Methods of Analysis for Chemicals that Promote/Disrupt Cellular Signaling.

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  • UMEZAWA Yoshio
    Department of Chemistry, School of Science, The University of Tokyo
  • OZAWA Takeaki
    Department of Chemistry, School of Science, The University of Tokyo
  • SATO Moritoshi
    Department of Chemistry, School of Science, The University of Tokyo

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Methods of analysis were presented for chemicals that promote or disrupt cellular signaling pathways. The developed analytical methods are based not only on receptor binding, but also on the following known molecular-level processes involved in signal transduction along signaling pathways, reconstituted in vitro or taken in part in living cells. The methods were discussed in relation to receptor binding assay and/or bioassay. Examples include: (1) Insulin signaling pathways; (1-i) Chemical selectivity of agonists for insulin signaling pathways based on agonist-induced phosphorylation of a target peptide; (1-ii) An SPR-based screening method for agonist selectivity for insulin signaling pathways based on the binding of phosphotyrosine to its specific binding protein; (1-iii) A fluorescent indicator for tyrosine phosphorylation-based insulin signaling pathways; (2) An optical method for evaluating ion selectivity for calcium signaling pathways in the cell; (3) Assay and screening of chemicals that disrupt cellular signaling pathways, potential endocrine disruptors in particular; (4) Protein conformational changes, and (5) A screening method for antigen-specific IgE using mast cells, based on intracellular calcium signaling.

収録刊行物

  • Analytical Sciences

    Analytical Sciences 18 (5), 503-516, 2002

    社団法人 日本分析化学会

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