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Identification of highly selective SIK1/2 inhibitors that modulate innate immune activation and suppress intestinal inflammation.
Babbe, Holger; Sundberg, Thomas B; Tichenor, Mark; Seierstad, Mark; Bacani, Genesis; Berstler, James; Chai, Wenying; Chang, Leon; Chung, De Michael; Coe, Kevin; Collins, Bernard; Finley, Michael; Guletsky, Alexander; Lemke, Christopher T; Mak, Puiying A; Mathur, Ashok; Mercado-Marin, Eduardo V; Metkar, Shailesh; Raymond, Donald D; Rives, Marie-Laure; Rizzolio, Michele; Shaffer, Paul L; Smith, Russell; Smith, Jacqueline; Steele, Ruth; Steffens, Helena; Suarez, Javier; Tian, Gaochao; Majewski, Nathan; Volak, Laurie P; Wei, Jianmei; Desai, Prerak T; Ong, Luvena L; Koudriakova, Tatiana; Goldberg, Steven D; Hirst, Gavin; Kaushik, Virendar K; Ort, Tatiana; Seth, Nilufer; Graham, Daniel B; Plevy, Scott; Venable, Jennifer D; Xavier, Ramnik J; Towne, Jennifer E.
Afiliação
  • Babbe H; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Sundberg TB; Broad Institute of MIT and Harvard, Center for the Development of Therapeutics, Cambridge, MA 02142.
  • Tichenor M; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Seierstad M; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Bacani G; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Berstler J; Broad Institute of MIT and Harvard, Center for the Development of Therapeutics, Cambridge, MA 02142.
  • Chai W; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Chang L; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Chung M; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Coe K; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Collins B; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Finley M; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Guletsky A; Broad Institute of MIT and Harvard, Center for the Development of Therapeutics, Cambridge, MA 02142.
  • Lemke CT; Broad Institute of MIT and Harvard, Center for the Development of Therapeutics, Cambridge, MA 02142.
  • Mak PA; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Mathur A; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Mercado-Marin EV; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Metkar S; Broad Institute of MIT and Harvard, Center for the Development of Therapeutics, Cambridge, MA 02142.
  • Raymond DD; Broad Institute of MIT and Harvard, Center for the Development of Therapeutics, Cambridge, MA 02142.
  • Rives ML; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Rizzolio M; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Shaffer PL; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Smith R; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Smith J; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Steele R; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Steffens H; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Suarez J; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Tian G; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Majewski N; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Volak LP; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Wei J; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Desai PT; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Ong LL; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Koudriakova T; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Goldberg SD; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Hirst G; Janssen Research and Development, LLC., San Diego, CA 92121.
  • Kaushik VK; Broad Institute of MIT and Harvard, Center for the Development of Therapeutics, Cambridge, MA 02142.
  • Ort T; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Seth N; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Graham DB; Center for Computational and Integrative Biology, Massachusetts General Hospital, Boston, MA 02114.
  • Plevy S; Department of Molecular Biology, Massachusetts General Hospital, Boston, MA 02114.
  • Venable JD; Klarman Cell Observatory, Broad Institute of MIT and Harvard, Cambridge, MA 02142.
  • Xavier RJ; Janssen Research and Development, LLC., Spring House, PA 19477.
  • Towne JE; Janssen Research and Development, LLC., San Diego, CA 92121.
Proc Natl Acad Sci U S A ; 121(1): e2307086120, 2024 Jan 02.
Article em En | MEDLINE | ID: mdl-38147543
ABSTRACT
The salt-inducible kinases (SIK) 1-3 are key regulators of pro- versus anti-inflammatory cytokine responses during innate immune activation. The lack of highly SIK-family or SIK isoform-selective inhibitors suitable for repeat, oral dosing has limited the study of the optimal SIK isoform selectivity profile for suppressing inflammation in vivo. To overcome this challenge, we devised a structure-based design strategy for developing potent SIK inhibitors that are highly selective against other kinases by engaging two differentiating features of the SIK catalytic site. This effort resulted in SIK1/2-selective probes that inhibit key intracellular proximal signaling events including reducing phosphorylation of the SIK substrate cAMP response element binding protein (CREB) regulated transcription coactivator 3 (CRTC3) as detected with an internally generated phospho-Ser329-CRTC3-specific antibody. These inhibitors also suppress production of pro-inflammatory cytokines while inducing anti-inflammatory interleukin-10 in activated human and murine myeloid cells and in mice following a lipopolysaccharide challenge. Oral dosing of these compounds ameliorates disease in a murine colitis model. These findings define an approach to generate highly selective SIK1/2 inhibitors and establish that targeting these isoforms may be a useful strategy to suppress pathological inflammation.
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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Proteínas Serina-Treonina Quinases / Proteína de Ligação ao Elemento de Resposta ao AMP Cíclico Limite: Animals / Humans Idioma: En Revista: Proc Natl Acad Sci U S A Ano de publicação: 2024 Tipo de documento: Article

Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Proteínas Serina-Treonina Quinases / Proteína de Ligação ao Elemento de Resposta ao AMP Cíclico Limite: Animals / Humans Idioma: En Revista: Proc Natl Acad Sci U S A Ano de publicação: 2024 Tipo de documento: Article