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      염증성 창자질환에서의 유전자 손상복구 반응 = DNA Repair Response in the Inflammatory Bowel disease

      한글로보기

      https://www.riss.kr/link?id=T11583932

      • 저자
      • 발행사항

        광주 : 조선대학교 대학원, 2008

      • 학위논문사항

        학위논문(박사) -- 조선대학교 대학원 , 의학과 , 2008

      • 발행연도

        2008

      • 작성언어

        한국어

      • DDC

        616.344 판사항(21)

      • 발행국(도시)

        광주

      • 형태사항

        33 p : 채색삽화 ; 26cm.

      • 일반주기명

        DNA Repair Response in the Inflammatory Bowel disease
        지도교수:장인엽
        참고문헌 : 24-28 p.

      • 소장기관
        • 국립중앙도서관 국립중앙도서관 우편복사 서비스
        • 조선대학교 도서관 소장기관정보
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      다국어 초록 (Multilingual Abstract) kakao i 다국어 번역

      Oxidative stress is an imbalance condition between production of reactive oxygen species (ROS) and diminished antioxidant defense systems. Oxidative stress develops chiefly in the processing ofinflammations since the inflammatory cells create enormous volume of ROS for the purpose of protection from many noxious assaults. It has been extensively identified extensively that oxidative stress in inflammatory tissue can head for malignant growth. Moreover oxidative stress acts as a chief pathogenetic factor for cancer development from inflammatory diseases, such as chronic inflammatory bowel disease (IBD)-related colorectal cancer. The levels of oxidized bases in the DNA molecule are a result of the balance between the amount of oxidative DNA damage and repair. Thereforewe analyzed the changes of colonic mucosal DNA repair proteins of the dextran sulfate sodium(DSS)-induced IBD. In this experiment, we studied the DSS- induced colonic mucosal changesof morphological localization and protein expression for DNA base mismatch repair(MMR) proteins, MSH2, MSH6; DNA base damage marker and base excision repair(BER) protein, 8-oxo-7,8-dihydro-2,-deoxyguanosine (8OHdG), Ref1, OGG1; DNA double strands breaks(DSB) marker and its repair(BER) protein, -H2AX, DNAPKCs, Ku70, Ku80. The patterns of DNA repair proteins expression were protein-specific with time-course. While the DNA repair proteins that show increased expression were Ref-1, OGG1, DNAPKCs and MSH2, but Ku80 was decreased. The proteins changed level of expression may be the target molecule in the pathogenesis and protection of IBD, but additional study are needed to be confirmed.
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      Oxidative stress is an imbalance condition between production of reactive oxygen species (ROS) and diminished antioxidant defense systems. Oxidative stress develops chiefly in the processing ofinflammations since the inflammatory cells create enormous...

      Oxidative stress is an imbalance condition between production of reactive oxygen species (ROS) and diminished antioxidant defense systems. Oxidative stress develops chiefly in the processing ofinflammations since the inflammatory cells create enormous volume of ROS for the purpose of protection from many noxious assaults. It has been extensively identified extensively that oxidative stress in inflammatory tissue can head for malignant growth. Moreover oxidative stress acts as a chief pathogenetic factor for cancer development from inflammatory diseases, such as chronic inflammatory bowel disease (IBD)-related colorectal cancer. The levels of oxidized bases in the DNA molecule are a result of the balance between the amount of oxidative DNA damage and repair. Thereforewe analyzed the changes of colonic mucosal DNA repair proteins of the dextran sulfate sodium(DSS)-induced IBD. In this experiment, we studied the DSS- induced colonic mucosal changesof morphological localization and protein expression for DNA base mismatch repair(MMR) proteins, MSH2, MSH6; DNA base damage marker and base excision repair(BER) protein, 8-oxo-7,8-dihydro-2,-deoxyguanosine (8OHdG), Ref1, OGG1; DNA double strands breaks(DSB) marker and its repair(BER) protein, -H2AX, DNAPKCs, Ku70, Ku80. The patterns of DNA repair proteins expression were protein-specific with time-course. While the DNA repair proteins that show increased expression were Ref-1, OGG1, DNAPKCs and MSH2, but Ku80 was decreased. The proteins changed level of expression may be the target molecule in the pathogenesis and protection of IBD, but additional study are needed to be confirmed.

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      목차 (Table of Contents)

      • 영문초록 = 1
      • 서론 = 3
      • 재료 및 방법 = 8
      • 결과 = 11
      • 고찰 = 14
      • 영문초록 = 1
      • 서론 = 3
      • 재료 및 방법 = 8
      • 결과 = 11
      • 고찰 = 14
      • 결론 = 24
      • 참고문헌 = 25
      • 사진부도설명 = 31
      • 사진부도 = 32
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