J. Büttner scite author profile

In AIDS therapy, attempts have been made to inhibit the virus-encoded enzymes, e.g. HIV-1 protease, using active site-directed inhibitors. This approach is questionable, however, due to virus mutations and the high toxicity of the drugs. An alternative method to inhibit the dimeric HIV protease is the targeting of the interface region of the protease subunits in order to prevent subunit dimerization and enzyme activity. This approach should be less prone to inactivation by mutation. A list of improved 'dimerization inhibitors' of HIV-1 protease is presented. The main structural features are a short 'interface' peptide segment, including non-natural amino acids, and an aliphatic N-terminal blocking group. The high inhibitory power of some of the lipopeptides [e.g. palmitoyl-Tyr-Glu-Leu-OH, palmitoyl-Tyr-Glu-(L-thyronine)-OH, palmitoyl-Tyr-Glu-(L-biphenyl-alanine)-OH] with low nanomolar K i values in the enzyme test suggests that mimetics with good bio-availability can be derived for AIDS therapy.

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Inhibition of HIV-1 Replication by Peptidic Protease Inhibitors

Petry¹,

Ast²,

Rosny³

et al. 2000

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Screening of Inhibitors of HIV-1 Protease Using anEscherichia coliCell Assay

Büttner

Dornmair²,

Schramm

1997

Biochemical and Biophysical Research Communications

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J. Büttner

The inhibition of human immunodeficiency virus proteases by ‘interface peptides’

Lipopeptides as Dimerization Inhibitors of HIV-1 Protease

Inhibition of HIV-1 Replication by Peptidic Protease Inhibitors

Screening of Inhibitors of HIV-1 Protease Using anEscherichia coliCell Assay

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