Artículo
Carnosic acid inhibits the proliferation and migration capacity of human colorectal cancer cells
Barni, María Verónica
; Carlini, María José
; Cafferata, Eduardo Gustavo Alfredo
; Puricelli, Lydia Ines
; Moreno, Silvia





Fecha de publicación:
04/2012
Editorial:
Spandidos Publications
Revista:
Oncology Reports
ISSN:
1021-335X
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
Colorectal cancer (CRC) is the third most common malignant neoplasm worldwide. The objective of this study was to examine whether carnosic acid (CA), the main antioxidant compound of Rosmarinus officinalis L., would inhibit the cell viability of three CRC cell lines: Caco-2, HT29 and LoVo in a dose-dependent manner, with IC50 values in the range of 24-96 µM. CA induced cell death by apoptosis in Caco-2 line after 24 h of treatment and inhibited cell adhesion and migration, possibly by reducing the activity of secreted proteases such as urokinase plasminogen activator (uPA) and metalloproteinases (MMPs). These effects may be associated through a mechanism involving the inhibition of the COX-2 pathway, because we have determined that CA downregulates the expression of COX-2 in Caco-2 cells at both the mRNA and protein levels. Therefore, CA modulates different targets involved in the development of CRC. These findings indicate that carnosic acid may have anticancer activity and may be useful as a novel chemotherapeutic agent.
Palabras clave:
Colorectal cancer
,
Carnosic acid
,
COX-2
,
Chemotherapeutic agent
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Articulos(IIBBA)
Articulos de INST.DE INVEST.BIOQUIMICAS DE BS.AS(I)
Articulos de INST.DE INVEST.BIOQUIMICAS DE BS.AS(I)
Articulos(OCA HOUSSAY)
Articulos de OFICINA DE COORDINACION ADMINISTRATIVA HOUSSAY
Articulos de OFICINA DE COORDINACION ADMINISTRATIVA HOUSSAY
Citación
Barni, María Verónica; Carlini, María José; Cafferata, Eduardo Gustavo Alfredo; Puricelli, Lydia Ines; Moreno, Silvia; Carnosic acid inhibits the proliferation and migration capacity of human colorectal cancer cells; Spandidos Publications; Oncology Reports; 27; 4; 4-2012; 1041-1048
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