Unexpected Phenotypic and Molecular Changes of Combined Glucocerebrosidase and Acid Sphingomyelinase Deficiency

Overview

Journal Dis Model Mech

Specialty General Medicine

Date 2023 Mar 23

PMID 36951087

Authors

Marcus Keatinge

Matthew E Gegg

Lisa Watson

Heather Mortiboys

Nan Li

Mark Dunning

Deepak Ailani

Hai Bui

Astrid van Rens

Dirk J Lefeber

Anthony H V Schapira

Ryan B MacDonald

Oliver Bandmann

Affiliations

Soon will be listed here.

Abstract

Heterozygous variants in GBA1, encoding glucocerebrosidase (GCase), are the most common genetic risk factor for Parkinson's disease (PD). Moreover, sporadic PD patients also have a substantial reduction of GCase activity. Genetic variants of SMPD1 are also overrepresented in PD cohorts, whereas a reduction of its encoded enzyme (acid sphingomyelinase or ASM) activity is linked to an earlier age of PD onset. Despite both converging on the ceramide pathway, how the combined deficiencies of both enzymes might interact to modulate PD has yet to be explored. Therefore, we created a double-knockout (DKO) zebrafish line for both gba1 (or gba) and smpd1 to test for an interaction in vivo, hypothesising an exacerbation of phenotypes in the DKO line compared to those for single mutants. Unexpectedly, DKO zebrafish maintained conventional swimming behaviour and had normalised neuronal gene expression signatures compared to those of single mutants. We further identified rescue of mitochondrial Complexes I and IV in DKO zebrafish. Despite having an unexpected rescue effect, our results confirm ASM as a modifier of GBA1 deficiency in vivo. Our study highlights the need for validating how genetic variants and enzymatic deficiencies may interact in vivo.

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