Evento
The antitumoral effects of HO-1 in colorectal cancer are dependent on the presence of a wild type p53
Alonso, Eliana Noelia
; Gandini, Norberto Ariel
; Ferronato, María Julia
; Fermento, María Eugenia
; Marquestaut, Mariquena Natali; Andrés, Nancy Carolina
; Abba, Martín Carlos
; Massillo, Cintia Lorena
; Curino, Alejandro Carlos
; Facchinetti, Maria Marta
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Tipo del evento:
Congreso
Nombre del evento:
LXI Reunión Científica Anual de la Sociedad Argentina de Investigación Clínica; LXIV Reunión Anual De La Sociedad Argentina De Inmunología; XLVIII Reunión Anual De La Sociedad Argentina De Farmacología Experimental; VII Reunión Anual De La Sociedad Argentina De Nanomedicina; V Congreso Nacional De La Asociación Argentina De Ciencia Y Tecnología De Animales De Laboratorio
Fecha del evento:
15/11/2016
Institución Organizadora:
Sociedad Argentina De Investigación Clínica;
Sociedad Argentina De Inmunología;
Asociación Argentina de Farmacología Experimental,;
Sociedad Argentina De Nanomedicina;
Asociación Argentina De Ciencia Y Tecnología De Animales De Laboratorio;
Título de la revista:
Medicina (Buenos Aires)
Editorial:
Fundación Revista Medicina
ISSN:
0025-7680
e-ISSN:
1669-9106
Idioma:
Inglés
Clasificación temática:
Resumen
Previously, we reported that heme oxygenase-1 (HO-1) is associated with increased overall survival time of patients with invasive colorectal cancer (CRC) and that HO-1 activation de- creases the viability of human CRC cell lines that carry a wild- type p53 although it has no effect on cells with absent/mutated p53. The hypothesis of this work is that p53 might be involved in the antitumoral effect of HO-1 in CRC. By using a xenograft of p53 wild type-containing HCT116, we first demonstrated that genetic overexpression of HO-1 delayed tumor growth (p<0.05) and decreased tumor volume and weight (p<0.01) compared to controls. Also, p53 was upregulated in HO-1-overexpressing cells (p<0.05). We then evaluated the effects of pharmacologic activa- tion of HO-1 (hemin) in HCT116 p53wt or HCT116 p53-/- xenograft tumors. Hemin (H) treatment delayed tumor growth (p<0.01) and decreased tumor volume (H=740.6 vs C=3082 mm3; p<0.01) and weight (H=0.8 vs C=3.2 g; p<0.05) only in HCT116 p53wt tumors, although it increased HO-1 levels in both tumor types (p<0.01). In support of these results, in silico studies showed a trend towards higher overall survival in CRC patients with high HO-1 and p53wt compared to those with low HO-1 or mutated p53. To start investigating p53 regulation by HO-1, we performed HO-1 chromatin immunoprecipitation assays and found that HO-1 does not bind to p53 promoter. In addition to affecting cell viabil- ity, genetic and pharmacological modulation of HO-1 decreased cell migration (p<0.05) and invasion (p<0.001) only in HCT116 cells, not affecting these processes in HCT116 p53-/- cells. These effects were accompanied by E-cadherin upregulation (p<0.05). In concordance, preliminary results obtained in human CRC biopsies by immunohistochemistry, showed a positive cor- relation between HO-1 and E-cadherin (p<0.01). In conclusion, our data demonstrate an antitumoral role for HO-1 in CRC and show evidence of the importance of a wild type p53 for this role
Palabras clave:
HEMEOXIGENASE-1
,
COLORECTAL CANCER
,
ANTITUMORAL
,
P53
Archivos asociados
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Eventos(IBYME)
Eventos de INST.DE BIOLOGIA Y MEDICINA EXPERIMENTAL (I)
Eventos de INST.DE BIOLOGIA Y MEDICINA EXPERIMENTAL (I)
Eventos(INIBIBB)
Eventos de INST.DE INVEST.BIOQUIMICAS BAHIA BLANCA (I)
Eventos de INST.DE INVEST.BIOQUIMICAS BAHIA BLANCA (I)
Eventos(INQUISUR)
Eventos de INST.DE QUIMICA DEL SUR
Eventos de INST.DE QUIMICA DEL SUR
Citación
The antitumoral effects of HO-1 in colorectal cancer are dependent on the presence of a wild type p53; LXI Reunión Científica Anual de la Sociedad Argentina de Investigación Clínica; LXIV Reunión Anual De La Sociedad Argentina De Inmunología; XLVIII Reunión Anual De La Sociedad Argentina De Farmacología Experimental; VII Reunión Anual De La Sociedad Argentina De Nanomedicina; V Congreso Nacional De La Asociación Argentina De Ciencia Y Tecnología De Animales De Laboratorio; Mar del Plata; Argentina; 2016; 307-307
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