Fragment-based lead discovery of indazole-based compounds as AXL kinase inhibitors.

Ng, Pearly Shuyi; Foo, Klement; Sim, Sandra; Wang, Gang; Huang, Chuhui; Tan, Li Hong; Poulsen, Anders; Liu, Boping; Tee, Doris Hui Ying; Ahmad, Nur Huda Binte; Wang, Sifang; Ke, Zhiyuan; Lee, May Ann; Kwek, Zekui P; Joy, Joma; Anantharajan, Jothi; Baburajendran, Nithya; Pendharkar, Vishal; Manoharan, Vithya; Vuddagiri, Susmitha; Sangthongpitag, Kanda; Hill, Jeffrey; Keller, Thomas H; Hung, Alvin W

Ng, Pearly Shuyi; Foo, Klement; Sim, Sandra; Wang, Gang; Huang, Chuhui; Tan, Li Hong; Poulsen, Anders; Liu, Boping; Tee, Doris Hui Ying; Ahmad, Nur Huda Binte; Wang, Sifang; Ke, Zhiyuan; Lee, May Ann; Kwek, Zekui P; Joy, Joma; Anantharajan, Jothi; Baburajendran, Nithya; Pendharkar, Vishal; Manoharan, Vithya; Vuddagiri, Susmitha; Sangthongpitag, Kanda; Hill, Jeffrey; Keller, Thomas H; Hung, Alvin W.

Afiliação

Ng PS; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore. Electronic address: pearly.ng.shuyi@gmail.com.
Foo K; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Sim S; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Wang G; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Huang C; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Tan LH; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Poulsen A; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Liu B; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Tee DHY; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Ahmad NHB; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Wang S; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Ke Z; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Lee MA; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Kwek ZP; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Joy J; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Anantharajan J; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Baburajendran N; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Pendharkar V; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Manoharan V; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Vuddagiri S; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Sangthongpitag K; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Hill J; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Keller TH; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore.
Hung AW; Experimental Drug Development Centre, 10 Biopolis Road #05-01 Chromos, 138670, Singapore. Electronic address: alvin@ligaturetx.com.

Bioorg Med Chem ; 49: 116437, 2021 11 01.

Article em En | MEDLINE | ID: mdl-34600239

ABSTRACT

ABSTRACT

AXL is a member of the TAM (TYRO3, AXL, MER) subfamily of receptor tyrosine kinases. It is upregulated in a variety of cancers and its overexpression is associated with poor disease prognosis and acquired drug resistance. Utilizing a fragment-based lead discovery approach, a new indazole-based AXL inhibitor was obtained. The indazole fragment hit 11, identified through a high concentration biochemical screen, was expeditiously improved to fragment 24 by screening our in-house expanded library of fragments (ELF) collection. Subsequent fragment optimization guided by docking studies provided potent inhibitor 54 with moderate exposure levels in mice. X-ray crystal structure of analog 50 complexed with the I650M mutated kinase domain of Mer revealed the key binding interactions for the scaffold. The good potency coupled with reasonable kinase selectivity, moderate in vivo exposure levels, and availability of structural information for the series makes it a suitable starting point for further optimization efforts.

Assuntos

Descoberta de Drogas; Indazóis/farmacologia; Inibidores de Proteínas Quinases/farmacologia; Proteínas Proto-Oncogênicas/antagonistas & inibidores; Receptores Proteína Tirosina Quinases/antagonistas & inibidores; Linhagem Celular Tumoral; Proliferação de Células/efeitos dos fármacos; Relação Dose-Resposta a Droga; Humanos; Indazóis/síntese química; Indazóis/química; Modelos Moleculares; Estrutura Molecular; Inibidores de Proteínas Quinases/síntese química; Inibidores de Proteínas Quinases/química; Proteínas Proto-Oncogênicas/metabolismo; Receptores Proteína Tirosina Quinases/metabolismo; Relação Estrutura-Atividade; Receptor Tirosina Quinase Axl

Palavras-chave

AXL inhibitor; Fragment hit-to-lead; Fragment optimization; Receptor tyrosine kinase inhibitor; TAM family of receptor tyrosine kinase

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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Proteínas Proto-Oncogênicas / Receptores Proteína Tirosina Quinases / Inibidores de Proteínas Quinases / Descoberta de Drogas / Indazóis Limite: Humans Idioma: En Revista: Bioorg Med Chem Assunto da revista: BIOQUIMICA / QUIMICA Ano de publicação: 2021 Tipo de documento: Article

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