AR, with the exception of neuroblastoma only seeming to express beta 2-AR; (2) adrenergic agonists are able to increase proliferation of several types of cancers; (3) the proliferative effect seems to be mediated by both beta 1- and beta 2-AR; (4) binding to beta-AR results in a cAMP transient flux which activates two major downstream effector systems: protein kinase A and EPAC and (5) beta-blockers might be putative adjuvants for cancer treatment. Overall, the reviewed studies show strong evidences that beta-AR activation, through several intracellular mechanisms, modulate tumor cell proliferation suggesting beta-blockers can be a feasible therapeutic approach to antagonize beta-adrenergic response or have a protective effect per se. This review highlight the need for intensifying the research not only on the molecular mechanisms underlying the beta-adrenergic influence in cancer, but also on the implications of biased agonism of beta-blockers as potential antitumor agents.
Language: English
Type (Professor's evaluation): Scientific
No. of pages: 17
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