Structure based development of novel specific inhibitors for cathepsin L and cathepsin S in vitro and in vivo.

نویسندگان

  • N Katunuma
  • E Murata
  • H Kakegawa
  • A Matsui
  • H Tsuzuki
  • H Tsuge
  • D Turk
  • V Turk
  • M Fukushima
  • Y Tada
  • T Asao
چکیده

Specific inhibitors for cathepsin L and cathepsin S have been developed with the help of computer-graphic modeling based on the stereo-structure. The common fragment, N-(L-trans-carbamoyloxyrane-2-carbonyl)-phenylalanine-dimethyla mide, is required for specific inhibition of cathepsin L. Seven novel inhibitors of the cathepsin L inhibitor Katunuma (CLIK) specifically inhibited cathepsin L at a concentration of 10(-7) M in vitro, while almost no inhibition of cathepsins B, C, S and K was observed. Four of the CLIKs are stable, and showed highly selective inhibition for hepatic cathepsin L in vivo. One of the CLIK inhibitors contains an aldehyde group, and specifically inhibits cathepsin S at 10(-7) M in vitro.

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عنوان ژورنال:
  • FEBS letters

دوره 458 1  شماره 

صفحات  -

تاریخ انتشار 1999