the evaluation and comparison of transcriptionally targeted noxa and puma killer genes to initiate apoptosis under cancer-specific promoter cxcr1 in hepatocarcinoma gene therapy

نویسندگان

shahryar khoshtinat nikkhoi department of medical biotechnology, faculty of medical sciences, tarbiat modares university, tehran, ir iran; baqiyatallah research center for gastroenterology and liver diseases, baqiyatallah university of medical sciences, tehran, ir iran

hedieh heydarzadeh department of microbiology, faculty of science, azad university of shahreh qods, tehran, ir iran

saeed ranjbar department of medical biotechnology, faculty of medical sciences, tarbiat modares university, tehran, ir iran

fatemeh salimi department of medical biotechnology, faculty of medical sciences, tarbiat modares university, tehran, ir iran

چکیده

methods the current study generated two recombinant lentiviruses, plex-gcn and plex-gcp, bearing noxa and puma, respectively. transduction of both genes to hepatocarcinoma (hepg2) was verified using fluorescent microscopic analysis, western blotting, and quantitative real-time polymerase chain reaction (pcr). to evaluate the potential of noxa and puma to initiate apoptosis, a caspase-9 real-time, mtt assay, and a 4’, 6-diamidino-2-phenylindole (dapi) reagent were performed to stain apoptotic cells. conclusions in this approach, the suicide gene was transferred to transformed cells and ignited apoptosis to exterminate them. puma is a more potent killer gene and has higher capabilities to start intrinsic apoptosis pathway. results the data verified successful transduction to hepg2 and hek293t. higher relative expression of noxa and puma rather than the untransduced cell line showed these genes are expressed more in hepg2 in comparison to hek293t. the results of the real-time pcr, mtt assay, and dapi reagent illustrated that higher cells initiated apoptosis following puma transduction rather than noxa. objectives this study evaluated the potential of inducing apoptosis using noxa and puma in a hepatocarcinoma cell line. background cancerous cells proliferate as fast as possible without a proper surveillance system. this rapid cell division leads to enormous mutation rates, which help a tumor establish.

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The Evaluation and Comparison of Transcriptionally Targeted Noxa and Puma Killer Genes to Initiate Apoptosis Under Cancer-Specific Promoter CXCR1 in Hepatocarcinoma Gene Therapy

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عنوان ژورنال:
hepatitis monthly

جلد ۱۶، شماره ۱۰، صفحات ۰-۰

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