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- Matthew J Farrer, Mary M Hulihan, Jennifer M Kachergus, Justus C Dächsel, A Jon Stoessl, Linda L Grantier, Susan Calne, Donald B Calne, Bernard Lechevalier, Francoise Chapon, Yoshio Tsuboi, Tatsuo Yamada, Ludwig Gutmann, Bülent Elibol, Kailash P Bhatia, Christian Wider, Carles Vilariño-Güell, Owen A Ross, Laura A Brown, Monica Castanedes-Casey, Dennis W Dickson, and Zbigniew K Wszolek.
- Division of Neurogenetics, Department of Neuroscience, Mayo Clinic Florida, Jacksonville, Florida 32224, USA. farrer.matthew@mayo.edu
- Nat. Genet. 2009 Feb 1; 41 (2): 163-5.
AbstractPerry syndrome consists of early-onset parkinsonism, depression, severe weight loss and hypoventilation, with brain pathology characterized by TDP-43 immunostaining. We carried out genome-wide linkage analysis and identified five disease-segregating mutations affecting the CAP-Gly domain of dynactin (encoded by DCTN1) in eight families with Perry syndrome; these mutations diminish microtubule binding and lead to intracytoplasmic inclusions. Our findings show that DCTN1 mutations, previously associated with motor neuron disease, can underlie the selective vulnerability of other neuronal populations in distinct neurodegenerative disorders.
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