Hepatitis Monthly. 2011; 11 (4): 255-262
en Inglés
| IMEMR
| ID: emr-131139
ABSTRACT
Core protein of the hepatitis C virus [HCV] has an important role in HCV self-replication, pathogenesis and carcinogenesis. To identify the effect of core proteins from different quasispecies of HCV genotype 1b expressed in a HepG2 cell line on human gene expression profiles. Core protein eukrocytic expression plasmids [pEGFP-N1] containing different quasispecie core protein genes of genotypes 1b HCV derived from of HCV-related hepatocellular carcinoma [HCC] tumoral tissue [T] and non-tumoral tissue [NT] were constructed and then transfected to HepG2 cell line. The gene expressions spectrum in the cell expression core proteins from T and NT were compared with those in the control by Affymetrix human genome HG-U 133 plus 2.0 microarray. Different gene expression profiles were acquired between HepG2 expressing core proteins derived from T and NT tissues. Both core proteins caused the modulation of several genes that are up/down-regulated as compared to control, including genes involved in oncogenesis, signal transduction, cell apoptosis, and cell growth cycle regulation. Surprisingly, only one gene-CNSK1A1- was up-regulated by both T and NT core variants. Core proteins isolated from tumoral or non-tumoral nodules mediate expression of different cellular genes suggesting that variants isolated from different quasispecies may have different biological effects
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Índice:
IMEMR (Mediterraneo Oriental)
Asunto principal:
Expresión Génica
/
Hepatitis C
/
Carcinoma Hepatocelular
/
Genotipo
/
Neoplasias Hepáticas
Límite:
Humanos
Idioma:
Inglés
Revista:
Hepat. Monthly
Año:
2011
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