JAK selectivity and the implications for clinical inhibition of pharmacodynamic cytokine signalling by filgotinib, upadacitinib, tofacitinib and baricitinib

Paqui G Traves; Bernard Murray; Federico Campigotto; René Galien; Amy Meng; Julie A Di Paolo

doi:10.1136/annrheumdis-2020-219012

JAK selectivity and the implications for clinical inhibition of pharmacodynamic cytokine signalling by filgotinib, upadacitinib, tofacitinib and baricitinib

Ann Rheum Dis. 2021 Jul;80(7):865-875. doi: 10.1136/annrheumdis-2020-219012. Epub 2021 Mar 19.

Authors

Paqui G Traves¹, Bernard Murray², Federico Campigotto³, René Galien⁴, Amy Meng⁵, Julie A Di Paolo⁶

Affiliations

¹ Inflammation Biology, Gilead Sciences, Foster City, California, USA.
² Drug Metabolism, Gilead Sciences, Foster City, California, USA.
³ Biology Core Support, Gilead Sciences, Foster City, California, USA.
⁴ Translational Research, Galapagos SASU, Romainville, France.
⁵ Clinical Pharmacology, Gilead Sciences, Foster City, California, USA.
⁶ External Innovation, Gilead Sciences, Foster City, California, USA julie.dipaolo@gilead.com.

Abstract

Objective: Janus kinase inhibitors (JAKinibs) are efficacious in rheumatoid arthritis (RA) with variable reported rates of adverse events, potentially related to differential JAK family member selectivity. Filgotinib was compared with baricitinib, tofacitinib and upadacitinib to elucidate the pharmacological basis underlying its clinical efficacy and safety.

Methods: In vitro JAKinib inhibition of signal transducer and activator of transcription phosphorylation (pSTAT) was measured by flow cytometry in peripheral blood mononuclear cells and whole blood from healthy donors and patients with RA following cytokine stimulation of distinct JAK/STAT pathways. The average daily pSTAT and time above 50% inhibition were calculated at clinical plasma drug exposures in immune cells. The translation of these measures was evaluated in ex vivo-stimulated assays in phase 1 healthy volunteers.

Results: JAKinib potencies depended on cytokine stimulus, pSTAT readout and cell type. JAK1-dependent pathways (interferon (IFN)α/pSTAT5, interleukin (IL)-6/pSTAT1) were among the most potently inhibited by all JAKinibs in healthy and RA blood, with filgotinib exhibiting the greatest selectivity for JAK1 pathways. Filgotinib (200 mg once daily) had calculated average daily target inhibition for IFNα/pSTAT5 and IL-6/pSTAT1 that was equivalent to tofacitinib (5 mg two times per day), upadacitinib (15 mg once daily) and baricitinib (4 mg once daily), with the least average daily inhibition for the JAK2-dependent and JAK3-dependent pathways including IL-2, IL-15, IL-4 (JAK1/JAK3), IFNγ (JAK1/JAK2), granulocyte colony stimulating factor, IL-12, IL-23 (JAK2/tyrosine kinase 2) and granulocyte-macrophage colony-stimulating factor (JAK2/JAK2). Ex vivo pharmacodynamic data from phase 1 healthy volunteers clinically confirmed JAK1 selectivity of filgotinib.

Conclusion: Filgotinib inhibited JAK1-mediated signalling similarly to other JAKinibs, but with less inhibition of JAK2-dependent and JAK3-dependent pathways, providing a mechanistic rationale for its apparently differentiated efficacy:safety profile.

Keywords: antirheumatic agents; arthritis; cytokines; immune system diseases; rheumatoid.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antirheumatic Agents / pharmacology*
Arthritis, Rheumatoid
Azetidines / pharmacology
Cells, Cultured
Cytokines / drug effects*
Heterocyclic Compounds, 3-Ring / pharmacology
Humans
Janus Kinase Inhibitors / pharmacology*
Janus Kinases / drug effects*
Piperidines / pharmacology
Purines / pharmacology
Pyrazoles / pharmacology
Pyridines / pharmacology*
Pyrimidines / pharmacology
Sulfonamides / pharmacology
Triazoles / pharmacology*

Substances

Antirheumatic Agents
Azetidines
Cytokines
GLPG0634
Heterocyclic Compounds, 3-Ring
Janus Kinase Inhibitors
Piperidines
Purines
Pyrazoles
Pyridines
Pyrimidines
Sulfonamides
Triazoles
upadacitinib
tofacitinib
Janus Kinases
baricitinib