Identification and Optimization of Novel Small c-Abl Kinase Activators Using Fragment and HTS Methodologies | Zendy

Graham L. Simpson | Zendy; Sophie M. Bertrand | Zendy; Alan D. Borthwick | Zendy; Nino Campobasso | Zendy; Julien Chabanet | Zendy; Susan Chen | Zendy; Julia Coggins | Zendy; Josh Cottom | Zendy; Siegfried B. Christensen | Zendy; Helen C. Dawson | Zendy; Helen L. Evans | Zendy; Andrew N. Hobbs | Zendy; Xuan Hong | Zendy; Biju Mangatt | Zendy; J. A. Muñoz | Zendy; Allen Oliff | Zendy; Donghui Qin | Zendy; Paul ScottStevens | Zendy; Paris Ward | Zendy; Yoshiaki Washio | Zendy; Jingsong Yang | Zendy; Robert J. Young | Zendy

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Identification and Optimization of Novel Small c-Abl Kinase Activators Using Fragment and HTS Methodologies

Author(s) -

Graham L. Simpson,

Sophie M. Bertrand,

Alan D. Borthwick,

Nino Campobasso,

Julien Chabanet,

Susan Chen,

Julia Coggins,

Josh Cottom,

Siegfried B. Christensen,

Helen C. Dawson,

Helen L. Evans,

Andrew N. Hobbs,

Xuan Hong,

Biju Mangatt,

J. A. Muñoz,

Allen Oliff,

Donghui Qin,

Paul ScottStevens,

Paris Ward,

Yoshiaki Washio,

Jingsong Yang,

Robert J. Young

Publication year - 2019

Publication title -

journal of medicinal chemistry

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.01

H-Index - 261

eISSN - 1520-4804

pISSN - 0022-2623

DOI - 10.1021/acs.jmedchem.8b01872

Subject(s) - chemistry , tyrosine kinase , abl , small molecule , kinase , microbiology and biotechnology , biochemistry , signal transduction , biology

Abelson kinase (c-Abl) is a ubiquitously expressed, nonreceptor tyrosine kinase which plays a key role in cell differentiation and survival. It was hypothesized that transient activation of c-Abl kinase via displacement of the N-terminal autoinhibitory "myristoyl latch", may lead to an increased hematopoietic stem cell differentiation. This would increase the numbers of circulating neutrophils and so be an effective treatment for chemotherapy-induced neutropenia. This paper describes the discovery and optimization of a thiazole series of novel small molecule c-Abl activators, initially identified by a high throughput screening. Subsequently, a scaffold-hop, which exploited the improved physicochemical properties of a dihydropyrazole analogue, identified through fragment screening, delivered potent, soluble, cell-active c-Abl activators, which demonstrated the intracellular activation of c-Abl in vivo.

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