Agonists of prostaglandin E 2 receptors as potential first in class treatment for nephronophthisis and related ciliopathies.
Hugo GarciaAlice S SerafinFlora SilbermannEsther PoréeAmandine ViauClémentine MahautKaty BillotÉléonore BirgyMeriem Garfa-TraoreStéphanie RoySalomé CeccarelliManon MehrazPamela C RodriguezBérangère DelegliseLaetitia FurioFabienne Jabot-HaninNicolas CagnardElaine Del NeryMarc FilaSoraya Sin-MonnotCorinne AntignacStanislas LyonnetPauline KrugRémi SalomonJean-Philippe AnnereauAlexandre BenmerahMarion DelousLuis Briseño-RoaSophie SaunierPublished in: Proceedings of the National Academy of Sciences of the United States of America (2022)
Nephronophthisis (NPH) is an autosomal recessive tubulointerstitial nephropathy belonging to the ciliopathy disorders and known as the most common cause of hereditary end-stage renal disease in children. Yet, no curative treatment is available. The major gene, NPHP1, encodes a protein playing key functions at the primary cilium and cellular junctions. Using a medium-throughput drug-screen in NPHP1 knockdown cells, we identified 51 Food and Drug Administration-approved compounds by their ability to alleviate the cellular phenotypes associated with the loss of NPHP1; 11 compounds were further selected for their physicochemical properties. Among those compounds, prostaglandin E1 (PGE1) rescued ciliogenesis defects in immortalized patient NPHP1 urine-derived renal tubular cells, and improved ciliary and kidney phenotypes in our NPH zebrafish and Nphp1 knockout mouse models. Furthermore, Taprenepag, a nonprostanoid prostaglandin E2 receptor agonist, alleviated the severe retinopathy observed in Nphp1−/− mice. Finally, comparative transcriptomics allowed identification of key signaling pathways downstream PGE1, including cell cycle progression, extracellular matrix, adhesion, or actin cytoskeleton organization. In conclusion, using in vitro and in vivo models, we showed that prostaglandin E2 receptor agonists can ameliorate several of the pleotropic phenotypes caused by the absence of NPHP1; this opens their potential as a first therapeutic option for juvenile NPH-associated ciliopathies.
Keyphrases
- cell cycle
- induced apoptosis
- extracellular matrix
- drug administration
- end stage renal disease
- cell cycle arrest
- chronic kidney disease
- signaling pathway
- peritoneal dialysis
- cell proliferation
- high throughput
- young adults
- mouse model
- metabolic syndrome
- type diabetes
- risk assessment
- case report
- single cell
- single molecule
- early onset
- oxidative stress
- genome wide
- gene expression
- endothelial cells
- electronic health record
- wild type
- cell adhesion