| Literature DB >> 34382076 |
Serena Galosi1, Ban H Edani2,3, Simone Martinelli4, Hana Hansikova5, Erik A Eklund6, Caterina Caputi1, Laura Masuelli7, Nicole Corsten-Janssen8, Myriam Srour9,10, Renske Oegema11, Daniëlle G M Bosch11, Colin A Ellis12, Louise Amlie-Wolf13, Andrea Accogli9,10, Isis Atallah14, Luisa Averdunk15, Kristin W Barañano16, Roberto Bei17, Irene Bagnasco18, Alfredo Brusco19, Scott Demarest20,21, Anne-Sophie Alaix22, Carlo Di Bonaventura1, Felix Distelmaier15, Frances Elmslie23, Ziv Gan-Or10,24,25, Jean-Marc Good14, Karen Gripp13, Erik-Jan Kamsteeg26, Ellen Macnamara27, Carlo Marcelis28, Noëlle Mercier29, Joseph Peeden30, Simone Pizzi31, Luca Pannone31, Marwan Shinawi32, Camilo Toro27, Nienke E Verbeek11, Sunita Venkateswaran33, Patricia G Wheeler34, Lucie Zdrazilova5, Rong Zhang2,3, Giovanna Zorzi35, Renzo Guerrini36, William C Sessa2,3, Dirk J Lefeber37, Marco Tartaglia31, Fadi F Hamdan38, Kariona A Grabińska2,3, Vincenzo Leuzzi1.
Abstract
Subcellular membrane systems are highly enriched in dolichol, whose role in organelle homeostasis and endosomal-lysosomal pathway remains largely unclear besides being involved in protein glycosylation. DHDDS encodes for the catalytic subunit (DHDDS) of the enzyme cis-prenyltransferase (cis-PTase), involved in dolichol biosynthesis and dolichol-dependent protein glycosylation in the endoplasmic reticulum. An autosomal recessive form of retinitis pigmentosa (retinitis pigmentosa 59) has been associated with a recurrent DHDDS variant. Moreover, two recurring de novo substitutions were detected in a few cases presenting with neurodevelopmental disorder, epilepsy and movement disorder. We evaluated a large cohort of patients (n = 25) with de novo pathogenic variants in DHDDS and provided the first systematic description of the clinical features and long-term outcome of this new neurodevelopmental and neurodegenerative disorder. The functional impact of the identified variants was explored by yeast complementation system and enzymatic assay. Patients presented during infancy or childhood with a variable association of neurodevelopmental disorder, generalized epilepsy, action myoclonus/cortical tremor and ataxia. Later in the disease course, they experienced a slow neurological decline with the emergence of hyperkinetic and/or hypokinetic movement disorder, cognitive deterioration and psychiatric disturbances. Storage of lipidic material and altered lysosomes were detected in myelinated fibres and fibroblasts, suggesting a dysfunction of the lysosomal enzymatic scavenger machinery. Serum glycoprotein hypoglycosylation was not detected and, in contrast to retinitis pigmentosa and other congenital disorders of glycosylation involving dolichol metabolism, the urinary dolichol D18/D19 ratio was normal. Mapping the disease-causing variants into the protein structure revealed that most of them clustered around the active site of the DHDDS subunit. Functional studies using yeast complementation assay and in vitro activity measurements confirmed that these changes affected the catalytic activity of the cis-PTase and showed growth defect in yeast complementation system as compared with the wild-type enzyme and retinitis pigmentosa-associated protein. In conclusion, we characterized a distinctive neurodegenerative disorder due to de novo DHDDS variants, which clinically belongs to the spectrum of genetic progressive encephalopathies with myoclonus. Clinical and biochemical data from this cohort depicted a condition at the intersection of congenital disorders of glycosylation and inherited storage diseases with several features akin to of progressive myoclonus epilepsy such as neuronal ceroid lipofuscinosis and other lysosomal disorders.Entities:
Keywords: congenital disorders of glycosylation; dolichol; movement disorder; myoclonus epilepsy; neurodegenerative disorder
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Year: 2022 PMID: 34382076 PMCID: PMC8967098 DOI: 10.1093/brain/awab299
Source DB: PubMed Journal: Brain ISSN: 0006-8950 Impact factor: 15.255