The Transgene Expression of the Immature Form of the HCV Core Protein (C191) and the LncRNA MEG3 Increases Apoptosis in HepG2 Cells.
Dina MofedSalwa SabetAhmed A BaiomyTamer Z SalemPublished in: Current issues in molecular biology (2022)
Long non-coding RNAs (lncRNAs) are regulated in cancer cells, including lncRNA MEG3, which is downregulated in Hepatocellular Carcinoma (HCC). In addition, hepatitis C virus (HCV) core proteins are known to dysregulate important cellular pathways that are linked to HCC development. In this study, we were interested in evaluating the overexpression of lncRNA MEG3, either alone or in combination with two forms of HCV core protein (C173 and C191) in HepG2 cells. Cell viability was assessed by MTT assay. Transcripts' levels of key genes known to be regulated in HCC, such as p53 , DNMT1 , miRNA152, TGF-b , and BCL-2, were measured by qRT-PCR. Protein expression levels of caspase-3 and MKI67 were determined by immunocytochemistry and apoptosis assays. The co-expression of lncRNA MEG3 and C191 resulted in a marked increase and accumulation of dead cells and a reduction in cell viability. In addition, a marked increase in the expression of tumor suppressor genes ( p53 and miRNA152), as well as a marked decrease in the expression of oncogenes ( DNMT1 , BCL2, and TGF-b ), were detected. Moreover, apoptosis assay results revealed a significant increase in total apoptosis (early and late). Finally, immunocytochemistry results detected a significant increase in apoptotic marker caspase-3 and a decrease in tumor marker MKI67. In this study, transgene expression of C191 and lncRNA MEG3 showed induction in apoptosis in HepG2 cells greater than the expression of each one alone. These results suggest potential anticancer characteristics.
Keyphrases
- poor prognosis
- long non coding rna
- hepatitis c virus
- cell cycle arrest
- cell death
- endoplasmic reticulum stress
- oxidative stress
- induced apoptosis
- binding protein
- high throughput
- dna methylation
- transcription factor
- gene expression
- small molecule
- cell proliferation
- transforming growth factor
- epithelial mesenchymal transition
- genome wide identification