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MCF-7 세포주의 γ선에 의한 DNA 손상 반응 유전자 발현 양상의 분석
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  • MCF-7 세포주의 γ선에 의한 DNA 손상 반응 유전자 발현 양상의 분석
  • A DNA-Damage Response Gene Expression Analysis in MCF-7 followed by γ-Radiation
저자명
박지윤,황창일,박웅양,김진규,채영규,Park. Ji-Yoon,Hwang. Chang-Il,Park. Woong-Yang,Kim. Jin-Kyu,Chai. Young Gyu
간행물명
환경생물
권/호정보
2005년|23권 1호|pp.21-26 (6 pages)
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한국환경생물학회
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이 논문은 한국과학기술정보연구원과 논문 연계를 통해 무료로 제공되는 원문입니다.
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기타언어초록

Cell response to genotoxic agents is complex and involves the participation of different classes of genes including cell cycle control, DNA repair and apoptosis. In this report, we presented a approach to characterize the cellular functions associated with the altered transcript profiles of MCF-7 exposed to low-dose in vitro gamma-irradiation. We used the method of human 2.4 k cDNA microarrays containing apoptosis, cell cycle, chromatin, repair, stress and chromosome genes to analyze the differential gene expression characterization that were displayed by radiation-exposed cell, human breast carcinoma MCF-7 cell line, such as 4 Gy 4 hr, 8 Gy 4 hr, and 8 Gy 12 hr. Among these genes, 66 were up-regulated and 49 were down-regulated. Specific genes were concomitantly induced in the results. Cyclin dependent kinase 4 (Cdk4) is induced for starting the cell cycle. This regulation is required for a DNA damage­induced G1 arrest. In addition to, an apoptotic pathways gene Bcl-w was concomitantly induced. Mismatch repair protein homologue-l (hMLH1), a necessary component of DNA mismatch protein repair (MMR), in G2-M cell cycle checkpoint arrest. The present study provides new information on the molecular mechanism underlying the cell response to genotoxic stress, with relevance to basic and clinical research.