The Clinical and Molecular Spectrum of GM1 Gangliosidosis

Research output: Contribution to journalResearch articleContributedpeer-review

Contributors

  • Laila Arash-Kaps - , Johannes Gutenberg University Mainz (Author)
  • Katalin Komlosi - , Johannes Gutenberg University Mainz (Author)
  • Marlene Seegräber - , Johannes Gutenberg University Mainz (Author)
  • Stefan Diederich - , Johannes Gutenberg University Mainz (Author)
  • Eduard Paschke - , Medical University of Vienna (Author)
  • Yasmina Amraoui - , Johannes Gutenberg University Mainz (Author)
  • Skadi Beblo - , Leipzig University (Author)
  • Andrea Dieckmann - , Friedrich Schiller University Jena (Author)
  • Martin Smitka - , Department of Paediatrics, Division of Neuropediatrics (Author)
  • Julia B. Hennermann - , Johannes Gutenberg University Mainz (Author)

Abstract

Objective: To evaluate the clinical presentation of patients with GM1 gangliosidosis and to determine whether specific clinical or biochemical signs could lead to a prompt diagnosis. Study design: We retrospectively analyzed clinical, biochemical, and genetic data of 22 patients with GM1 gangliosidosis from 5 metabolic centers in Germany and Austria. Results: Eight patients were classified as infantile, 11 as late-infantile, and 3 as juvenile form. Delay of diagnosis was 6 ± 2.6 months in the infantile, 2.6 ± 3.79 years in the late-infantile, and 14 ± 3.48 years in the juvenile form. Coarse facial features, cherry red spots, and visceromegaly occurred only in patients with the infantile form. Patients with the late-infantile and juvenile forms presented with variable neurologic symptoms. Seventeen patients presented with dystonia and 14 with dysphagia. Laboratory analysis revealed an increased ASAT concentration (13/20), chitotriosidase activity (12/15), and pathologic urinary oligosaccharides (10/19). Genotype analyses revealed 23 causative or likely causative mutations in 19 patients, 7 of them being novel variants. In the majority, a clear genotype–phenotype correlation was found. Conclusions: Diagnosis of GM1 gangliosidosis often is delayed, especially in patients with milder forms of the disease. GM1 gangliosidosis should be considered in patients with progressive neurodegeneration and spastic-dystonic movement disorders, even in the absence of visceral symptoms or cherry red spots. ASAT serum concentrations and chitotriosidase activity may be of value in screening for GM1 gangliosidosis.

Details

Original languageEnglish
Pages (from-to)152-157.e3
JournalJournal of Pediatrics
Volume215
Publication statusPublished - Dec 2019
Peer-reviewedYes

External IDs

PubMed 31761138

Keywords

Keywords

  • beta-galactosidase-1 deficiency, chitotriosidase activity, elevated ASAT, genotype-phenotype-correlation, GLB1 gene, GLB1-deficiency

Library keywords