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Bioorganic and Medicinal Chemistry Letters 2015-Feb

Structure-based design and optimization of potent inhibitors of the adenoviral protease.

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Philipp Grosche
Finton Sirockin
Aengus Mac Sweeney
Paul Ramage
Paul Erbel
Samu Melkko
Anna Bernardi
Nicola Hughes
David Ellis
Keith D Combrink

Ključne riječi

Sažetak

Adenoviral infections are associated with a wide range of acute diseases, among which ocular viral conjunctivitis (EKC) and disseminated disease in immunocompromised patients. To date, no approved specific anti-adenoviral drug is available, but there is a growing need for an effective treatment of such infections. The adenoviral protease, adenain, plays a crucial role for the viral lifecycle and thus represents an attractive therapeutic target. Structure-guided design with the objective to depeptidize tetrapeptide nitrile 1 led to the novel chemotype 2. Optimization of scaffold 2 resulted in picomolar adenain inhibitors 3a and 3b. In addition, a complementary series of irreversible vinyl sulfone containing inhibitors were rationally designed, prepared and evaluated against adenoviral protease. High resolution X-ray co-crystal structures of representatives of each series proves the successful design of these inhibitors and provides an excellent basis for future medicinal chemistry optimization of these compounds.

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