Down-regulation of SLC8A1 as a putative apoptosis evasion mechanism by modulation of calcium levels in penile carcinoma

Munoz, Juan J.; Drigo, Sandra A.; Barros-Filho, Mateus C.; Marchi, Fabio A.; Scapulatempo-Neto, Cristovam; Pessoa, Gustavo S.; Guimaraes, Gustavo C.; Trindade Filho, Jose Carlos S.; Lopes, Ademar; Arruda, Marco A. Z.; Rogatto, Silvia Regina

Utilize este identificador para citar ou criar um link para este item: http://acervodigital.unesp.br/handle/11449/128599

Título:

Down-regulation of SLC8A1 as a putative apoptosis evasion mechanism by modulation of calcium levels in penile carcinoma

Autor(es):

Instituição:

A.C.Camargo Cancer Center
Hospital de Câncer de Barretos
Universidade Estadual Paulista (UNESP)
Universidade Estadual de Campinas (UNICAMP)

ISSN:

0022-5347

Financiador:

National Council of Technological and Scientific Development
Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

Número do financiamento:

FAPESP: 2009/52088-3
FAPESP: 2010/51601-6
FAPESP: 2012/21344-7

Resumo:

Purpose: The SLC8A1 gene, which encodes the Na+/Ca2(+) exchanger, has a key role in calcium homeostasis. Our previous gene expression oligoarray data revealed SLC8A1 under expression in penile carcinoma. We investigated whether dysregulation of SLC8A1 expression is associated with apoptosis and cell proliferation in penile carcinoma via modulation of the calcium concentration. The underlying mechanisms of SLC8A1 under expression were also explored, focusing on copy number alteration and miRNA.Materials and Methods: Transcript levels of the SLC8A1 gene and miR-223 were evaluated by quantitative polymerase chain reaction to compare penile carcinoma samples with normal glans tissue. SLC8A1 copy number was evaluated by microarray based comparative genomic hybridization. In normal and tumor samples we investigated caspase-3 and Ki-67 immunostaining as well as calcium distribution by laser ablation imaging inductively coupled plasma mass spectrometry.Results: SLC8A1 under expression was detected in penile carcinoma samples (p = 0.001), confirming our previous data. It was not associated with gene copy number loss. In contrast, miR-223 over expression (p = 0.002) inversely correlated with its putative repressor SLC8A1 (r = -0.426, p = 0.015). SLC8A1 under expression was associated with decreased calcium distribution, high Ki-67 and low caspase-3 immunoexpression in penile carcinoma compared to normal tissue.Conclusions: Down-regulation of the SLC8A1 gene, most likely mediated by its regulator miR-223, can lead to decreased calcium in penile carcinoma and consequently to suppressed apoptosis and increased tumor cell proliferation. These data suggest that the miR-223-NCX1-calcium signaling axis may represent a potential therapeutic approach to penile carcinoma.

Data de publicação:

1-Jul-2015

Citação:

Journal Of Urology, v. 194, n. 1, p. 245-251, 2015.

Duração:

245-251

Publicador:

Elsevier B.V.

Palavras-chaves:

Penis
Carcinoma
Sodium-calcium exchanger 1
Calcium
MIRN223 microRNA
Human

Fonte:

http://www.sciencedirect.com/science/article/pii/S0022534714050381

Endereço permanente:

Direitos de acesso:

Acesso aberto

Tipo:

outro

Fonte completa:

http://repositorio.unesp.br/handle/11449/128599

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