Journal of Medicinal Chemistry 2006-10-19

New efficient substrates for semicarbazide-sensitive amine oxidase/VAP-1 enzyme: analysis by SARs and computational docking.

Francesc Yraola, Silvia García-Vicente, Juan Fernandez-Recio, Fernando Albericio, Antonio Zorzano, Luc Marti, Miriam Royo

文献索引:J. Med. Chem. 49 , 6197-208, (2006)

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摘要

Structure activity relationships for semicarbazide-sensitive amine oxidase/vascular adhesion protein-1 (SSAO/VAP-1) were studied using a library of arylalkylamine substrates, with the aim of contributing to the discovery of more efficient SSAO substrates. Experimental data were contrasted with computational docking studies, thereby allowing us to examine the mechanism and substrate-binding affinity of SSAO and thus contribute to the discovery of more efficient SSAO substrates and provide a structural basis for their interactions. We also built a model of the mouse SSAO structure, which provides several structural rationales for interspecies differences in SSAO substrate selectivity and reveals new trends in SSAO substrate recognition. In this context, we identified novel efficient substrates for human SSAO that can be used as a lead for the discovery of antidiabetic agents.


相关化合物

  • 氨甲苯酸
  • 间苯二甲胺
  • β-苯乙胺
  • 对氟苄胺
  • 1-(1-萘基)乙胺
  • 4-甲基苄胺
  • 3-苯基丙基胺
  • 3,4-二甲氧基苯乙胺
  • 1,4-苯二甲胺
  • 4-叔丁基苄胺

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