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Yongzhuo Jiang

NanJing University
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  •  Publications
    7
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 More details
  • NanJing University
    Department of Philosophy
    Graduate student
Areas of Interest
Philosophy of Language
Philosophy of Mind
Philosophy of Cognitive Science
  • All publications (7)
  •  64
    Investigation of the microstructure and optical properties of hydrogenated polymorphous silicon films prepared with pure silane
    with S. B. Li, Z. M. Wu, W. Li, and N. M. Liao
    Philosophical Magazine 87 (35): 5539-5549. 2007.
  •  73
    Effects of gas temperature on optical and transport properties of a-Si:H films deposited by PECVD
    with N. -M. Liao, W. Li, Z. -M. Wu, K. -C. Qi, and S. -B. Li
    Philosophical Magazine 88 (25): 3051-3057. 2008.
  •  27
    Genetic ME–a visualization application for merging and editing pedigrees for genetic studies
    with D. K. Bui, X. Wei, M. C. Ortube, Y. P. de WeeksConley, and M. B. Gorin
  •  101
    Concurrent formation of two different type precipitation-free zones during the initial stage of homogenization
    with Y. Q. Chen, D. Q. Yi, B. Wang, and H. Q. Liu
    Philosophical Magazine 93 (18): 2269-2278. 2013.
    Freedom and Liberty
  •  120
    Atomic structure of the Fe/Fe3C interface with the Isaichev orientation in pearlite
    with Y. T. Zhou, S. J. Zheng, T. Z. Zhao, Y. J. Wang, and X. L. Ma
    Philosophical Magazine 1-12. forthcoming.
  •  18
    Effect of hydroxyurea on the promoter occupancy profiles of tumor suppressor p53 and p73
    with V. Huang, X. Lu, and J. Y. J. Wang
    Background: The p53 tumor suppressor and its related protein, p73, share a homologous DNA binding domain, and mouse genetics studies have suggested that they have overlapping as well as distinct biological functions. Both p53 and p73 are activated by genotoxic stress to regulate an array of cellular responses. Previous studies have suggested that p53 and p73 independently activate the cellular apoptotic program in response to cytotoxic drugs. The goal of this study was to compare the promoter-bi…Read more
    Background: The p53 tumor suppressor and its related protein, p73, share a homologous DNA binding domain, and mouse genetics studies have suggested that they have overlapping as well as distinct biological functions. Both p53 and p73 are activated by genotoxic stress to regulate an array of cellular responses. Previous studies have suggested that p53 and p73 independently activate the cellular apoptotic program in response to cytotoxic drugs. The goal of this study was to compare the promoter-binding activity of p53 and p73 at steady state and after genotoxic stress induced by hydroxyurea. Results: We employed chromatin immunoprecipitation, the NimbleGen promoter arrays and a model-based algorithm for promoter arrays to identify promoter sequences enriched in anti-p53 or anti-p73 immunoprecipitates, either before or after treatment with hydroxyurea, which increased the expression of both p53 and p73 in the human colon cancer cell line HCT116-3. We calculated a model-based algorithm for promoter array score for each promoter and found a significant correlation between the promoter occupancy profiles of p53 and p73. We also found that after hydroxyurea treatment, the p53-bound promoters were still bound by p73, but p73 became associated with additional promoters that that did not bind p53. In particular, we showed that hydroxyurea induces the binding of p73 but not p53 to the promoter of MLH3, which encodes a mismatch repair protein, and causes an up-regulation of the MLH3 mRNA. Conclusion: These results suggest that hydroxyurea exerts differential effects on the promoter-binding functions of p53 and p73 and illustrate the power of model-based algorithm for promoter array in the analyses of promoter occupancy profiles of highly homologous transcription factors. © 2009 Huang et al; licensee BioMed Central Ltd.
  • Visual short-term memory
    with M. C. Potter
    In Patrick Wilken, Timothy J. Bayne & Axel Cleeremans (eds.), The Oxford Companion to Consciousness, Oxford University Press. pp. 436--438. 2009.
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