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      KCI등재 SCOPUS SCIE

      Alleviation of Senescence via ATM Inhibition in Accelerated Aging Models

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      https://www.riss.kr/link?id=A106096731

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      다국어 초록 (Multilingual Abstract)

      The maintenance of mitochondrial function is closely linked to the control of senescence. In our previous study, we uncovered a novel mechanism in which senescence amelioration in normal aging cells is mediated by the recovered mitochondrial function ...

      The maintenance of mitochondrial function is closely linked to the control of senescence. In our previous study, we uncovered a novel mechanism in which senescence amelioration in normal aging cells is mediated by the recovered mitochondrial function upon Ataxia telangiectasia mutated (ATM) inhibition. However, it remains elusive whether this mechanism is also applicable to senescence amelioration in accelerated aging cells. In this study, we examined the role of ATM inhibition on mitochondrial function in Hutchinson-Gilford progeria syndrome (HGPS) and Werner syndrome (WS) cells. We found that ATM inhibition induced mitochondrial functional recovery accompanied by metabolic reprogramming, which has been known to be a prerequisite for senescence alleviation in normal aging cells. Indeed, the induced mitochondrial metabolic reprogramming was coupled with senescence amelioration in accelerated aging cells. Furthermore, the therapeutic effect via ATM inhibition was observed in HGPS as evidenced by reduced progerin accumulation with concomitant decrease of abnormal nuclear morphology. Taken together, our data indicate that the mitochondrial functional recovery by ATM inhibition might represent a promising strategy to ameliorate the accelerated aging phenotypes and to treat agerelated disease.

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      참고문헌 (Reference)

      1 Gray, M. D., "The werner syndrome protein is a DNA helicase" 17 : 100-103, 1997

      2 Shiloh, Y., "The ATM-mediated DNA-damage response : taking shape" 31 : 402-410, 2006

      3 Collins, F. S., "Seeking a cure for one of the rarest diseases : progeria" 134 : 126-129, 2016

      4 Rottenberg, H., "Quantitative assay by flow cytometry of the mitochondrial membrane potential in intact cells" 1404 : 393-404, 1998

      5 Tohma, H., "Quantification of ceroid and lipofuscin in skeletal muscle" 59 : 769-779, 2011

      6 Debacq-Chainiaux, F., "Protocols to detect senescence-associated beta-galactosidase(SA-[beta]gal)activity, a biomarker of senescent cells in culture and in vivo" 4 : 1798-1806, 2009

      7 Lachapelle, S., "Proteome-wide identification of WRN-interacting proteins in untreated and nuclease-treated samples" 10 : 1216-1227, 2011

      8 Verstraeten, V. L. R. M., "Protein farnesylation inhibitors cause donut-shaped cell nuclei attributable to a centrosome separation defect" 108 : 4997-5002, 2011

      9 Shimizu, K., "Paraquat induces long-lasting dopamine overflow through the excitotoxic pathway in the striatum of freely moving rats" 976 : 243-252, 2003

      10 Kang, H. T., "Nicotinamide enhances mitochondria quality through autophagy activation in human cells" 8 : 426-438, 2009

      1 Gray, M. D., "The werner syndrome protein is a DNA helicase" 17 : 100-103, 1997

      2 Shiloh, Y., "The ATM-mediated DNA-damage response : taking shape" 31 : 402-410, 2006

      3 Collins, F. S., "Seeking a cure for one of the rarest diseases : progeria" 134 : 126-129, 2016

      4 Rottenberg, H., "Quantitative assay by flow cytometry of the mitochondrial membrane potential in intact cells" 1404 : 393-404, 1998

      5 Tohma, H., "Quantification of ceroid and lipofuscin in skeletal muscle" 59 : 769-779, 2011

      6 Debacq-Chainiaux, F., "Protocols to detect senescence-associated beta-galactosidase(SA-[beta]gal)activity, a biomarker of senescent cells in culture and in vivo" 4 : 1798-1806, 2009

      7 Lachapelle, S., "Proteome-wide identification of WRN-interacting proteins in untreated and nuclease-treated samples" 10 : 1216-1227, 2011

      8 Verstraeten, V. L. R. M., "Protein farnesylation inhibitors cause donut-shaped cell nuclei attributable to a centrosome separation defect" 108 : 4997-5002, 2011

      9 Shimizu, K., "Paraquat induces long-lasting dopamine overflow through the excitotoxic pathway in the striatum of freely moving rats" 976 : 243-252, 2003

      10 Kang, H. T., "Nicotinamide enhances mitochondria quality through autophagy activation in human cells" 8 : 426-438, 2009

      11 Skoczynska, A., "New look at the role of progerin in skin aging" 14 : 53-58, 2015

      12 Seo, A. Y., "New insights into the role of mitochondria in aging : mitochondrial dynamics and more" 123 : 2533-2542, 2010

      13 Reunert, J., "Neonatal progeria : increased ratio of progerin to lamin A leads to progeria of the newborn" 20 : 933-937, 2012

      14 Robbins, E., "Morphologic changes accompanying senescence of cultured human diploid cells" 131 : 1211-1222, 1970

      15 Passos, J. F., "Mitochondrial dysfunction accounts for the stochastic heterogeneity in telomere-dependent senescence" 5 : e110-, 2007

      16 Wallace, D. C., "Mitochondrial DNA sequence variation in human evolution and disease" 91 : 8739-8746, 1994

      17 Brunk, U. T., "Lipofuscin : mechanisms of agerelated accumulation and influence on cell function" 33 : 611-619, 2002

      18 Sahin, E., "Linking functional decline of telomeres, mitochondria and stem cells during ageing" 464 : 520-528, 2010

      19 Oshima, J., "Lack of WRN results in extensive deletion at nonhomologous joining ends" 62 : 547-551, 2002

      20 Mitsui, Y., "Increased nuclear sizes in senescent human diploid fibroblast cultures" 100 : 147-152, 1976

      21 Lee, H. C., "Increase in mitochondrial mass in human fibroblasts under oxidative stress and during replicative cell senescence" 9 : 517-526, 2002

      22 Collins, T. J., "ImageJ for microscopy" 43 : 25-30, 2007

      23 Rivera-Torres, J., "Identification of mitochondrial dysfunction in Hutchinson–Gilford progeria syndrome through use of stable isotope labeling with amino acids in cell culture" 91 : 466-477, 2013

      24 McClintock, D., "Hutchinson–Gilford progeria mutant lamin A primarily targets human vascular cells as detected by an anti-Lamin A G608G antibody" 103 : 2154-2159, 2006

      25 McKenzie, R., "Hepatic failure and lactic acidosis due to fialuridine(FIAU), an investigational nucleoside analogue for chronic hepatitis B" 333 : 1099-1105, 1995

      26 Li, B., "Downregulation of the werner syndrome protein induces a metabolic shift that compromises redox homeostasis and limits proliferation of cancer cells" 13 : 367-378, 2014

      27 Drechsel, D. A., "Differential contribution of the mitochondrial respiratory chain complexes to reactive oxygen species production by redox cycling agents implicated in parkinsonism" 112 : 427-434, 2009

      28 Pekovic, V., "Conserved cysteine residues in the mammalian lamin A tail are essential for cellular responses to ROS generation" 10 : 1067-1079, 2011

      29 Cocheme, H. M., "Complex I is the major site of mitochondrial superoxide production by paraquat" 283 : 1786-1798, 2008

      30 Azqueta, A., "Comet assay to measure DNA repair : approach and applications" 5 : 288-, 2014

      31 Benhammou, V., "Clinical mitochondrial dysfunction in uninfected children born to HIV-infected mothers following perinatal exposure to nucleoside analogues" 48 : 173-178, 2007

      32 Kang, H. T., "Chemical screening identifies ATM as a target for alleviating senescence" 13 : 616-623, 2017

      33 Shiloh, Y., "Ataxia-telangiectasia(A-T) : An emerging dimension of premature ageing" 33 : 76-88, 2016

      34 Brand, Martin D., "Assessing mitochondrial dysfunction in cells" 435 : 297-312, 2011

      35 Harhouri, K., "An overview of treatment strategies for Hutchinson-Gilford Progeria syndrome" 9 : 246-257, 2018

      36 Weber, A. M., "ATM and ATR as therapeutic targets in cancer" 149 : 124-138, 2015

      37 Dimri, G. P., "A biomarker that identifies senescent human cells in culture and in aging skin in vivo" 92 : 9363-9367, 1995

      38 유승민, "A Molecular Approach to Mitophagy and Mitochondrial Dynamics" 한국분자세포생물학회 41 (41): 18-26, 2018

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      연월일 이력구분 이력상세 등재구분
      2023 평가예정 해외DB학술지평가 신청대상 (해외등재 학술지 평가)
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      2008-01-01 평가 SCI 등재 (등재유지) KCI등재
      2006-01-01 평가 등재학술지 유지 (등재유지) KCI등재
      2004-01-01 평가 등재학술지 유지 (등재유지) KCI등재
      2001-01-01 평가 등재학술지 선정 (등재후보2차) KCI등재
      1998-07-01 평가 등재후보학술지 선정 (신규평가) KCI등재후보
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      기준연도 WOS-KCI 통합IF(2년) KCIF(2년) KCIF(3년)
      2016 2.77 0.19 1.85
      KCIF(4년) KCIF(5년) 중심성지수(3년) 즉시성지수
      1.37 1.11 0.379 0.03
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