Patrick Y.S. Lam scite author profile

Mechanistic information and structure-based design methods have been used to design a series of nonpeptide cyclic ureas that are potent inhibitors of human immunodeficiency virus (HIV) protease and HIV replication. A fundamental feature of these inhibitors is the cyclic urea carbonyl oxygen that mimics the hydrogen-bonding features of a key structural water molecule. The success of the design in both displacing and mimicking the structural water molecule was confirmed by x-ray crystallographic studies. Highly selective, preorganized inhibitors with relatively low molecular weight and high oral bioavailability were synthesized.

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New aryl/heteroaryl CN bond cross-coupling reactions via arylboronic acid/cupric acetate arylation

Lam

Clark

Saubern

et al. 1998

Tetrahedron Letters

1,022

475

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Patrick Y.S. Lam

Rational Design of Potent, Bioavailable, Nonpeptide Cyclic Ureas as HIV Protease Inhibitors

New aryl/heteroaryl CN bond cross-coupling reactions via arylboronic acid/cupric acetate arylation

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