The role of the acidity of N-heteroaryl sulfonamides as inhibitors of bcl-2 family protein-protein interactions.

B. Barry Touré,Karen Miller-Moslin,Naeem Yusuff,Lawrence Blas Perez,Michael Dore,Carol Joud,Walter Michael,Lucian Dipietro,Simon van der Plas,Michael McEwan,Francois Lenoir,Madelene Y. Hoe,Rajesh Karki,Clayton Springer,John T. Sullivan,Kymberly Levine,Catherine Fiorilla,Xiaoling Xie,Raviraj Kulathila,Kara Herlihy,Dale Porter,Michael Scott Visser

The role of the acidity of N-heteroaryl sulfonamides as inhibitors of bcl-2 family protein-protein interactions.

2013

Overexpression of the antiapoptotic members of the Bcl-2 family of proteins is commonly associated with cancer cell survival and resistance to chemotherapeutics. Here, we describe the structure-based optimization of a series of N-heteroaryl sulfonamides that demonstrate potent mechanism-based cell death. The role of the acidic nature of the sulfonamide moiety as it relates to potency, solubility, and clearance is examined. This has led to the discovery of novel heterocyclic replacements for the acylsulfonamide core of ABT-737 and ABT-263.

Keywords:

Pharmacology
Cancer
Bcl-2 family
Biochemistry
Biology
Apoptosis Inhibitor
Moiety
Protein–protein interaction
Cancer cell
Programmed cell death
Apoptosis

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