Science. 1994 Jan 21;263(5145):380-4.

Rational design of potent, bioavailable, nonpeptide cyclic ureas as HIV protease inhibitors.

Lam PY, Jadhav PK, Eyermann CJ, Hodge CN, Ru Y, Bacheler LT, Meek JL, Otto MJ, Rayner MM, Wong YN, et al.

Department of Virology Research, DuPont Merck Pharmaceutical Company, Wilmington, DE 19880.

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.

PMID: 8278812 [PubMed - indexed for MEDLINE]

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Improved cyclic urea inhibitors of the HIV-1 protease: synthesis, potency, resistance profile, human pharmacokinetics and X-ray crystal structure of DMP 450.
Chem Biol. 1996 Apr; 3(4):301-14.

[Chem Biol. 1996]
Nonpeptide cyclic cyanoguanidines as HIV-1 protease inhibitors: synthesis, structure-activity relationships, and X-ray crystal structure studies.
J Med Chem. 1998 Apr 23; 41(9):1446-55.

[J Med Chem. 1998]
Cyclic HIV protease inhibitors: design and synthesis of orally bioavailable, pyrazole P2/P2' cyclic ureas with improved potency.
J Med Chem. 1998 Jun 4; 41(12):2019-28.

[J Med Chem. 1998]
ReviewDesign of symmetry-based, peptidomimetic inhibitors of human immunodeficiency virus protease.
Methods Enzymol. 1994; 241:334-54.

[Methods Enzymol. 1994]
ReviewDe novo design and discovery of cyclic HIV protease inhibitors capable of displacing the active-site structural water molecule.
Pharm Biotechnol. 1998; 11:257-84.

[Pharm Biotechnol. 1998]
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Cited by 36 PubMed Central articles

Structure of HIV-1 protease in complex with potent inhibitor KNI-272 determined by high-resolution X-ray and neutron crystallography.
Adachi M, Ohhara T, Kurihara K, Tamada T, Honjo E, Okazaki N, Arai S, Shoyama Y, Kimura K, Matsumura H, et al. Proc Natl Acad Sci U S A. 2009 Mar 24; 106(12):4641-6. Epub 2009 Mar 9.

[Proc Natl Acad Sci U S A. 2009]
Solution kinetics measurements suggest HIV-1 protease has two binding sites for darunavir and amprenavir.
Kovalevsky AY, Ghosh AK, Weber IT. J Med Chem. 2008 Oct 23; 51(20):6599-603. Epub 2008 Sep 20.

[J Med Chem. 2008]
Interaction of HIV-1 aspartic protease with its inhibitor, by molecular dynamics and ab initio fragment molecular orbital method.
Koyano K, Nakano T. J Synchrotron Radiat. 2008 May; 15(Pt 3):239-42. Epub 2008 Apr 18.

[J Synchrotron Radiat. 2008]
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Structures reported by this article

Rational Design Of Potent, Bioavailable, Nonpeptide Cyclic Ureas As Hiv Protease Inhibitors

PDB: 1HVR

Source: Human immunodeficiency virus 1

Method: X-Ray Diffraction | Resolution: 1.8 Å

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