Povetacicept for IgA Nephropathy and Primary Membranous Nephropathy
Arvind Madan, Rajesh Yalavarthy, Dong Ki Kim, Ju-Young Moon, Inwhee Park, Sreedhar Mandayam, Frank B. Cortazar, Sung Gyun Kim, Amanda Enstrom, Heather Thomas, Jiahua Li, Stanford L. Peng, Yih‐Chieh Chen, Jason C. Sanders, Ogo Egbuna, James A. Tumlin, Inwhee Park, Dong Ki Kim, James Tumlin, Rania K. El Fekih, Yong Kyu, Sung Gyun Kim, Eun Young Lee, Sang-Woong Han, Frank Cortazar, Arvind Madan, Rajesh Yalavarthy, Eugenia Pedagogos, Sreedhar Mandayam, Angus Ritchie, Ju-Young Moon, Alexander Nimri
Abstract
Introduction: Povetacicept is an inhibitor of B-cell activating factor (BAFF) and A proliferation-inducing ligand (APRIL), 2 cytokines central to the pathogenesis of autoimmune glomerulonephritis. Both BAFF and APRIL promote B-cell and plasma cell survival and function. APRIL primarily supports plasma cell survival and function, whereas BAFF regulates early pathogenic B-cell development, activates pathogenic T cells and innate immune cells, and contributes to mesangial cell proliferation and podocyte injury. Methods: . The primary objective was safety. Secondary objectives included change from baseline in urine protein-to-creatinine ratio (UPCR), eGFR, galactose-deficient IgA1 (Gd-IgA1) (IgAN), antiphospholipase A2 receptor autoantibody (aPLA2R; pMN), and clinical remission (with hematuria resolution for IgAN). Results: Povetacicept was administered subcutaneously every 4 weeks (Q4W) to 54 participants with IgAN (21 received 80 mg, 33 received 240 mg) and 10 with pMN (all received 80 mg). In this interim analysis, participants with IgAN on 80 mg had a 64% mean 24-hour UPCR decrease (95% confidence interval: -76 to -48) from baseline (1.3 g/g to 0.5 g/g; 65% with UPCR < 0.5 g/g) with stable eGFR at week 48. Early decline in Gd-IgA1 at week 12 (57%), continued at week 48 (77%). Approximately 90% achieved hematuria resolution and 53% achieved clinical remission. Efficacy outcomes were similar with 240 mg povetacicept. Participants with pMN had an 82% mean 24-hour UPCR decrease (95% confidence interval: -92 to -60) from baseline (3.8 g/g to 0.7 g/g) with stable eGFR. Early decline in aPLA2R at week 12 (73%), continued at week 48 (83%) with 100% in immunologic remission (40% achieved complete remission; 100% achieved partial remission). Povetacicept was generally safe and well-tolerated for IgAN and pMN. Conclusion: Povetacicept had substantial, sustained UPCR reductions with stable eGFR, significant Gd-IgA1 reductions, hematuria resolution, clinical remission, with favorable safety in IgAN. Similar results were observed in pMN. By inhibiting both BAFF and APRIL, povetacicept targets the underlying cause of disease and has potential to provide a significant therapeutic advancement for autoimmune glomerular diseases.