BACKGROUND: hereditary spastic paraplegias (HSP) are a group of neurodegenerative disorders characterized by progressive lower extremity spastic weakness. SPG7, SPG4 and SPG3A are some of the autosomal genes recently found as mutated in recessive or dominant forms of HSP in childhood. SPG31 is more often associated with a pure spastic paraplegia phenotype, but genotype-phenotype correlation is still unclear. The aims of the current study was: (i) to verify the mutational frequency of SPG4, SPG3A, SPG31 and SPG7 genes in our very-well-selected childhood sample, and (ii) to improve our knowledge about the clinical and electrophysiological HSP phenotypes and their possible correlation with a specific mutation. METHODS: a sample of 14 Italian children affected by pure HSP (mean age at diagnosis 5.9 years) was extensively investigated with electrophysiological, neuroradiological and genetic tests. RESULTS: three SPG4 mutations were identified in three patients: two novel missense mutations, both sporadic, and one multiexonic deletion already reported. A novel large deletion in SPG31 gene involving exons 2-5 was also detected in one young patient. No mutations in the SPG7 and in the SPG3A genes were found. CONCLUSIONS: our data confirm that HSP represent a heterogeneous group of genetic neurodegenerative disorders, also in sporadic or autosomal recessive early onset forms. Multiplex Ligation-dependent Probe Amplification-based mutation screening for SPG4 and SPG31 genes would be added to sequencing-based screening of SPG4, SPG31 and SPG3A genes in the routine diagnosis of HSP children.
BACKGROUND:hereditary spastic paraplegias (HSP) are a group of neurodegenerative disorders characterized by progressive lower extremity spastic weakness. SPG7, SPG4 and SPG3A are some of the autosomal genes recently found as mutated in recessive or dominant forms of HSP in childhood. SPG31 is more often associated with a pure spastic paraplegia phenotype, but genotype-phenotype correlation is still unclear. The aims of the current study was: (i) to verify the mutational frequency of SPG4, SPG3A, SPG31 and SPG7 genes in our very-well-selected childhood sample, and (ii) to improve our knowledge about the clinical and electrophysiological HSP phenotypes and their possible correlation with a specific mutation. METHODS: a sample of 14 Italian children affected by pure HSP (mean age at diagnosis 5.9 years) was extensively investigated with electrophysiological, neuroradiological and genetic tests. RESULTS: three SPG4 mutations were identified in three patients: two novel missense mutations, both sporadic, and one multiexonic deletion already reported. A novel large deletion in SPG31 gene involving exons 2-5 was also detected in one young patient. No mutations in the SPG7 and in the SPG3A genes were found. CONCLUSIONS: our data confirm that HSP represent a heterogeneous group of genetic neurodegenerative disorders, also in sporadic or autosomal recessive early onset forms. Multiplex Ligation-dependent Probe Amplification-based mutation screening for SPG4 and SPG31 genes would be added to sequencing-based screening of SPG4, SPG31 and SPG3A genes in the routine diagnosis of HSP children.
Authors: Claudia Dufke; Nina Schlipf; Rebecca Schüle; Michael Bonin; Michaela Auer-Grumbach; Giovanni Stevanin; Christel Depienne; Jan Kassubek; Stephan Klebe; Sven Klimpe; Thomas Klopstock; Susanne Otto; Sven Poths; Andrea Seibel; Henning Stolze; Andreas Gal; Ludger Schöls; Peter Bauer Journal: Neurogenetics Date: 2012-05-03 Impact factor: 2.660
Authors: Philip M Boone; Pengfei Liu; Feng Zhang; Claudia M B Carvalho; Charles F Towne; Sat Dev Batish; James R Lupski Journal: Genet Med Date: 2011-06 Impact factor: 8.822
Authors: Christian Beetz; Thomas R Pieber; Nicole Hertel; Maria Schabhüttl; Carina Fischer; Slave Trajanoski; Elisabeth Graf; Silke Keiner; Ingo Kurth; Thomas Wieland; Rita-Eva Varga; Vincent Timmerman; Mary M Reilly; Tim M Strom; Michaela Auer-Grumbach Journal: Am J Hum Genet Date: 2012-06-14 Impact factor: 11.025
Authors: Christian G Bouwkamp; Zaid Afawi; Aviva Fattal-Valevski; Inge E Krabbendam; Stefano Rivetti; Rafik Masalha; Marialuisa Quadri; Guido J Breedveld; Hanna Mandel; Muhammad Abu Tailakh; H Berna Beverloo; Giovanni Stevanin; Alexis Brice; Wilfred F J van IJcken; Meike W Vernooij; Amalia M Dolga; Femke M S de Vrij; Vincenzo Bonifati; Steven A Kushner Journal: Neurol Genet Date: 2018-03-21