Melatonin decreases breast cancer metastasis by modulating Rho‐associated kinase protein‐1 expression

Author:

Borin Thaiz Ferraz1,Arbab Ali Syed2,Gelaleti Gabriela Bottaro13,Ferreira Lívia Carvalho13,Moschetta Marina Gobbe1,Jardim‐Perassi Bruna Victorasso1,Iskander ASM2,Varma Nadimpalli Ravi S.4,Shankar Adarsh2,Coimbra Verena Benedick1,Fabri Vanessa Alves1,de Oliveira Juliana Garcia5,Zuccari Debora Aparecida Pires de Campos13

Affiliation:

1. Laboratory of Molecular Investigation of Cancer – LIMC Department of Molecular Biology Faculdade de Medicina de Sao Jose do Rio Preto – FAMERP Sao Jose do Rio Preto SP Brazil

2. Tumor angiogenesis laboratory Cancer Center Georgia Regents University Augusta GA USA

3. Universidade Estadual Paulista Julio de Mesquita Filho – IBILCE/UNESP Sao Jose do Rio Preto SP Brazil

4. Cellular and Molecular Imaging Laboratory Department of Radiology Henry Ford Hospital Detroit MI USA

5. Universidade do Sagrado Coração (USC) Pro‐Reitoria de Pesquisa e Pos‐Graduação Bauru SP Brazil

Abstract

AbstractThe occurrence of metastasis, an important breast cancer prognostic factor, depends on cell migration/invasion mechanisms, which can be controlled by regulatory and effector molecules such as Rho‐associated kinase protein (ROCK‐1). Increased expression of this protein promotes tumor growth and metastasis, which can be restricted by ROCK‐1 inhibitors. Melatonin has shown oncostatic, antimetastatic, and anti‐angiogenic effects and can modulate ROCK‐1 expression. Metastatic and nonmetastatic breast cancer cell lines were treated with melatonin as well as with specific ROCK‐1 inhibitor (Y27632). Cell viability, cell migration/invasion, and ROCK‐1 gene expression and protein expression were determined in vitro. In vivo lung metastasis study was performed using female athymic nude mice treated with either melatonin or Y27832 for 2 and 5 wk. The metastases were evaluated by X‐ray computed tomography and single photon emission computed tomography (SPECT) and by immunohistochemistry for ROCK‐1 and cytokeratin proteins. Melatonin and Y27632 treatments reduced cell viability and invasion/migration of both cell lines and decreased ROCK‐1 gene expression in metastatic cells and protein expression in nonmetastatic cell line. The numbers of ‘hot’ spots (lung metastasis) identified by SPECT images were significantly lower in treated groups. ROCK‐1 protein expression also was decreased in metastatic foci of treated groups. Melatonin has shown to be effective in controlling metastatic breast cancer in vitro and in vivo, not only via inhibition of the proliferation of tumor cells but also through direct antagonism of metastatic mechanism of cells rendered by ROCK‐1 inhibition. When Y27632 was used, the effects were similar to those found with melatonin treatment.

Funder

Fundacao de Amparo a Pesquisa do Estado de Sao Paulo - FAPESP

Fundacao de Apoio a Pesquisa e Extensao de Sao Jose do Rio Preto - FAPERP

Publisher

Wiley

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