Small molecule inhibitors of Apaf-1-related caspase-3/-9 activation that control mitochondrial-dependent apoptosis

Author:

Malet, G.

Martin, A. G.

Orzaez, M.

Vicent, M. J.

Masip, I.

Sanclimens, G.

Ferrer-Montiel, A.

Mingarro, I.

Messeguer, A.

O Fearnhead, H.

Perez-Paya, E.
Author Address

Ctr Invest Principe Felipe, Dept Med Chem, E-46013 Valencia, Spain. Univ Valencia, Dept Biochem & Mol Biol, E-46100 Burjassot, Valencia, Spain. NCI, NIH, Apoptosis Sect, Regulat Cell Growth Lab, Frederick, MD 21702 USA. IIQAB, CSIC, Dept Biol Organ Chem, E-08034 Barcelona, Spain. Univ Miguel Hernandez, Inst Biol Mol & Celular, Elx Alacant 03202, Spain. CSIC, E-46013 Valencia, Spain.;Perez-Paya, E, Ctr Invest Principe Felipe, Dept Med Chem, Avda Autopista Saler,16, E-46013 Valencia, Spain.;eperez@ochoa.fib.es

Abstract:

Apoptosis is a biological process relevant to human disease states that is strongly regulated through protein-protein complex formation. These complexes represent interesting points of chemical intervention for the development of molecules that could modulate cellular apoptosis. The apoptosome is a holoenzyme multiprotein complex formed by cytochrome c-activated Apaf-1 (apoptotic protease-activating factor), dATP and procaspase- 9 that link mitochondria disfunction with activation of the effector caspases and in turn is of interest for the development of apoptotic modulators. In the present study we describe the identification of compounds that inhibit the apoptosome-mediated activation of procaspase-9 from the screening of a diversity-oriented chemical library. The active compounds rescued from the library were chemically optimised to obtain molecules that bind to both recombinant and human endogenous Apaf-1 in a cytochrome c-noncompetitive mechanism that inhibits the recruitment of procaspase- 9 by the apoptosome. These newly identified Apaf-1 ligands decrease the apoptotic phenotype in mitochondrial-mediated models of cellular apoptosis.

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