biostudies-literatureUnknown8(9)Cabasso OSHIREIsrael Science FoundationPfizer PharmaceuticalsGaucher disease (GD) results from mutations in the <i>GBA1</i> gene, which encodes lysosomal glucocerebrosidase (GCase). The large number of mutations known to date in the gene lead to a heterogeneous disorder, which is divided into a non-neuronopathic, type 1 GD, and two neurological, type 2 and type 3, forms. We studied the two fly <i>GBA1</i> orthologs, <i>GBA1a</i> and <i>GBA1b</i>. Each contains a Minos element insertion, which truncates its coding sequence. In the <i>GBA1a</i>^m/m flies, which express a mutant protein, missing 33 C-terminal amino acids, there was no decrease in GCase activity or substrate accumulation. However, <i>GBA1b</i>^m/m mutant flies presented a significant decrease in GCase activity with concomitant substrate accumulation, which included C14:1 glucosylceramide and C14:0 glucosylsphingosine. <i>GBA1b</i>^m/m mutant flies showed activation of the Unfolded Protein Response (UPR) and presented inflammation and neuroinflammation that culminated in development of a neuronopathic disease. Treatment with ambroxol did not rescue GCase activity or reduce substrate accumulation; however, it ameliorated UPR, inflammation and neuroinflammation, and increased life span. Our results highlight the resemblance between the phenotype of the <i>GBA1b</i>^m/m mutant fly and neuronopathic GD and underlie its relevance in further GD studies as well as a model to test possible therapeutic modalities.Journal of clinical medicinehttps://www.ebi.ac.uk/biostudies/studies/S-EPMC6780790biostudies-literature<i>Drosophila melanogaster</i> Mutated in its <i>GBA1b</i> Ortholog Recapitulates Neuronopathic Gaucher Disease.PMC6780790IIR-ISR-0008771300/13WI22427Ferraz MPasmanik-Chor MKrivoruk OMirzaian MHorowitz MDorot OPaul SAerts JMaor GCabasso Ofalse<i>Drosophila melanogaster</i> Mutated in its <i>GBA1b</i> Ortholog Recapitulates Neuronopathic Gaucher Disease.Gaucher disease (GD) results from mutations in the <i>GBA1</i> gene, which encodes lysosomal glucocerebrosidase (GCase). The large number of mutations known to date in the gene lead to a heterogeneous disorder, which is divided into a non-neuronopathic, type 1 GD, and two neurological, type 2 and type 3, forms. We studied the two fly <i>GBA1</i> orthologs, <i>GBA1a</i> and <i>GBA1b</i>. Each contains a Minos element insertion, which truncates its coding sequence. In the <i>GBA1a</i>^m/m flies, which express a mutant protein, missing 33 C-terminal amino acids, there was no decrease in GCase activity or substrate accumulation. However, <i>GBA1b</i>^m/m mutant flies presented a significant decrease in GCase activity with concomitant substrate accumulation, which included C14:1 glucosylceramide and C14:0 glucosylsphingosine. <i>GBA1b</i>^m/m mutant flies showed activation of the Unfolded Protein Response (UPR) and presented inflammation and neuroinflammation that culminated in development of a neuronopathic disease. Treatment with ambroxol did not rescue GCase activity or reduce substrate accumulation; however, it ameliorated UPR, inflammation and neuroinflammation, and increased life span. Our results highlight the resemblance between the phenotype of the <i>GBA1b</i>^m/m mutant fly and neuronopathic GD and underlie its relevance in further GD studies as well as a model to test possible therapeutic modalities.2019-01-01T00:00:00Z2019 Sep2021-03-18T08:13:19Z2019-11-07T08:04:23ZS-EPMC67807903150586510.3390/jcm8091420