hVAPB, the causative gene of a heterogeneous group of motor neuron diseases in humans, is functionally interchangeable with its Drosophila homologue DVAP-33A at the neuromuscular junction

doi:10.1093/hmg/ddm303

Human Molecular Genetics Advance Access originally published online on October 18, 2007
Human Molecular Genetics 2008 17(2):266-280; doi:10.1093/hmg/ddm303

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hVAPB, the causative gene of a heterogeneous group of motor neuron diseases in humans, is functionally interchangeable with its Drosophila homologue DVAP-33A at the neuromuscular junction

Andrea Chai¹, James Withers¹, Young Ho Koh²^,4, Katherine Parry¹, Hong Bao³, Bing Zhang³, Vivian Budnik² and Giuseppa Pennetta¹^,*

¹ Center for Neuroscience Research, Royal (Dick) School of Veterinary Studies, University of Edinburgh, Summerhall, Edinburgh EH9 1QH, UK ² Department of Neurobiology, University of Massachusetts Medical School, Worcester, MA 01605-2324, USA ³ Department of Zoology, University of Oklahoma, Norman, OK 73019, USA ⁴ Ilsong Institute of Life Science, Hallym University, Anyang, Kyunggi-do 431-060, Korea

^* To whom correspondence should be addressed at: Tel: +44 (0)1316506144; Fax: +44 (0)1316506576; Email: g.pennetta{at}ed.ac.uk

Received September 3, 2007; Accepted October 10, 2007

Motor neuron diseases (MNDs) are progressive neurodegenerativedisorders characterized by selective death of motor neuronsleading to spasticity, muscle wasting and paralysis. Human VAMP-associatedprotein B (hVAPB) is the causative gene of a clinically diversegroup of MNDs including amyotrophic lateral sclerosis (ALS),atypical ALS and late-onset spinal muscular atrophy. The pathogenicmutation is inherited in a dominant manner. Drosophila VAMP-associatedprotein of 33 kDa A (DVAP-33A) is the structural homologueof hVAPB and regulates synaptic remodeling by affecting thesize and number of boutons at neuromuscular junctions. Associatedwith these structural alterations are compensatory changes inthe physiology and ultrastructure of synapses, which maintainevoked responses within normal boundaries. DVAP-33A and hVAPBare functionally interchangeable and transgenic expression ofmutant DVAP-33A in neurons recapitulates major hallmarks ofthe human diseases including locomotion defects, neuronal deathand aggregate formation. Aggregate accumulation is accompaniedby a depletion of the endogenous protein from its normal localization.These findings pinpoint to a possible role of hVAPB in synaptichomeostasis and emphasize the relevance of our fly model inelucidating the patho-physiology underlying motor neuron degenerationin humans.

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