Spastic paraplegia type 4: a novel SPAST splice site donor mutation and expansion of the phenotype variability

A. Orlacchio, C. Montecchiani, R. Miyamoto, M. Mearini, L. D'Onofrio, M. Miele, F. Gaudiello, Y. Izumi, C. Caltagirone, R. Kaji, T. Kawarai (Rome, Italy)

Meeting: 2017 International Congress

Abstract Number: 453

Keywords: Spasticity: Clinical features, Spasticity: Etiology and Pathogenesis, Spasticity: Genetics

Session Information

Date: Tuesday, June 6, 2017

Session Title: Genetics (Non-PD)

Session Time: 1:45pm-3:15pm

Location: Exhibit Hall C

Objective: The aim of this study is to reveal molecular pathogenicity and genotype-phenotype correlations in spastic paraplegia type 4 (SPG4).

Background: Mutations in SPG4/SPAST represent the most frequent molecular etiology in an autosomal dominant form of Hereditary Spastic Paraplegia (HSP). Previous studies demonstrated various molecular pathogenesis in SPG, including loss-of-function, haploinsufficiency, dominant-negative effect, and dysregulation of microtubule-severing activity.

Methods: A cohort of patients with spastic paraplegia recruited in Italy and Japan was investigated clinically and genetically. Initial diagnostic approach included targeted resequencing of currently-known HSP genes or resequencing of whole exomes. Biological effects by nucleotide variation were predicted using bioinformatic tools and confirmed by reverse transcription polymerase chain reaction (RT-PCR) experiment. Measurement of SPG4 transcripts were conducted in cultured T cells treated with nonsense pre-mRNA mediated decay (NMD) inhibitor.

Results: A novel SPAST intronic variation was found in two families, one from Italy and the other from Japan. The variant is located at the third position at 5′-splice-site of intron 6, c.1004+3A>C. RNA secondary structure seems to remain unchanged by the variant; however, skipping of exon 6 was shown by RT-PCR experiment, presumably leading to generation of frame shifts and premature stop codons (p.Gly290Trpfs*5). Measurement of SPAST transcripts in lymphocytes demonstrated a reduction through NMD. Intra- and inter-familial phenotypic variations were observed, including age-at-onset, severity of spasticity, as well as scoliosis.

Conclusions: Our study demonstrated further evidence of allelic heterogeneity in SPG4, dosage effects through NMD, and broad clinical features of SPAST mutation.

References: 1. Lo Giudice T, Lombardi F, Santorelli FM, Kawarai T, Orlacchio A. 2014. Hereditary spastic paraplegia: clinical-genetic characteristics and evolving molecular mechanisms. Exp Neurol. 261: 518-539.

2. Orlacchio A, Kawarai T, Totaro A, Errico A, St George-Hyslop PH, Rugarli EI, Bernardi G. 2004. Hereditary spastic paraplegia: clinical genetic study of 15 families. Arch Neurol. 61(6): 849-855.

To cite this abstract in AMA style:

A. Orlacchio, C. Montecchiani, R. Miyamoto, M. Mearini, L. D'Onofrio, M. Miele, F. Gaudiello, Y. Izumi, C. Caltagirone, R. Kaji, T. Kawarai. Spastic paraplegia type 4: a novel SPAST splice site donor mutation and expansion of the phenotype variability [abstract]. Mov Disord. 2017; 32 (suppl 2). https://www.mdsabstracts.org/abstract/spastic-paraplegia-type-4-a-novel-spast-splice-site-donor-mutation-and-expansion-of-the-phenotype-variability/. Accessed June 15, 2025.

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