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The acute lymphoblastic leukemia prognostic scoring whether it is possible by BCL-2, BAX gene promoter genotyping

Authors :
Moazami-Goudarzi, M.
Majid Farshdousti Hagh
Hoseinpour-Feizi, A.
Talebi, M.
Movassaghpour-Akbari, A. A.
Shams-Asanjan, K.
Eyvazi-Ziyaee, J.
Seifi, M.
Source :
Caspian Journal of Internal Medicine, Vol 7, Iss 2, Pp 105-113 (2016), Caspian Journal of Internal Medicine, Scopus-Elsevier, Europe PubMed Central
Publication Year :
2016
Publisher :
Babol University of Medical Sciences, 2016.

Abstract

Background: BCL-2 is the most important anti-apoptotic regulator and Bax is a pro-apoptotic protein. The status of these parameters or the ration of BCL-2 to BAX is important in malignant cell fate as well as normal cells. Methods: Sixty-two ALL patients and 62 healthy sex-and age-matched controls were studied. After genotyping, the promoter region of the BAX and BCL-2 genes by RFLP-PCR method the patients were classified in nine prognostic groups, after that, the overall survival ratio of each score was compared with others pair-wise or between groups. Results: The frequencies of the AA, AC, CC alleles of the BCL-2 C-938A polymorphism in patient group were 33 (53.23%), 18 (29.03%), 11 (17.74%), and in the control group were 13 (21.0%), 27 (43.5%), 22 (35.5%), respectively (P=0.003). Also, the frequencies of AA, AG, GG alleles of the BAX G-248A SNP were 15 (24.2%), 24 (38.7%), 23 (37.1%) in ALL group and 13 (21.0%), 25 (40.3%), 24 (38.7%) (p>0.05) in the control group. The survival time estimation and ratio were significantly different between different SNPs in BCL-2 (P=0.002). Conclusion: These findings showed that the BCL-2 promoter region polymorphism is more reliable than BAX gene promoter polymorphism in any ALL scoring system. But the establishment of complete scoring system requires further more clinical and laboratory findings along with genetic polymorphisms is necessary

Details

Language :
English
ISSN :
20086172 and 20086164
Volume :
7
Issue :
2
Database :
OpenAIRE
Journal :
Caspian Journal of Internal Medicine
Accession number :
edsair.pmid.dedup....830984aa14887aacc5bca306fdf04e8e