Neuronopathic Gaucher disease models reveal defects in cell growth promoted by Hippo pathway activation

Author:

Messelodi Daria,Strocchi SilviaORCID,Bertuccio Salvatore Nicola,Baden Pascale,Indio Valentina,Giorgi Federico M.ORCID,Taddia Alberto,Serravalle Salvatore,Valente Sabrina,di Fonzo AlessioORCID,Frattini Emanuele,Bernardoni Roberto,Pession Annalisa,Grifoni DanielaORCID,Deleidi MichelaORCID,Astolfi AnnalisaORCID,Pession Andrea

Abstract

AbstractGaucher Disease (GD), the most common lysosomal disorder, arises from mutations in the GBA1 gene and is characterized by a wide spectrum of phenotypes, ranging from mild hematological and visceral involvement to severe neurological disease. Neuronopathic patients display dramatic neuronal loss and increased neuroinflammation, whose molecular basis are still unclear. Using a combination of Drosophila dGBA1b loss-of-function models and GD patient-derived iPSCs differentiated towards neuronal precursors and mature neurons we showed that different GD- tissues and neuronal cells display an impairment of growth mechanisms with an increased cell death and reduced proliferation. These phenotypes are coupled with the downregulation of several Hippo transcriptional targets, mainly involved in cells and tissue growth, and YAP exclusion from nuclei. Interestingly, Hippo knock-down in the GBA-KO flies rescues the proliferative defect, suggesting that targeting the Hippo pathway can be a promising therapeutic approach to neuronopathic GD.

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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