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(사)한국바이오칩학회 The Korean BioChip Society



BT+IT+NTThe Korean BioChip Society

BioChip Journal

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Info. Vol.6 - No.4 (2012.12.20)
Title Genomewide transcription profiles altered by BMI-1026 and Roscovitine and its implication in cellular senescence
Authors Ji-Hye Lee1, Changhee Min3,*, Sahng-June Kwak2 & Yeon-Sun Seong1
Institutions 1Department of Nanobiomedical Science, 2Department of Biochemistry College of Medicine, Dankook University, San 29, Anseo-Dong, Cheonan 330-714, Korea
3LG Life Sciences Ltd., R&D Park, 104-1 Munji-Dong, Yuseong-Gu, Daejeon 305-380, Korea
*Current affiliation: Hanall Biopharma Ltd., Central Research Institute, 533 Yongsan-Dong, Yuseong-Gu, Daejeon 305-500, Korea
Correspondence and requests for materials should be addressed to Y.S. Seong ( seongys@dankook.ac.kr) and S.J. Kwak ( ftpn2100@dankook.ac.kr)
Abstract Cyclin-dependent kinases (CDKs) are highly conserved over evolutionary path and function as master regulators of the cell division cycle. Thus CDK inhibitors have been focused in the drug development for cancer and other cell proliferative disorders. Among these inhibitors Roscovitine is well known compound and under clinical trial currently while far less has been reported on another CDK inhibitor - BMI-1026, designed as a drug candidate also targeting the cell cycle. In this study we tried to define biological effects and possible mechanisms of the two chemicals by analyzing the altered transcriptome profiles when BMI-1026 and Roscovitine are applied on WI-38 cells. Our result revealed both BMI-1026 and Roscovitine produced similar gene expression profiles, where E2F target genes were suppressed in common, including cyclin A, MCM3 and PCNA along with activated p53 pathway. This finding strongly indicates that molecular machineries responsible for other established senescence models are also employed in the changes in WI-38 cells induced by the two CDK inhibitors.
Keyword CDK inhibitor, BMI-1026, Roscovitine, E2F target genes, Senescence
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