Potential protease inhibitors based on a functionalized cyclic sulfamide scaffold

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Authors
Zhong, Jiaying
Gan, Xiangdong
Alliston, Kevin R.
Lai, Zhong
Yu, Hongyi
Groutas, Christopher S.
Wong, Tzutshin
Groutas, William C.
Advisors
Issue Date
2004-07-01
Type
Article
Keywords
Research Support, Non-U.S. Gov't , Research Support, U.S. Gov't, P.H.S.
Research Projects
Organizational Units
Journal Issue
Citation
Journal of combinatorial chemistry. 2004 Jul-Aug; 6(4): 556-63.
Abstract

Exploratory studies related to the design and synthesis of functionalized cyclic sulfamides (I) as potential inhibitors of proteolytic enzymes were carried out. The structural motif and three diversity sites embodied in the scaffold render it amenable to combinatorial parallel synthesis and the facile generation of lead discovery prospecting libraries. The scaffold was readily assembled starting with (DL) serine methyl ester, and a series of compounds was generated and screened against human leukocyte elastase. Modification of the P(1) recognition element, believed to be accommodated at the primary specificity site (S(1) subsite) of the enzyme, yielded compounds that inhibited the enzyme by an apparent hyperbolic partial mixed-type inhibition.

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Publisher
American Chemical Society
Journal
Book Title
Series
Journal of combinatorial chemistry
J Comb Chem
PubMed ID
DOI
ISSN
1520-4766
EISSN