Delineating pathological pathways in a chemically induced mouse model of Gaucher disease |
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Authors: | Anna Meshcheriakova Chen Yaacobi Raya Eilam Brandon M Kenwood Ahad A Rahim Giulia Massaro Alfred H Merrill Jr Anthony H Futerman |
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Affiliation: | 1. Department of Biological Chemistry, Weizmann Institute of Science, Rehovot, Israel;2. Department of Veterinary Resources, Weizmann Institute of Science, Rehovot, Israel;3. School of Biology and Petit Institute for Bioengineering and Bioscience, Georgia Institute of Technology, Atlanta, GA, USA;4. Department of Pharmacology, School of Pharmacy, University College London, London, UK |
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Abstract: | Great interest has been shown in understanding the pathology of Gaucher disease (GD) due to the recently discovered genetic relationship with Parkinson's disease. For such studies, suitable animal models of GD are required. Chemical induction of GD by inhibition of acid β‐glucosidase (GCase) using the irreversible inhibitor conduritol B‐epoxide (CBE) is particularly attractive, although few systematic studies examining the effect of CBE on the development of symptoms associated with neurological forms of GD have been performed. We now demonstrate a correlation between the amount of CBE injected into mice and levels of accumulation of the GD substrates, glucosylceramide and glucosylsphingosine, and show that disease pathology, indicated by altered levels of pathological markers, depends on both the levels of accumulated lipids and the time at which their accumulation begins. Gene array analysis shows a remarkable similarity in the gene expression profiles of CBE‐treated mice and a genetic GD mouse model, the Gbaflox/flox;nestin‐Cre mouse, with 120 of the 144 genes up‐regulated in CBE‐treated mice also up‐regulated in Gbaflox/flox;nestin‐Cre mice. We also demonstrate that various aspects of neuropathology and some behavioural abnormalities can be arrested upon cessation of CBE treatment during a specific time window. Together, our data demonstrate that injection of mice with CBE provides a rapid and relatively easy way to induce symptoms typical of neuronal forms of GD. This is particularly useful when examining the role of specific biochemical pathways in GD pathology, since CBE can be injected into mice defective in components of putative pathological pathways, alleviating the need for time‐consuming crossing of mice. Copyright © 2016 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd. |
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Keywords: | Gaucher disease Parkinson's disease acid β ‐glucosidase glucosylceramide glucosylsphingosine neuropathology neuroinflammation |
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