Fabhalta Kidney Treatment Shows Promise in Slowing Disease Progression for IgA Nephropathy

Novartis has announced positive final results from the Phase III APPLAUSE-IgAN trial, which demonstrated that Fabhalta kidney treatment (iptacopan) achieved a statistically significant and clinically meaningful slowing of kidney function decline in patients with IgA nephropathy compared to placebo over two years. This outcome was measured by estimated glomerular filtration rate (eGFR) slope, marking the first Phase III trial to show that a complement inhibitor can slow IgAN disease progression. These findings build upon Fabhalta’s previously granted accelerated approval for proteinuria reduction in the United States in 2024, and the data supports Novartis’s planned 2026 submission for traditional FDA approval of Fabhalta for this indication.

Key Therapeutic Insights

The APPLAUSE-IgAN trial revealed that Fabhalta kidney treatment directly addresses the underlying pathophysiology of IgA nephropathy, a disease that involves inappropriate complement system activation driving kidney damage. The two-year data showing reduced eGFR decline represents a clinically significant outcome, as eGFR is considered the gold standard metric for measuring kidney function and disease progression in nephrology. These results build upon earlier nine-month data that showed a 38.3% greater reduction in proteinuria with Fabhalta compared to placebo, thereby establishing a dual therapeutic benefit where the treatment both reduces proteinuria—a key risk factor for progression—and directly slows kidney function decline. As the first and only complement inhibitor to demonstrate this dual effect in IgAN, Fabhalta potentially represents an important shift in the treatment approach for this progressive autoimmune kidney disease, which leads to kidney failure in many patients.

Disease Background and Unmet Needs

IgA nephropathy is recognized by the National Institutes of Health as the most common primary glomerulonephritis worldwide, with approximately 2.5 new cases per 100,000 people annually in the United States and higher prevalence in Asian populations. The National Kidney Foundation reports that about 30-40% of patients with IgAN progress to end-stage kidney disease within 20 years, even despite current standard of care that primarily focuses on blood pressure control with ACE inhibitors or ARBs and proteinuria reduction.

Research in the Journal of the American Society of Nephrology has increasingly identified the alternative complement pathway as critically involved in IgAN pathogenesis, which explains why targeted inhibition with iptacopan has shown such promising results. However, current treatment options often fail to halt disease progression, leaving a significant unmet medical need, as the Kidney Disease: Improving Global Outcomes (KDIGO) guidelines note that many patients continue to experience progressive kidney function decline despite optimal supportive care.

Broader Implications and Future Impact

For health economics and outcomes research, Fabhalta kidney treatment’s ability to slow eGFR decline in IgAN is a potentially transformative intervention that could substantially alter the disease trajectory and associated healthcare costs. According to Medicare data, end-stage kidney disease treatment costs exceed $90,000 annually per patient, so even modest delays in progression to kidney failure could generate substantial healthcare savings despite Fabhalta’s likely premium pricing. The dual benefit of reducing proteinuria and slowing eGFR decline suggests Fabhalta may improve both clinical outcomes and patient quality of life while also reducing the need for more intensive and costly interventions like dialysis.

As a targeted oral therapy, Fabhalta addresses the underlying disease mechanism rather than just symptoms, and it could establish a new treatment paradigm that shifts IgAN management from reactive symptom control to proactive disease modification. This shift has significant implications for future health technology assessments, value-based pricing models, and comparative effectiveness research in nephrology. Moreover, the positive Phase III results validate the complement pathway as a therapeutic target, which could accelerate development of similar mechanisms for other complement-mediated kidney diseases. For more information, you can visit the detailed press release by Novartis here.