ALDH18A1gene mutations cause dominant spastic paraplegia SPG9: loss of function effect and plausibility of a dominant negative mechanism | Zendy

Emanuele Panza | Zendy; Juan Manuel Escamilla | Zendy; Clara MarcoMarín | Zendy; Nadine Gougeard | Zendy; Giuseppe De Michele | Zendy; Vincenzo Brescia Morra | Zendy; Rocco Liguori | Zendy; Leonardo Salviati | Zendy; Maria Alice Donati | Zendy; Roberto Cusano | Zendy; Tommaso Pippucci | Zendy; Roberto Ravazzolo | Zendy; Andrea H. Németh | Zendy; Sarah Smithson | Zendy; Sally Davies | Zendy; Jane A. Hurst | Zendy; Domenico Bordo | Zendy; Vicente Rubio | Zendy; Marco Seri | Zendy

Open Access

ALDH18A1gene mutations cause dominant spastic paraplegia SPG9: loss of function effect and plausibility of a dominant negative mechanism

Author(s) -

Emanuele Panza,

Juan Manuel Escamilla,

Clara MarcoMarín,

Nadine Gougeard,

Giuseppe De Michele,

Vincenzo Brescia Morra,

Rocco Liguori,

Leonardo Salviati,

Maria Alice Donati,

Roberto Cusano,

Tommaso Pippucci,

Roberto Ravazzolo,

Andrea H. Németh,

Sarah Smithson,

Sally Davies,

Jane A. Hurst,

Domenico Bordo,

Vicente Rubio,

Marco Seri

Publication year - 2015

Publication title -

brain

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 5.142

H-Index - 336

eISSN - 1460-2156

pISSN - 0006-8950

DOI - 10.1093/brain/awv247

Subject(s) - mechanism (biology) , hereditary spastic paraplegia , loss function , paraplegia , spastic , genetics , mutation , neuroscience , gene , function (biology) , psychology , phenotype , medicine , biology , physical medicine and rehabilitation , spinal cord , cerebral palsy , philosophy , epistemology

In support of the message of this paper, we would like to report that mutations in ALDH18A1 , the causative gene in Coutelier’s paper, are the cause of SPG9 (MIM#601162), a rare form of autosomal dominant hereditary spastic paraplegia (HSP) complicated with vomiting and congenital bilateral cataracts that was reported by our group in a British family and an Italian family ( Slavotinek et al. , 1996 ; Seri et al. , 1999 ). The British family that we report presents one of the dominant mutations reported by Coutelier et al. (2015) . Furthermore, we show that the mutations we report here are loss-of-function mutations by using site-directed mutagenesis and enzyme activity studies with purified recombinant Δ 1 -pyrroline-5-carboxylate synthetase (P5CS), the enzyme encoded by ALDH18A1 . Finally, we provide some experimental and structural evidence that renders plausible a dominant negative mechanism for the dominant inheritance of the disease for these mutations and for other ALDH18A1 mutations exhibiting this type of inheritance

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