Discovery and characterization of the potent, selective and orally bioavailable MMP inhibitor ABT-770

Michael L Curtin,Alan S. Florjancic,H. Robin Heyman,Michael R. Michaelides,Robert B. Garland,James H. Holms,Douglas H. Steinman,Joseph F. Dellaria,Jane Gong,Carol K. Wada,Yan Guo,Ildiko B. Elmore,Paul Tapang,Daniel H. Albert,Terrance J. Magoc,Patrick A. Marcotte,Jennifer J. Bouska,Carole L. Goodfellow,Joy Bauch,Kennan C. Marsh,Douglas W. Morgan,Steven K. Davidsen

Discovery and characterization of the potent, selective and orally bioavailable MMP inhibitor ABT-770

2001

Modification of the biphenyl portion of MMP inhibitor 2a gave analogue 2i which is greater than 1000-fold selective against MMP-2 versus MMP-1. The stereospecific synthesis of both enantiomers of 2i was achieved beginning with (S)- or (R)-benzyl glycidyl ether. The (S)-enantiomer, 11 (ABT-770), is orally bioavailable and efficacious in an in vivo model of tumor growth.

Keywords:

Enzyme
Matrix metalloproteinase
Hydroxamic acid
Organic chemistry
Bioavailability
Biochemistry
Chemistry
Enzyme inhibitor
Chemical synthesis
Biological activity
Oral administration
In vivo
Stereochemistry
Pharmacokinetics

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