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DOI: 10.1055/s-0044-1788729
Early Diagnosis of AP5Z1/SPG48 Spastic Paraplegia: Case Report and Review of the Literature
Autoren
Funding This research was supported in part by 2023 RC 5 × 1000, RF-2019–12370112 (to A.T.), and Ministero della Salute Grant SG-2021–12375552 (to S.M.).
Abstract
Hereditary spastic paraplegias (HSPs) are a genetically heterogeneous group of neurodegenerative disorders clinically characterized by progressive lower limb spasticity with pyramidal weakness. Around a dozen potential molecular mechanisms are recognized. Childhood HSP is a significant diagnostic challenge in clinical practice. Mutations in AP5Z1, which are associated with spastic paraplegia type 48 (SPG48), are extremely rare and seldom described in children.
We report the clinical, radiologic, and molecular studies performed in a child harboring novel biallelic mutations in AP5Z1.
The child presented a neurodevelopmental disorder with slight lower limb pyramidal signs. Brain magnetic resonance imaging (MRI) showed minimal white matter changes in the frontal horns of the lateral ventricles and a normally shaped corpus callosum. Western blotting in cultured skin fibroblasts indicated reduced protein expression, which confirmed the genetic diagnosis and framed this as a case of protein reduction in a context of impaired autophagy.
Our findings expand the spectrum of phenotypes associated with mutations in AP5Z1, highlighting their clinical and pathophysiologic overlap with lysosomal storage disorders. SPG48 should be considered in the differential diagnosis of neurodevelopmental disorders even when pyramidal signs are minimal and brain MRI not fully informative.
Publikationsverlauf
Eingereicht: 23. April 2024
Angenommen: 10. Juli 2024
Artikel online veröffentlicht:
26. Juli 2024
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References
- 1 Bellofatto M, De Michele G, Iovino A, Filla A, Santorelli FM. Management of hereditary spastic paraplegia: a systematic review of the literature. Front Neurol 2019; 10: 3
- 2 Khundadze M, Ribaudo F, Hussain A. et al. A mouse model for SPG48 reveals a block of autophagic flux upon disruption of adaptor protein complex five. Neurobiol Dis 2019; 127: 419-431
- 3 Hirst J, Hesketh GG, Gingras AC, Robinson MS. Rag GTPases and phosphatidylinositol 3-phosphate mediate recruitment of the AP-5/SPG11/SPG15 complex. J Cell Biol 2021; 220 (02) e202002075
- 4 Renaud F, Béliveau MJ, Akzam-Ouellette MA, Jauvin K, Labelle F. Comparison of the Wechsler Preschool and Primary Scale of Intelligence-Third Edition and the Leiter-R Intellectual Assessments for Clinic-Referred Children. J Psychoed Assess 2022; 40 (07) 825-838
- 5 Mozzanica F, Salvadorini R, Sai E. et al. Reliability, validity and normative data of the Italian version of the Bus Story test. Int J Pediatr Otorhinolaryngol 2016; 89: 17-24
- 6 Schüle R, Holland-Letz T, Klimpe S. et al. The Spastic Paraplegia Rating Scale (SPRS): a reliable and valid measure of disease severity. Neurology 2006; 67 (03) 430-434
- 7 Dosi C, Galatolo D, Rubegni A. et al. Expanding the clinical and genetic heterogeneity of SPAX5. Ann Clin Transl Neurol 2020; 7 (04) 595-601
- 8 Kircher M, Witten DM, Jain P, O'Roak BJ, Cooper GM, Shendure J. A general framework for estimating the relative pathogenicity of human genetic variants. Nat Genet 2014; 46 (03) 310-315
- 9 Ioannidis NM, Rothstein JH, Pejaver V. et al. REVEL: an ensemble method for predicting the pathogenicity of rare missense variants. Am J Hum Genet 2016; 99 (04) 877-885
- 10 Wesselborg S, Stork B. Autophagy signal transduction by ATG proteins: from hierarchies to networks. Cell Mol Life Sci 2015; 72 (24) 4721-4757
- 11 Garver WS, Heidenreich RA, Erickson RP, Thomas MA, Wilson JM. Localization of the murine Niemann-Pick C1 protein to two distinct intracellular compartments. J Lipid Res 2000; 41 (05) 673-687
- 12 Alecu JE, Saffari A, Ziegler M. et al. Plasma neurofilament light chain is elevated in adaptor protein complex 4–related hereditary spastic paraplegia. Mov Disord 2023; 38 (09) 1742-1750
- 13 Hirst J, Irving C, Borner GHH. Adaptor protein complexes AP-4 and AP-5: new players in endosomal trafficking and progressive spastic paraplegia. Traffic 2013; 14 (02) 153-164
- 14 Davies AK, Itzhak DN, Edgar JR. et al. AP-4 vesicles contribute to spatial control of autophagy via RUSC-dependent peripheral delivery of ATG9A. Nat Commun 2018; 9 (01) 3958
- 15 Saffari A, Brechmann B, Böger C. et al. High-content screening identifies a small molecule that restores AP-4-dependent protein trafficking in neuronal models of AP-4-associated hereditary spastic paraplegia. Nat Commun 2024; 15 (01) 584
- 16 Słabicki M, Theis M, Krastev DB. et al. A genome-scale DNA repair RNAi screen identifies SPG48 as a novel gene associated with hereditary spastic paraplegia. PLoS Biol 2010; 8 (06) e1000408
- 17 Pensato V, Castellotti B, Gellera C. et al. Overlapping phenotypes in complex spastic paraplegias SPG11, SPG15, SPG35 and SPG48. Brain 2014; 137 (Pt 7): 1907-1920
- 18 Schlipf NA, Schüle R, Klimpe S. et al. AP5Z1/SPG48 frequency in autosomal recessive and sporadic spastic paraplegia. Mol Genet Genomic Med 2014; 2 (05) 379-382
- 19 Hirst J, Madeo M, Smets K. et al. Complicated spastic paraplegia in patients with AP5Z1 mutations (SPG48). Neurol Genet 2016; 2 (05) e98
- 20 D'Amore A, Tessa A, Casali C. et al. Next generation molecular diagnosis of hereditary spastic paraplegias: an Italian cross-sectional study. Front Neurol 2018; 9: 981
- 21 Wei Q, Dong HL, Pan LY. et al. Clinical features and genetic spectrum in Chinese patients with recessive hereditary spastic paraplegia. Transl Neurodegener 2019; 8: 19
- 22 Maruta K, Ando M, Otomo T, Takashima H. A case of spastic paraplegia 48 with a novel mutation in the AP5Z1 gene [in Japanese]. Rinsho Shinkeigaku 2020; 60 (08) 543-548
- 23 Jin P, Wang Y, Nian N, Wang GQ, Fu XM. Hereditary spastic paraplegia (SPG 48) with deafness and azoospermia: a case report. Front Neurol 2023; 14: 1156100