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Journal of Pediatric Neurology 2022; 20(03): 235-236
DOI: 10.1055/s-0041-1732483
Letter to the Editor

Spastic Paraplegia Type 57: A Cerebral Palsy Mimic

Silvia Beatriz Sánchez Marco
1   Department of Paediatric Neurology, Hospital Infantil Universitario Miguel Servet, Zaragoza, Spain
,
José Luis Peña Segura
1   Department of Paediatric Neurology, Hospital Infantil Universitario Miguel Servet, Zaragoza, Spain
,
Amparo López Lafuente
1   Department of Paediatric Neurology, Hospital Infantil Universitario Miguel Servet, Zaragoza, Spain
,
Javier López Pisón
1   Department of Paediatric Neurology, Hospital Infantil Universitario Miguel Servet, Zaragoza, Spain
,
Miguel Lafuente Hidalgo
1   Department of Paediatric Neurology, Hospital Infantil Universitario Miguel Servet, Zaragoza, Spain
,
Raquel Pérez Delgado
1   Department of Paediatric Neurology, Hospital Infantil Universitario Miguel Servet, Zaragoza, Spain
› Author Affiliations Funding None.
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Hereditary spastic paraplegias (HSP) are a heterogeneous group of gait disorders, which caused by a distal neuropathy of the longest corticospinal tract axons; ascending fibers are also often involved.[1] [2]

HSP can be associated with autosomal dominant or recessive inheritance patterns, and more than 67 HSP genes are currently known to date.[3]

Clinical features of HSP include weakness and spasticity of the lower extremities. HSP can be classified as pure (uncomplicated) or complex according to the absence or presence of additional neurological and non-neurological manifestations, including polyneuropathy, amyotrophy, optic and cerebellar atrophy, cognitive impairment, and epilepsy and neuroradiology findings such as thinning of the corpus callosum and skeletal abnormalities.[3]

Spastic paraplegia type 57 (SPG57) is an extremely rare cause of HSP. This condition has been associated with homozygous mutations of the TFG gene (3q12.2) encoding protein TFG, which is a highly conserved regulator of protein secretion and functions at the interface between the endoplasmic reticulum (ER) and ER-Golgi intermediate compartments. The transmission pattern of SPG57 is autosomal recessive.[4]

SPG57 is clinically characterized by profound lower limb spasticity (inability to walk independently), hyperreflexia, and may include optic atrophy, demyelinating sensorimotor neuropathy, urinary incontinence, and thinning of the corpus callosum. Few affected families have been described worldwide.[4] [5] We present a new case of SPG57.

A 14-year-old boy presented at 10 months of age with a history of spastic tetraplegia and a presumed diagnosis of cerebral palsy. He is the second child of non-consanguineous parents. He was born at full term following an uneventful pregnancy and delivery. His older sister has a diagnosis of incontinentia pigmenti, resulting from a de novo mutation causing exon 4 to 10 deletion of the inhibitor of kappa light polypeptide gene enhancer in B-cells, kinase gamma (IKBKG) gene (MIM 300248).

The patient never achieved the ability to sit, stand, or walk independently. His neurological examination revealed axial weakness and spastic tetraplegia; the spasticity was more prominent in the lower than upper extremities. The patient presented generalised spikes and waves in the EEG, but without 3 hz amplitude. Therefore, categorize these episodes as typical absence seizures would be inaccurate. He began treatment with valproic acid, which was withdrawn after 2 years without further seizures. He achieved bowel and bladder control at 3 years of age but developed urinary retention by age five, which required bladder catheterization. At 6 years of age, he developed both bowel and bladder incontinence. His ophthalmology exam showed a progressive papilla excavation with temporal optic disc pallor. He was diagnosed with severe optic atrophy at the age of 13. His spasticity was progressive over time and required treatment with botulinum toxin and physiotherapy.

Several neurometabolic investigations were repeatedly normal. Nerve conduction studies demonstrated a chronic neurogenic pattern with mild demyelination. Magnetic resonance imaging of the brain showed thinning of the corpus callosum, white matter periventricular hyperintensities, and frontal horn asymmetry ([Fig. 1]). His muscle biopsy was normal. Genetic testing with karyotype and Array CGH were normal.

Zoom Image
Fig. 1 Brain magnetic resonance imaging findings. (A) Thinning of the corpus callosum. (B) Mild periventricular hyperintensities with frontal horn asymmetry.

At the age of 15 years, clinical whole exome sequencing identified homozygous likely pathogenic recessive missense mutations involving exon 2 of the TFG gene; (NM_001195478.1):c.65G > A (p.Arg22Gln), associated with spastic paraplegia type 57 (SPG57). Genetic targeted testing showed a heterozygous mutation in the same gene in both parents and his sister.

Spastic paraplegia type 57 is a rare condition,[6] with an autosomal recessive inheritance pattern and progressive pyramidal tract involvement with an early onset and a variable degree of motor neuronal demyelination in addition to motor axonal degeneration.[5] [6] Brain MRI changes may include thinning of the corpus callosum, white matter hyperintensities, and cerebellar atrophy.[4] [5] Clinical exome sequencing has helped identify several genetic etiologies for cerebral palsy with a diagnostic yield that exceeds 50%. Therefore, some authors have suggested the next-generation sequencing first-line for diagnosis in cases of cryptogenic cerebral palsy.[7] Diagnosis of these conditions gives a better understanding of the disease, prognosis, and anticipated complications. It also offers to families the possibility of genetic counseling to assist with family planning.

In our patient, the progressive evolution of his condition, the presentation of new symptoms such as optic atrophy, polyneuropathy, loss of bladder and bowel control, and brain MRI findings (thinning of the corpus callosum), prompted a thorough investigation to determine the etiology. We present a rare type of HSP mimicking cerebral palsy.

Note

The procedures employed were reviewed and approved by the appropriate institutional review committee.




Publication History

Received: 19 April 2021

Accepted: 09 June 2021

Article published online:
23 July 2021

© 2021. Thieme. All rights reserved.

Georg Thieme Verlag KG
Rüdigerstraße 14, 70469 Stuttgart, Germany

 

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