Exploring therapeutic strategies for infantile neuronal axonal dystrophy (INAD/PARK14)

Authors

Guang Lin, Baylor College of Medicine
Burak Tepe, Baylor College of Medicine
Geoff McGrane, The New York Stem Cell Foundation Research Institute
Regine C. Tipon, The New York Stem Cell Foundation Research Institute

Document Type

Article

Publication Title

eLife

Abstract

Infantile neuroaxonal dystrophy (INAD) is caused by recessive variants in PLA2G6 and is a lethal pediatric neurodegenerative disorder. Loss of the Drosophila homolog of PLA2G6, leads to ceramide accumulation, lysosome expansion, and mitochondrial defects. Here, we report that retromer function, ceramide metabolism, the endolysosomal pathway, and mitochondrial morphology are affected in INAD patient-derived neurons. We show that in INAD mouse models, the same features are affected in Purkinje cells, arguing that the neuropathological mechanisms are evolutionary conserved and that these features can be used as biomarkers. We tested 20 drugs that target these pathways and found that Ambroxol, Desipramine, Azoramide, and Genistein alleviate neurodegenerative phenotypes in INAD flies and INAD patient-derived neural progenitor cells. We also develop an AAV-based gene therapy approach that delays neurodegeneration and prolongs lifespan in an INAD mouse model.

DOI

10.7554/eLife.82555

Publication Date

1-1-2023

Recommended Citation

Lin, Guang; Tepe, Burak; McGrane, Geoff; and Tipon, Regine C., "Exploring therapeutic strategies for infantile neuronal axonal dystrophy (INAD/PARK14)" (2023). Open Access archive. 6340.
https://impressions.manipal.edu/open-access-archive/6340