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Liporetro-D-peptides - a novel class of highly selective thrombin inhibitors
Authors:Poyarkov Alexey A  Poyarkova Svetlana A  Smirnova Irina V  Kukhar Valery P
Affiliation:
  • a Institute of Bioorganic Chemistry and Petrochemistry of the Ukrainian National Academy of Sciences, 1, Murmanska St, Kyiv 94, 02660 Ukraine
  • b Department of Physical Therapy and Rehabilitation Science, University of Kansas Medical Center, 3901 Rainbow Blvd, Kansas City KS, 66160 USA
  • Abstract:

    Introduction

    Plasma serine protease thrombin plays a key role in coagulation, haemostasis and thromboembolic diseases. Direct thrombin inhibitors could be beneficial for future anticoagulant therapy. We have synthesized and studied liporetro-D-peptides - efficient thrombin inhibitors resistant to enzymatic degradation.

    Materials and Methods

    Compounds X-D-Arg-D-Phe-OMe, where X = residue of lauric or myristic acid or 9-fluorenylmethoxycarbonyl, have been synthesized by conventional peptide synthesis in solution and their comparative inhibitory analysis in relation to thrombin, factor X, plasmin and trypsin has been conducted.

    Results

    Modification of the synthetic liporetro-D-peptides with the myristic acid residue was the most successful one. This modification has dramatically increased the inhibition efficacy (Ki = 0,17 μM) and selectivity toward the chosen target enzyme, thrombin, in comparison to factor X, plasmin and trypsin (more than 600, 900, and 5000-fold, respectively).

    Conclusions

    Our findings establish an important role of the fatty moiety in the structure of peptide inhibitors with regards to their potency and selectivity toward thrombin.
    Keywords:DCC, N N'dicyclohexylcarbodiimide   DMF, dimethyl formamide   DMSO, dimethyl sulfoxide   HRMS, high resolution mass spectra   LDI, laser desorption ionization   PEG, polyethylene glycol   TAFI, thrombin activatable fibrinolysis inhibitor   TLC, thin layer chromatography
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