Kidney International Reports (Dec 2023)
Randomized Trial on the Effect of an Oral Spleen Tyrosine Kinase Inhibitor in the Treatment of IgA Nephropathy
- Frederick W.K. Tam,
- James Tumlin,
- Jonathan Barratt,
- Brad H. Rovin,
- Ian S.D. Roberts,
- Candice Roufosse,
- H. Terence Cook,
- Gurjeet Bhangal,
- Alison L. Brown,
- Martin Busch,
- Fayaz Dudhiya,
- Anne-Marie Duliege,
- Donald J. Fraser,
- Daniel P. Gale,
- Chiu-Ching Huang,
- Ping-Chin Lai,
- Meng Lee,
- Esteban S. Masuda,
- Stephen P. McAdoo,
- Alexander R. Rosenkranz,
- Claudia Sommerer,
- Gere Sunder-Plassmann,
- Cheuk-Chun Szeto,
- Sydney C.W. Tang,
- Don E. Williamson,
- Lisa Willcocks,
- Volker Vielhauer,
- Min Jeong Kim,
- Leslie Todd,
- Hany Zayed,
- Sandra Tong-Starksen,
- Richard Lafayette
Affiliations
- Frederick W.K. Tam
- Centre for Inflammatory Disease, Department of Immunology and Inflammation, Imperial College London, Hammersmith Hospital, Imperial College Healthcare NHS Trust, London, UK; Correspondence: Frederick Wai Keung Tam, Centre for Inflammatory Disease, 9th floor, Commonwealth Building, Hammersmith Hospital Campus, Imperial College London, Du Cane Road, London W12 0NN, UK.
- James Tumlin
- Department of Nephrology, Emory University School Medicine, Atlanta, Georgia, USA
- Jonathan Barratt
- Department of Cardiovascular Sciences, University of Leicester, Leicester, UK
- Brad H. Rovin
- Division of Nephrology, Ohio State University Wexner Medical Center, Columbus, Ohio, USA
- Ian S.D. Roberts
- Department of Cellular Pathology, John Radcliffe Hospital, Oxford University Hospital NHS FT, Oxford, UK
- Candice Roufosse
- Centre for Inflammatory Disease, Department of Immunology and Inflammation, Imperial College London, Hammersmith Hospital, Imperial College Healthcare NHS Trust, London, UK
- H. Terence Cook
- Centre for Inflammatory Disease, Department of Immunology and Inflammation, Imperial College London, Hammersmith Hospital, Imperial College Healthcare NHS Trust, London, UK
- Gurjeet Bhangal
- Centre for Inflammatory Disease, Department of Immunology and Inflammation, Imperial College London, Hammersmith Hospital, Imperial College Healthcare NHS Trust, London, UK
- Alison L. Brown
- Freeman Hospital, Newcastle upon Tyne, UK
- Martin Busch
- Department of Internal Medicine III, University Hospital Jena, Friedrich Schiller University, Jena, Germany
- Fayaz Dudhiya
- Centre for Inflammatory Disease, Department of Immunology and Inflammation, Imperial College London, Hammersmith Hospital, Imperial College Healthcare NHS Trust, London, UK
- Anne-Marie Duliege
- Department of Clinical Development, Rigel Pharmaceuticals, Inc., South San Francisco, California, USA
- Donald J. Fraser
- Wales Kidney Research Unit, Cardiff University, School of Medicine, Heath Park, Cardiff, UK
- Daniel P. Gale
- Department of Renal Medicine, University College London, London, UK
- Chiu-Ching Huang
- Division of Nephrology, China Medical University Hospital, Taichung, Taiwan
- Ping-Chin Lai
- Division of Nephrology, China Medical University Hospital, Taichung, Taiwan; School of Medicine, Chang Gung University, Taoyuan, Taiwan
- Meng Lee
- Department of Clinical Development, Rigel Pharmaceuticals, Inc., South San Francisco, California, USA
- Esteban S. Masuda
- Department of Clinical Development, Rigel Pharmaceuticals, Inc., South San Francisco, California, USA
- Stephen P. McAdoo
- Centre for Inflammatory Disease, Department of Immunology and Inflammation, Imperial College London, Hammersmith Hospital, Imperial College Healthcare NHS Trust, London, UK
- Alexander R. Rosenkranz
- Division of Nephrology, Department of Internal Medicine, Medical University of Graz, Graz, Austria
- Claudia Sommerer
- Nephrology, University Hospital Heidelberg, Heidelberg, Germany
- Gere Sunder-Plassmann
- Division of Nephrology and Dialysis, Department of Medicine III, Medical University of Vienna, Vienna, Austria
- Cheuk-Chun Szeto
- Department of Medicine and Therapeutics, The Chinese University of Hong Kong, Prince of Wales Hospital, Shatin, N.T., Hong Kong SAR, China
- Sydney C.W. Tang
- Division of Nephrology, Department of Medicine, School of Clinical Medicine, The University of Hong Kong, Queen Mary Hospital, Hong Kong
- Don E. Williamson
- Southeastern Clinical Research Institute, Augusta, Georgia, USA
- Lisa Willcocks
- Addenbrookes Hospital, Cambridge, UK
- Volker Vielhauer
- Medizinische Klinik und Poliklinik IV, Nephrologisches Zentrum, Klinikum der Universität München, Munich, Germany
- Min Jeong Kim
- Division of Nephrology, Cantonal Hospital Aarau, Aarau, Switzerland
- Leslie Todd
- Department of Clinical Development, Rigel Pharmaceuticals, Inc., South San Francisco, California, USA
- Hany Zayed
- Department of Clinical Development, Rigel Pharmaceuticals, Inc., South San Francisco, California, USA
- Sandra Tong-Starksen
- Department of Clinical Development, Rigel Pharmaceuticals, Inc., South San Francisco, California, USA
- Richard Lafayette
- Department of Nephrology, Stanford University Medical Center, Stanford, California, USA
- Journal volume & issue
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Vol. 8,
no. 12
pp. 2546 – 2556
Abstract
Introduction: We reported increased spleen tyrosine kinase (SYK) expression in kidney biopsies of patients with IgA nephropathy (IgAN) and that inhibition of SYK reduces inflammatory cytokines production from IgA stimulated mesangial cells. Methods: This study was a double-blind, randomized, placebo-controlled phase 2 trial of fostamatinib (an oral SYK inhibitor) in 76 patients with IgAN. Patients were randomized to receive placebo, fostamatinib at 100 mg or 150 mg twice daily for 24 weeks on top of maximum tolerated dose of renin-angiotensin system inhibitors. The primary end point was reduction of proteinuria. Secondary end points included change from baseline in estimated glomerular filtration rate (eGFR) and kidney histology. Results: Although we could not detect significant reduction in proteinuria with fostamatinib overall, in a predetermined subgroup analysis, there was a trend for dose-dependent reduction in median proteinuria (from baseline to 24 weeks by 14%, 27%, and 36% in the placebo, fostamatinib 100 mg, and 150 mg groups, respectively) in patients with baseline urinary protein-to-creatinine ratios (UPCR) more than 1000 mg/g. Kidney function (eGFR) remained stable in all groups. Fostamatinib was well-tolerated. Side effects included diarrhea, hypertension, and increased liver enzymes. Thirty-nine patients underwent repeat biopsy showing reductions in SYK staining associated with therapy at low dose (−1.5 vs. 1.7 SYK+ cells/glomerulus in the placebo group, P < 0.05). Conclusions: There was a trend toward reduction in proteinuria with fostamatinib in a predefined analysis of high risk patients with IgAN despite maximal care, as defined by baseline UPCR greater than 1000 mg/g. Further study may be warranted.
