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    1,2,5-Thiadiazolidin-3-one 1,1-dioxide-based heterocyclic sulfides are potent inhibitors of human tryptase

    Date
    2005-04-01
    Author
    Wong, Tzutshin
    Groutas, Christopher S.
    Mohan, Swathi
    Lai, Zhong
    Alliston, Kevin R.
    Vu, Nga T.
    Schechter, Norman M.
    Groutas, William C.
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    Citation
    Archives of biochemistry and biophysics. 2005 Apr 1; 436(1): 1-7.
    Abstract
    We describe herein the design, synthesis, and in vitro biochemical evaluation of a series of potent, time-dependent inhibitors of the mast cell-derived serine protease tryptase. The inhibitors were readily obtained by attaching various heterocyclic thiols, as well as a basic primary specificity residue P(1), to the 1,2,5-thiadiazolidin-3-one 1,1-dioxide scaffold. The inhibitors were found to be devoid of any inhibitory activity toward a neutral (elastase) or cysteine (papain) protease, however they were also fairly efficient inhibitors of bovine trypsin. The differential inhibition observed with trypsin suggests that enzyme selectivity can be optimized by exploiting differences in the S' subsites of the two enzymes. The results described herein demonstrate the versatility of the heterocyclic scaffold in fashioning mechanism-based inhibitors of neutral, basic, and acidic (chymo)trypsin-like serine proteases.
    Description
    Click on the DOI link below to access the article (may not be free).
    URI
    http://dx.doi.org/10.1016/j.abb.2005.01.022
    http://hdl.handle.net/10057/4260
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