The organizing committee of PARASOL (PROTEINURIA AND OTHER BIOMARKERS AS ENDPOINTS FOR CLINICAL TRIALS IN KIDNEY DISEASE) is pleased to announce that the PARASOL Project will extend its efforts to investigate potential clinical trial endpoints for two additional kidney diseases with significant unmet needs: APOL1 kidney disease and primary membranous nephropathy (PMN), including the association of anti-PLA2R antibodies. Both projects will be operationally coordinated by the International Society of Glomerular Disease (ISGD). NephCure, the Kidney Health Initiative (ASN), and the National Kidney Foundation will also continue their roles as overall project sponsors.
In parallel, the consortium continues its work on assessing endpoints in focal segmental glomerulosclerosis (FSGS) given the growth of that dataset, with publication anticipated in late 2025.
Endpoints for APOL1 Kidney Disease
APOL1 kidney disease (also known as AMKD for APOL1-mediated or APOL1-modified kidney disease) is a rapidly progressive category of proteinuric kidney disease modified by high-risk variants of the apolipoprotein L1 gene. Genetic testing has shown that a significant proportion of various kidney disease diagnoses involve an underlying APOL1 variant, including FSGS, viral-associated nephropathy, and hypertension. A high-risk APOL1 genotype also contributes to progression in other autoimmune kidney diseases and diabetic kidney disease.
Outcomes are poor: patients with a high-risk APOL1 genotype experience onset of kidney disease earlier in life, leading to a median age of kidney failure of 45.1 years. There is no currently approved drug that specifically targets APOL1 kidney disease, but interventional trials are ongoing.
In 2025, Rosenberg et al. analyzed ARIC, CRIC, and AASK cohorts, showing eGFR and UPCR at 3 years predict kidney failure, though further validation is needed. The PARASOL group with expertise in global data and endpoint evaluation, together with international APOL1 experts, is advancing this effort.
Primary Membranous Nephropathy and Anti-PLA2R Antibodies
In January 2023, NephCure hosted a workshop on anti-PLA2R antibodies in membranous nephropathy, with proceedings published in 2025. Key needs identified were clarifying aPLA2R’s role as a biomarker, regulatory pathways for its use in drug development, applications in trial design (inclusion, monitoring, endpoints), and refining proteinuria-based endpoints. These insights will guide future therapeutic development in PMN.
PARASOL will leverage the project’s infrastructure and processes to explore the potential for aPLA2R to be used as a surrogate endpoint for clinical trials and a qualitative marker for monitoring disease severity, as well as expanding the data-driven understanding of other potential proteinuria-based endpoints for PMN trials.
Organization and Project Structure
ISGD and all PARASOL stakeholders remain committed to collaboratively advancing patient care in glomerular diseases through multi-stakeholder collaboration and analysis of shared data. As with PARASOL-FSGS, collaboration and data sharing among multiple stakeholders will be crucial to project success. In alignment with the previous project structure, the projects will include three key meetings (kick off, interim, and public consensus) and will follow a timeline of approximately one year.
PARASOL-MN will be chaired by Patrick Nachman (University of Minnesota) and Tobias B. Huber (UKE Hamburg), with PARASOL-FSGS chairs Laura Mariani and Matthias Kretzler (both University of Michigan) as well as Brad Rovin (Ohio State University) serving as senior advisors.
PARASOL-AMKD will be chaired by Laura Mariani (University of Michigan), Rulan Parekh (University of Toronto), and Keisha Gibson (University of North Carolina) with Matthias Kretzler (University of Michigan) as a senior advisor.
The University of Michigan will serve as the data coordinating center, with Abigail Smith (Northwestern University) leading the data analysis for AMKD and Jarcy Zee (University of Pennsylvania) leading the data analysis for PMN.
The PARASOL team welcomes collaboration from other interested parties. For more information about the PARASOL project and how to participate, please visit the project website or contact the steering committee at parasol@is-gd.org.
Contact:
Steering Committee: parasol@is-gd.org
References
- Rosenberg AT, Flaherty C, Anderson AH, Appel LJ, Coresh J, He J, Lash JP, Liu C, Rao PS, Taliercio J, Surapaneni A, Grams ME; CRIC Study Investigators. Surrogate End Points in Apolipoprotein L1 - Associated Kidney Disease : Evaluation in Three Cohorts. Clin J Am Soc Nephrol. 2025 Jan 1;20(1):23-30. doi: 10.2215/CJN.0000000000000575. Epub 2024 Nov 5. PMID: 39499577; PMCID: PMC11737446.
- Prunotto M, Nachman PH, Gillespie BS, Beck LH Jr, Thompson AM, Hu AH, Stafford EA, Tarnoff JM, Rovin BH. Designing Clinical Trials for the Treatment of Membranous Nephropathy in the Anti-Phospholipase A2 Receptor 1 Era: Results of a NephCure Membranous Nephropathy Workshop. Glomerular Dis. 2025 Mar 14;5(1):133-141. doi: 10.1159/000544808. PMID: 40092585; PMCID: PMC11908811.
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