AUTHOR=El-Sitt Sally , Soueid Jihane , Al Ali Jamal , Makoukji Joelle , Makhoul Nadine J. , Harati Hayat , Boustany Rose-Mary 

TITLE=Developmental Comparison of Ceramide in Wild-Type and Cln3Δex7/8 Mouse Brains and Sera

JOURNAL=Frontiers in Neurology

VOLUME=10

YEAR=2019

URL=https://www.frontiersin.org/journals/neurology/articles/10.3389/fneur.2019.00128

DOI=10.3389/fneur.2019.00128

ISSN=1664-2295

ABSTRACT=<p>CLN3 disease is a neurodevelopmental disease leading to early visual failure, motor decline, and death. CLN3 pathogenesis has been linked to dysregulation of ceramide, a key intracellular messenger impacting various biological functions. Ceramide is upregulated in brains of CLN3 patients and activates apoptosis. Ceramide levels over the lifespan of WT and <italic>Cln3</italic><sup>Δ<italic>ex7/8</italic></sup> mice were measured using the DGK assay. Ceramide subspecies were determined by LC-MS. Ceramide synthesis enzymes and pre- and post-synaptic mRNA expression was measured in <italic>Cln3</italic><sup>Δ<italic>ex7/8</italic></sup> and normal mouse brains. Neuronal cell death was established by PARP cleavage and Caspases 3/6/9 and cytochrome C mRNA expression in <italic>Cln3</italic><sup>Δ<italic>ex7/8</italic></sup> and normal mouse brains. In WT mouse, a ceramide peak was noted at 3 weeks of age. The absence of this peak in <italic>Cln3</italic><sup>Δ<italic>ex7/8</italic></sup> mice might be related to early disease pathogenesis. Increase of ceramide in <italic>Cln3</italic><sup>Δ<italic>ex7/8</italic></sup> mouse brain at 24 weeks of age precedes neuronal apoptosis. The correlation between serum and brain ceramide in WT mice, and dysregulation of ceramide in serum and brain of <italic>Cln3</italic><sup>Δ<italic>ex7/8</italic></sup> mice, and the significant increase in ceramide in <italic>Cln3</italic><sup>Δ<italic>ex7/8</italic></sup> mouse brains and sera argue for use of easily accessible serum ceramide levels to track response to novel therapies in human CLN3 disease.</p>