Small Molecule APOL1 Inhibitors as a Precision Medicine Approach for APOL1-mediated Kidney Disease

Author:

Zimmerman Brandon1,Dakin Leslie1,Fortier Anne1,Nanou Evanthia1,Blasio Angelo1,Mann James1,Miller Howard1,Fletcher Marissa1ORCID,Wang Tiansheng1,Nanthakumar Suganthini1,McCarthy Gizelle1,Matar Caline1,Matsye Prachi2,Wang Guanyu1,Snyder Phillip3,Daniel Kevin1,Swamy Harsha1ORCID,Sullivan Kelly1,Bright Franklin1,Powers Audrey1,Lu Fan1,Paula Steven1,Khare-Pandit Suvarna1,Henry Larry1,Hamel Martine1,Denis Francois1,Nicolas Olivier1,Hariparsad Niresh1,Kumar Shyamesh1,Proctor Jennifer1,Senter Timothy1ORCID,Furey Brinley4,Bunnage Mark2

Affiliation:

1. Vertex Pharmaceuticals

2. Vertex

3. Vertex Pharmaceuticals Inc.

4. Vertex Pharmaceuticals Incorporated

Abstract

Abstract Chronic kidney disease affects ~10% of people worldwide and there are no disease modifying therapeutics that address the underlying cause of any form of kidney disease. Genome wide association studies have identified the G1 and G2 variants in the apolipoprotein L1 (APOL1) gene as major contributors to a subtype of proteinuric kidney disease now referred to as APOL1‑mediated kidney disease (AMKD). We hypothesized that inhibition of APOL1 could have therapeutic potential for this genetically-defined form of kidney disease. Here we describe the development of preclinical assays and the discovery of highly potent and specific APOL1 inhibitors with drug-like properties. We provide evidence that APOL1 channel activity drives podocyte injury and that inhibition of this activity stops APOL1-mediated cell death and kidney damage in a transgenic mouse model. These preclinical data, combined with recent clinical data, support the potential of APOL1 channel inhibition for the treatment of AMKD.

Publisher

Research Square Platform LLC

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