Your search keyword '"FAMILIAL spastic paraplegia"' showing total 154 results

1. A Homoplasmic MT‐TV Mutation Associated with Mitochondrial Inheritance of Hereditary Spastic Paraplegia.

Author

Shi, Yan, Xie, Junhao, Jiang, Junyi, Yan, Xinyu, Chen, Xuejiao, Hong, Shunyan, Liu, Jiyuan, Xu, Guorong, Su, Huizhen, Chen, Wanjin, Wang, Ning, and Lin, Xiang

Subjects

*GENETIC testing, *FAMILIAL spastic paraplegia, *MITOCHONDRIAL DNA, *PERONEAL nerve, *PHENOTYPES, *MOVEMENT disorders

Abstract

Background Objectives Methods Results Conclusions Hereditary spastic paraplegia (HSP) is characterized by progressive lower limb weakness and spasticity, with unknown genetic cause in many cases.To identify novel genetic causes of HSP.Phenotypic characterization, genetic screening, transcriptome sequencing, and peroneal nerve biopsy were conducted in a Chinese HSP family.We found a homoplasmic MT‐TV (mitochondrial tRNAVal) mutation, m.1661A > G, present in all affected individuals across four generations of a family with complex HSP. Fourth‐generation affected individuals displayed earlier onset, likely due to presumptive anticipation, and greater symptom severity, potentially caused by decreased mitochondrial DNA (mtDNA) copy number. Upregulation of mitochondrial autophagy genes in these patients suggested that MT‐TV mutations could lead to reduced mtDNA copy number. Neural biopsies revealed ultrastructural abnormalities in myelin and mitochondria.The rare MT‐TV m.1661A > G mutation is associated with HSP. Variations in mtDNA copy number may play a causal role in differences among clinical phenotypes. © 2024 International Parkinson and Movement Disorder Society. [ABSTRACT FROM AUTHOR]

Published

2024

2. Expanding SPG18 clinical spectrum: autosomal dominant mutation causes complicated hereditary spastic paraplegia in a large family.

Author

Trinchillo, Assunta, Valente, Valeria, Esposito, Marcello, Migliaccio, Miriana, Iovino, Aniello, Picciocchi, Michele, Cuomo, Nunzia, Caccavale, Carmela, Nocerino, Cristofaro, De Rosa, Laura, Salvatore, Elena, Pierantoni, Giovanna Maria, Menchise, Valeria, Paladino, Simona, and Criscuolo, Chiara

Subjects

*AMYOTROPHIC lateral sclerosis, *LIPID rafts, *TEMPORAL lobe epilepsy, *ENDOPLASMIC reticulum, *FAMILIAL spastic paraplegia, *PHENOTYPES

Abstract

Background: SPG18 is caused by mutations in the endoplasmic reticulum lipid raft associated 2 (ERLIN2) gene. Autosomal recessive (AR) mutations are usually associated with complicated hereditary spastic paraplegia (HSP), while autosomal dominant (AD) mutations use to cause pure SPG18. Aim: To define the variegate clinical spectrum of the SPG18 and to evaluate a dominant negative effect of erlin2 (encoded by ERLIN2) on oligomerization as causing differences between AR and AD phenotypes. Methods: In a four-generation pedigree with an AD pattern, a spastic paraplegia multigene panel test was performed. Oligomerization of erlin2 was analyzed with velocity gradient assay in fibroblasts of the proband and healthy subjects. Results: Despite the common p.V168M mutation identified in ERLIN2, a phenoconversion to amyotrophic lateral sclerosis (ALS) was observed in the second generation, pure HSP in the third generation, and a complicated form with psychomotor delay and epilepsy in the fourth generation. Erlin2 oligomerization was found to be normal. Discussion: We report the first AD SPG18 family with a complicated phenotype, and we ruled out a dominant negative effect of V168M on erlin2 oligomerization. Therefore, our data do not support the hypothesis of a relationship between the mode of inheritance and the phenotype, but confirm the multifaceted nature of SPG18 on both genetic and clinical point of view. Clinicians should be aware of the importance of conducting an in-depth clinical evaluation to unmask all the possible manifestations associated to an only apparently pure SPG18 phenotype. We confirm the genotype–phenotype correlation between V168M and ALS emphasizing the value of close follow-up. [ABSTRACT FROM AUTHOR]

Published

2024

3. Novel ERLIN2 variant expands the phenotype of Spastic Paraplegia 18.

Author

de Souza, Guilherme Carvalho, Malta, Maria Carolina, Santos, Mirele Raíssa Silva, Fontes, Marshall Ítalo Barros, de Sousa Anjos, Juliana Lopes, Ribeiro, Diego Patrício, Kok, Fernando, and Figueiredo, Thalita

Subjects

*PARAPLEGIA, *FAMILIAL spastic paraplegia, *MEDICAL genetics, *PHENOTYPES, *CONSANGUINITY, *GENETIC disorders

Abstract

Background: The Brazilian Northeast region is notable for its high prevalence of consanguineous marriages and isolated populations, which has led to a significant prevalence of rare genetic disorders. This study describes the clinical presentation of four affected individuals from the same family, comprising two siblings and their cousins, with ages ranging from 11 to 20 years. Methods: In a small and isolated community in Northeastern Brazil, affected individuals initially underwent a clinical assessment. Subsequently, written consent was obtained from their legal guardians, and an extensive clinical evaluation was conducted at a medical genetics center. Family data provided the basis for constructing the pedigree, and biological samples (blood or oral swabs) were collected from both affected and unaffected family members. Following informed consent from one patient, Whole Exome Sequencing (WES) was carried out, encompassing exome sequencing, assembly, genotyping, and annotation. A potentially deleterious variant was then singled out for further segregation analysis through Sanger Sequencing, involving both the proband and select family members. Results and conclusion: These individuals exhibit severe neurodevelopmental delays, encompassing symptoms such as spastic paraplegia, neuropathy, intellectual impairments, and language challenges. Through next-generation sequencing (NGS) techniques, a previously unreported homozygous variant within the ERLIN2 gene linked to spastic paraplegia 18 (SPG18) was identified across all four patients. Also, all patients displayed childhood cataract, expanding the known clinical spectrum of SPG18. [ABSTRACT FROM AUTHOR]

Published

2024

4. POLR3A-related disorders: expanding the clinical phenotype.

Author

McKenna, Mary Clare, O'Connor, Antoinette, Lockhart, Andrew, Bogdanova-Mihaylova, Petya, Brett, Francesca, Langan, Yvonne, Meaney, James, Costigan, Donal, Doherty, Colin P., Bede, Peter, Murphy, Sinéad M., and Hutchinson, Siobhán

Subjects

*PHENOTYPES, *SPINOCEREBELLAR ataxia, *FRIEDREICH'S ataxia, *MOTOR unit, *FAMILIAL spastic paraplegia, *MEDICAL genetics, *LEG pain

Abstract

This article discusses POLR3A-related disorders, which encompass a range of clinical phenotypes beyond the classical triad of hypomyelinating leukodystrophy, hypodontia, and hypogonadotrophic hypogonadism. The case study presented focuses on a 46-year-old woman with walking difficulties, lower limb pain, weakness, and stiffness. The patient exhibited various neurological symptoms, including a waddling gait, dystonic posturing of the feet, and head tremors. The article highlights the importance of considering POLR3A-related disorders in the differential diagnosis of spastic or cerebellar ataxias in adolescents and adults. [Extracted from the article]

Published

2024

5. Biallelic variants in the COQ4 gene caused hereditary spastic paraplegia predominant phenotype.

Author

Wei, Qiao, Yu, Hao, Wang, Pei‐Shan, Xie, Juan‐Juan, Dong, Hai‐Lin, Wu, Zhi‐Ying, and Li, Hong‐Fu

Subjects

*FAMILIAL spastic paraplegia, *PHENOTYPES, *GENETIC variation, *MOTOR neurons, *UBIQUINONES

Abstract

Introduction: Hereditary spastic paraplegias (HSPs) comprise a group of neurodegenerative disorders characterized by progressive degeneration of upper motor neurons. Homozygous or compound heterozygous variants in COQ4 have been reported to cause primary CoQ10 deficiency‐7 (COQ10D7), which is a mitochondrial disease. Aims: We aimed to screened COQ4 variants in a cohort of HSP patients. Methods: A total of 87 genetically unidentified HSP index patients and their available family members were recruited. Whole exome sequencing (WES) was performed in all probands. Functional studies were performed to identify the pathogenicity of those uncertain significance variants. Results: In this study, five different COQ4 variants were identified in three Chinese HSP pedigrees and two variants were novel, c.87dupT (p.Arg30*), c.304C>T (p.Arg102Cys). More importantly, we firstly described two early‐onset pure HSP caused by COQ4 variants. Functional studies in patient‐derived fibroblast lines revealed a reduction cellular CoQ10 levels and the abnormal mitochondrial structure. Conclusions: Our findings revealed that bilateral variants in the COQ4 gene caused HSP predominant phenotype, expanding the phenotypic spectrum of the COQ4‐related disorders. [ABSTRACT FROM AUTHOR]

Published

2024

6. Functional Characteristics of the Nav1.1 p.Arg1596Cys Mutation Associated with Varying Severity of Epilepsy Phenotypes.

Author

Witkowski, Grzegorz, Szulczyk, Bartlomiej, Nurowska, Ewa, Jurek, Marta, Pasierski, Michal, Lipiec, Agata, Charzewska, Agnieszka, Dawidziuk, Mateusz, Milewski, Michal, Owsiak, Szymon, Rola, Rafal, Sienkiewicz Jarosz, Halina, and Hoffman-Zacharska, Dorota

Subjects

*SODIUM channels, *PHENOTYPES, *EPILEPSY, *MOTOR neurons, *GENETIC mutation, *FEBRILE seizures, *FAMILIAL spastic paraplegia

Abstract

Mutations of the SCN1A gene, which encodes the voltage-dependent Na+ channel's α subunit, are associated with diverse epileptic syndromes ranging in severity, even intra-family, from febrile seizures to epileptic encephalopathy. The underlying cause of this variability is unknown, suggesting the involvement of additional factors. The aim of our study was to describe the properties of mutated channels and investigate genetic causes for clinical syndromes' variability in the family of five SCN1A gene p.Arg1596Cys mutation carriers. The analysis of additional genetic factors influencing SCN1A-associated phenotypes was conducted through exome sequencing (WES). To assess the impact of mutations, we used patch clamp analysis of mutated channels expressed in HEK cells and in vivo neural excitability studies (NESs). In cells expressing the mutant channel, sodium currents were reduced. NESs indicated increased excitability of peripheral motor neurons in mutation carriers. WES showed the absence of non-SCA1 pathogenic variants that could be causative of disease in the family. Variants of uncertain significance in three genes, as potential modifiers of the most severe phenotype, were identified. The p.Arg1596Cys substitution inhibits channel function, affecting steady-state inactivation kinetics. Its clinical manifestations involve not only epileptic symptoms but also increased excitability of peripheral motor fibers. The role of Nav1.1 in excitatory neurons cannot be ruled out as a significant factor of the clinical phenotype. [ABSTRACT FROM AUTHOR]

Published

2024

7. Congenital Myopathy as a Phenotypic Expression of CACNA1S Gene Mutation: Case Report and Systematic Review of the Literature.

Author

Marinella, Gemma, Orsini, Alessandro, Scacciati, Massimo, Costa, Elisa, Santangelo, Andrea, Astrea, Guja, Frosini, Silvia, Pasquariello, Rosa, Rubegni, Anna, Sgherri, Giada, Corsi, Martina, Bonuccelli, Alice, and Battini, Roberta

Subjects

*FAMILIAL spastic paraplegia, *NEMALINE myopathy, *GENETIC mutation, *MUSCLE diseases, *GENE expression, *SENSORINEURAL hearing loss, *PHENOTYPES, *AGENESIS of corpus callosum

Abstract

Background: Congenital myopathies are a group of clinically, genetically, and histologically heterogeneous diseases caused by mutations in a large group of genes. One of these is CACNA1S, which is recognized as the cause of Dihydropyridine Receptor Congenital Myopathy. Methods: To better characterize the phenotypic spectrum of CACNA1S myopathy, we conducted a systematic review of cases in the literature through three electronic databases following the PRISMA guidelines. We selected nine articles describing 23 patients with heterozygous, homozygous, or compound heterozygous mutations in CACNA1S and we added one patient with a compound heterozygous mutation in CACNA1S (c.1394-2A>G; c.1724T>C, p.L575P) followed at our Institute. We collected clinical and genetic data, muscle biopsies, and muscle MRIs when available. Results: The phenotype of this myopathy is heterogeneous, ranging from more severe forms with a lethal early onset and mild–moderate forms with a better clinical course. Conclusions: Our patient presented a phenotype compatible with the mild–moderate form, although she presented peculiar features such as a short stature, myopia, mild sensorineural hearing loss, psychiatric symptoms, and posterior-anterior impairment gradient on thigh muscle MRI. [ABSTRACT FROM AUTHOR]

Published

2023

8. The phenotypic spectrum of pathogenic ATP1A1 variants expands: the novel p.P600R substitution causes demyelinating Charcot–Marie–Tooth disease.

Author

Cinarli Yuksel, Feride, Nicolaou, Paschalis, Spontarelli, Kerri, Dohrn, Maike F., Rebelo, Adriana P., Koutsou, Pantelitsa, Georghiou, Anthi, Artigas, Pablo, Züchner, Stephan L., Kleopa, Kleopas A., and Christodoulou, Kyproula

Subjects

*CHARCOT-Marie-Tooth disease, *DEMYELINATION, *PHENOTYPES, *OUABAIN, *FAMILIAL spastic paraplegia, *PERIPHERAL neuropathy

Abstract

Background: Charcot–Marie–Tooth disease (CMT) is a genetically and clinically heterogeneous group of inherited neuropathies. Monoallelic pathogenic variants in ATP1A1 were associated with axonal and intermediate CMT. ATP1A1 encodes for the catalytic α1 subunit of the Na+/ K+ ATPase. Besides neuropathy, other associated phenotypes are spastic paraplegia, intellectual disability, and renal hypomagnesemia. We hereby report the first demyelinating CMT case due to a novel ATP1A1 variant. Methods: Whole-exome sequencing on the patient's genomic DNA and Sanger sequencing to validate and confirm the segregation of the identified p.P600R ATP1A1 variation were performed. To evaluate functional effects, blood-derived mRNA and protein levels of ATP1A1 and the auxiliary β1 subunit encoded by ATP1B1 were investigated. The ouabain-survival assay was performed in transfected HEK cells to assess cell viability, and two-electrode voltage clamp studies were performed in Xenopus oocytes. Results: The variant was absent in the local and global control datasets, falls within a highly conserved protein position, and is in a missense-constrained region. The expression levels of ATP1A1 and ATP1B1 were significantly reduced in the patient compared to healthy controls. Electrophysiology indicated that ATP1A1p.P600R injected Xenopus oocytes have reduced Na+/ K+ ATPase function. Moreover, HEK cells transfected with a construct encoding ATP1A1p.P600R harbouring variants that confers ouabain insensitivity displayed a significant decrease in cell viability after ouabain treatment compared to the wild type, further supporting the pathogenicity of this variant. Conclusion: Our results further confirm the causative role of ATP1A1 in peripheral neuropathy and broaden the mutational and phenotypic spectrum of ATP1A1-associated CMT. [ABSTRACT FROM AUTHOR]

Published

2023

9. NMNAT1 and hereditary spastic paraplegia (HSP): expanding the phenotypic spectrum of NMNAT1 variants.

Author

Sadr, Zahra, Ghasemi, Aida, Rohani, Mohammad, and Alavi, Afagh

Subjects

*SCHOENLEIN-Henoch purpura, *PHENOTYPES, *FAMILIAL spastic paraplegia, *NEUROLOGICAL disorders, *SYMPTOMS

Abstract

• NMNAT1 , a key enzyme for NAD+ synthesis , roles in the maintenance of NAD homeostasis of neurons. • Mutations in NMNAT1 cause syndromic and non-syndromic Leber congenital amaurosis-type 9 (LCA9). • For the first time, a probable association between a NMNAT1 variant and HSP disease is detected. • It seems NMNAT1 mutations can present phenotypic heterogeneity. • Phenotypic heterogeneity has already been reported in HSP cases with mutations in other genes. In the NAD biosynthetic network, the nicotinamide mononucleotide adenylyltransferase (NMNAT) enzyme fuels NAD as a co-substrate for a group of enzymes. Mutations in the nuclear-specific isoform, NMNAT1 , have been extensively reported as the cause of Leber congenital amaurosis-type 9 (LCA9). However, there are no reports of NMNAT1 mutations causing neurological disorders by disrupting the maintenance of physiological NAD homeostasis in other types of neurons. In this study, for the first time, the potential association between a NMNAT1 variant and hereditary spastic paraplegia (HSP) is described. Whole-exome sequencing was performed for two affected siblings diagnosed with HSP. Runs of homozygosity (ROH) were detected. The shared variants of the siblings located in the homozygosity blocks were selected. The candidate variant was amplified and Sanger sequenced in the proband and other family members. Homozygous variant c.769G> A :p.(Glu257Lys) in NMNAT1 , the most common variant of NMNAT1 in LCA9 patients, located in the ROH of chromosome 1, was detected as a probable disease-causing variant. After detection of the variant in NMNAT1 , as a LCA9-causative gene, ophthalmological and neurological re-evaluations were performed. No ophthalmological abnormality was detected and the clinical manifestations of these patients were completely consistent with pure HSP. No NMNAT1 variant had ever been previously reported in HSP patients. However, NMNAT1 variants have been reported in a syndromic form of LCA which is associated with ataxia. In conclusion, our patients expand the clinical spectrum of NMNAT1 variants and represent the first evidence of the probable correlation between NMNAT1 variants and HSP. [ABSTRACT FROM AUTHOR]

Published

2023

10. Novel phenotype with prominent cerebellar oculomotor dysfunction in spastic paraplegia type 39.

Author

Viertauer, Sebastian, Kurth, Ingo, Eggermann, Katja, and Eggers, Christian

Subjects

*FAMILIAL spastic paraplegia, *PARAPLEGIA, *PHENOTYPES, *MOVEMENT disorders, *POTASSIUM antagonists, *NEUROLOGICAL disorders

Abstract

Objectives: The term hereditary spastic paraplegia comprises an ever-expanding array of neurological disorders with distinct aetiologies. Spastic paraplegia gene 39 is one of the many genetically defined types with features of other organs and neurological systems in addition to paraspasticity. We describe a large kindred with a novel clinical phenotype as, in addition to spastic paraplegia, affected subjects suffered from a prominent cerebellar oculomotor dysfunction with two hitherto undescribed mutations of PNPLA6. Methods: Three of five genetically tested family members of a large kindred were affected by spastic gait and a unique and prominent cerebellar oculomotor dysfunction. Further clinical, imaging, laboratory and videonystagmographic data were analyzed. Genetic analysis was done using next-generation sequencing. Results: The most salient clinical feature, in addition to paraspasticity, in three of five subjects was cerebellar oculomotor dysfunction with an upbeating nystagmus provoked by downward gaze. Genetic analysis revealed two hitherto unknown sequence variants in the PNPLA6 gene, a splice-site variant c.1635 + 3G > T and a missense variant c.3401A > T, p.(Asp1134Val). In addition to cerebellar oculomotor dysfunction, compound-heterozygous siblings presented with paraspasticity and a moderate hypogonadotropic hypogonadism in the female. A paternal uncle being homozygous for the splice-site variant of PNPLA6 presented with increased lower limb reflexes and an unstable gait. Treatment with 4-aminopyridine, a potassium channel blocker, lead to meaningful improvement of clinical symptoms. Conclusions: The unique and prominent cerebellar ocular motor disorder in our family broadens the spectrum of clinical phenotypes associated with variations in the PNLA6 gene. The finding of paraspasticity with cerebellar oculomotor dysfunction alongside inconspicuous brainstem imaging may raise suspicion of complex HSP with PNPLA6 mutations. [ABSTRACT FROM AUTHOR]

Published

2022

11. Phenotypic continuum of NFU1‐related disorders.

Author

Kaiyrzhanov, Rauan, Zaki, Maha S., Lau, Tracy, Sen, Sambuddha, Azizimalamiri, Reza, Zamani, Mina, Sayin, Gözde Yeşil, Hilander, Taru, Efthymiou, Stephanie, Chelban, Viorica, Brown, Ruth, Thompson, Kyle, Scarano, Maria Irene, Ganesh, Jaya, Koneev, Kairgali, Gülaçar, Ismail Musab, Person, Richard, Sadykova, Dinara, Maidyrov, Yerdan, and Seifi, Tahereh

Subjects

*FAMILIAL spastic paraplegia, *PHENOTYPES, *LEUKOENCEPHALOPATHIES, *MISSENSE mutation, *WHITE matter (Nerve tissue)

Abstract

Bi‐allelic variants in Iron–Sulfur Cluster Scaffold (NFU1) have previously been associated with multiple mitochondrial dysfunctions syndrome 1 (MMDS1) characterized by early‐onset rapidly fatal leukoencephalopathy. We report 19 affected individuals from 10 independent families with ultra‐rare bi‐allelic NFU1 missense variants associated with a spectrum of early‐onset pure to complex hereditary spastic paraplegia (HSP) phenotype with a longer survival (16/19) on one end and neurodevelopmental delay with severe hypotonia (3/19) on the other. Reversible or irreversible neurological decompensation after a febrile illness was common in the cohort, and there were invariable white matter abnormalities on neuroimaging. The study suggests that MMDS1 and HSP could be the two ends of the NFU1‐related phenotypic continuum. [ABSTRACT FROM AUTHOR]

Published

2022

12. Phenotypic and Genetic Heterogeneity of Adult Patients with Hereditary Spastic Paraplegia from Serbia.

Author

Perić, Stojan, Marković, Vladana, Candayan, Ayşe, De Vriendt, Els, Momčilović, Nikola, Savić, Andrija, Dragašević-Mišković, Nataša, Svetel, Marina, Stević, Zorica, Božović, Ivo, Mesaroš, Šarlota, Drulović, Jelena, Basta, Ivana, Petrović, Igor, Tamaš, Olivera, Mijajlović, Milija, Novaković, Ivana, Sokić, Dragoslav, and Jordanova, Albena

Subjects

*RECESSIVE genes, *GENETIC epidemiology, *FAMILIAL spastic paraplegia, *PHENOTYPES, *ADULTS, *MOLECULAR diagnosis, *HETEROGENEITY

Abstract

Hereditary spastic paraplegia (HSP) is among the most genetically diverse of all monogenic diseases. The aim was to analyze the genetic causes of HSP among adult Serbian patients. The study comprised 74 patients from 65 families clinically diagnosed with HSP during a nine-year prospective period. A panel of thirteen genes was analyzed: L1CAM (SPG1), PLP1 (SPG2), ATL1 (SPG3A), SPAST (SPG4), CYP7B1 (SPG5A), SPG7 (SPG7), KIF5A (SPG10), SPG11 (SPG11), ZYFVE26 (SPG15), REEP1 (SPG31), ATP13A2 (SPG78), DYNC1H1, and BICD2 using a next generation sequencing-based technique. A copy number variation (CNV) test for SPAST, SPG7, and SPG11 was also performed. Twenty-three patients from 19 families (29.2%) had conclusive genetic findings, including 75.0% of families with autosomal dominant and 25.0% with autosomal recessive inheritance, and 15.7% of sporadic cases. Twelve families had mutations in the SPAST gene, usually with a pure HSP phenotype. Three sporadic patients had conclusive findings in the SPG11 gene. Two unrelated patients carried a homozygous pathogenic mutation c.233T>A (p.L78*) in SPG7 that is a founder Roma mutation. One patient had a heterozygous de novo variant in the KIF5A gene, and one had a compound heterozygous mutation in the ZYFVE26 gene. The combined genetic yield of our gene panel and CNV analysis for HSP was around 30%. Our findings broaden the knowledge on the genetic epidemiology of HSP, with implications for molecular diagnostics in this region. [ABSTRACT FROM AUTHOR]

Published

2022

13. Expansion of the mutation and phenotypic spectrum of hereditary spastic paraplegia.

Author

Xing, Fu and Du, Juan

Subjects

*PROTEINS, *GENETIC mutation, *FAMILIAL spastic paraplegia, *MEMBRANE transport proteins, *PHENOTYPES

Abstract

Background: Hereditary spastic paraplegias (HSPs) are a heterogeneous group of rare neurodegenerative disorders affecting the corticospinal tracts, and more than 80 HSP loci have been mapped to cause HSP. In this study, we aim to perform a genetic and clinical study of ten (6 male, 4 female) sporadic Chinese HSP patients.Methods: Next-generation sequencing (NGS) gene panels combined with multiplex ligation-dependent probe amplification assay (MLPA) analysis and the trinucleotide repeat dynamic mutation detection are available for the ten patients.Results: Among the 10 patients, one SPG7 patient, one SPG11 patient, and one pure SPG31 patient were detected. Two variants (deletion of exon 3-9 of SPG7 gene and the heterozygous mutation c.1861C > T/p.Q621* of SPG11 gene) were novel and three (c.1150_1150 + 1insCTAC/p.G384Afs*13 in SPG7 gene, c.3075dupA/p.E1026Rfs*4 in SPG11 gene, and c.478delA/p.R160Gfs*63 of REEP1 gene/SPG31) were previously reported. The SPG11 patient presented mild intellectual with peripheral neuropathy and thin corpus callosum (TCC) with no white matter abnormalities (WMA). The SPG7 patient detected in this study is the third SPG7 family reported in China; he manifested peripheral neuropathy, scoliosis, and polydactyly which expand the phenotype spectrum of SPG7.Conclusions: The AAO overlapped among each HSP subtype, which limited the ability to predict the subtype of HSP from AAO. Compared with non-Asian patients, the mutation frequency of SPG7 is relatively low in Asian populations. Considering the varieties of mutation types of HSP, we suggested targeted sequencing gene panels should be combined with MLPA for diagnosis of HSP. [ABSTRACT FROM AUTHOR]

Published

2022

14. New phenotype of RTN2‐related spectrum: Complicated form of spastic paraplegia‐12.

Author

Tian, Wotu, Zheng, Haoran, Zhu, Zeyu, Zhang, Chao, Luan, Xinghua, and Cao, Li

Subjects

*FAMILIAL spastic paraplegia, *MUSCLE tone, *EPILEPSY, *PHENOTYPES, *ENDOPLASMIC reticulum, *WESTERN immunoblotting

Abstract

Objective: Spastic paraplegia‐12 (SPG12) is a subtype of hereditary spastic paraplegia caused by Reticulon‐2 (RTN2) mutations. We described the clinical and genetic features of three SPG12 patients, functionally explored the potential pathogenic mechanism of RTN2 mutations, and reviewed RTN2‐related cases worldwide. Methods: The three patients were 31, 36, and 50 years old, respectively, with chronic progressive lower limb spasticity and walking difficulty. Physical examination showed elevated muscle tone, hyperreflexia and Babinski signs in the lower limbs. Patients 1 and 3 additionally had visual, urinary, and/or coordination dysfunctions. Patient 2 also had epileptic seizures. RTN2 mutations were identified by whole‐exome sequencing, followed by Sanger sequencing, segregation analysis, and phenotypic reevaluation. Functional examination of identified mutations was further explored. Results: Three variants in RTN2 were identified in Patient 1 (c.103C>T, p.R35X), Patient 2 (c.230G>A, p.G77D), and Patient 3 (c.337C>A, p.P113T) with SPG, respectively. Western blotting revealed the p.R35X with smaller molecular weight than WT and other two missense mutants. Immunostaining showed the wild type colocalized with endoplasmic reticulum (ER) in vitro. p.R35X mutant diffusely distributes in the cytoplasm, losing colocalization with ER. p.G77D and p.P113T co‐localized with ER, which was abnormally aggregated in clumps. Interpretation: In this study, we identified three cases with complicated SPG12 due to three novel RTN2 mutations, respectively, presenting various phenotypes: classic SPG symptoms with (1) visual abnormalities and sphincter disturbances or (2) seizures. The phenotypic heterogeneity might arise from the abnormal subcellular localization of mutant Reticulon‐2 and improper ER morphogenesis, revealing the RTN2‐related spectrum is still expanding. [ABSTRACT FROM AUTHOR]

Published

2022

15. Massive Parallel Sequencing and the Problem of Overlapping Phenotypes in Hereditary Spastic Paraplegias and Spinocerebellar Ataxias.

Author

Nuzhnyi, E. P., Abramycheva, N. Yu., Safonov, D. G., Fedotova, E. Yu., and Illarioshkin, S. N.

Subjects

*FAMILIAL spastic paraplegia, *NONSENSE mutation, *PHENOTYPES, *FRIEDREICH'S ataxia, *SPINOCEREBELLAR ataxia, *CEREBELLAR ataxia

Abstract

Hereditary spastic paraplegia (HSP) and spinocerebellar ataxia (SCA) are heterogeneous groups of neurodegenerative disorders with the main clinical manifestations including progressive pyramidal syndrome and cerebellar ataxia. The differential diagnosis of these diseases is difficult owing to the significant genetic and phenotypic polymorphism. The use of massive parallel sequencing (MPS) technologies makes it possible to assess the genetic basis of specific clinical syndromes and to clarify the systematization of these overlapping phenotypes. We examined 70 patients with degenerative cerebellar ataxias who were admitted to the clinic with one of the suspected forms of SCA. Mutation screening included panel sequencing on the Illumina MiSeq platform. In the group of patients with SCA phenotypes, four individuals (5.7%) were identified—carriers of mutations in the HSP genes: SPG5—1 patient, SPG7—1 patient, and SPG11—2 patients. Seven mutations were identified: CYP7B1 (SPG5) gene—p.R63X and p.R486C mutations; SPG7 gene—c.1047dupC (p.G352Rfs*43) and splice site mutation c.1779+1G>T, which was described by us for the first time. Two patients with SPG11 carried a compound heterozygous nonsense mutation p.Q811X in the SPG11 gene; other mutations were c.7168dupC (p.P2390fs) and c.733_734del (p.M245fs). The presented data confirm the concept that HSP and SCA represent a single continuum of spinocerebellar degenerations with a significant phenotypic overlap. To verify the diagnosis in patients with cerebellar and pyramidal syndrome of degenerative genesis, MPS methods should be used. [ABSTRACT FROM AUTHOR]

Published

2022

16. Identification of novel mutations by targeted NGS in Moroccan families clinically diagnosed with a neuromuscular disorder.

Author

Rochdi, Khaoula, Cerino, Mathieu, Da Silva, Nathalie, Delague, Valerie, Bouzidi, Aymane, Nahili, Halima, Zouiri, Ghizlane, Kriouile, Yamna, Gorokhova, Svetlana, Bartoli, Marc, Saïle, Rachid, Barakat, Abdelhamid, and Krahn, Martin

Subjects

*NEUROMUSCULAR diseases, *FAMILIAL spastic paraplegia, *GENETIC mutation, *DIAGNOSIS, *PHENOTYPES, *SYMPTOMS

Abstract

• NGS was used to identify homozygous mutation in two unrelated patients with neuromuscular disorders. • SIL1 mutation identified for the first time in the Moroccan population, associated to MSS. • Novel homozygous frames-shift FA2H mutation, responsible for the SPG-35. The identification of underlying genes of genetic conditions has expanded greatly in the past decades, which has broadened the field of genes responsible for inherited neuromuscular diseases. We aimed to investigate mutations associated with neuromuscular disorders phenotypes in 2 Moroccan families. Next-generation sequencing combined with Sanger sequencing could assist with understanding the hereditary variety and underlying disease mechanisms in these disorders. Two novel homozygous mutations were described in this study. The SIL1 mutation is the first identified in the Moroccan population, the mutation was identified as the main cause of Marinesco-Sjogren syndrome in one patient. While the second mutation identified in the fatty acid 2-hydroxylase gene (FA2H) was associated with the Spastic paraplegia 35 in another patient, both transmitted in an autosomal recessive pattern. These conditions are extremely rare in the North African population and may be underdiagnosed due to overlapping clinical characteristics and heterogeneity of these diseases. We have reported in this study mutations associated with the diseases found in the patients. In addition, we have narrowed the phenotypic spectrum, as well as the diagnostic orientation of patients with neuromuscular disorders, who might have very similar symptoms to other disease groups. [ABSTRACT FROM AUTHOR]

Published

2022

17. A Chinese Patient with Spastic Paraplegia Type 4 with a De Novo Mutation in the SPAST Gene.

Author

Xu, Li, Peng, Zijuan, Zhou, Chunhui, Wang, Jiqing, Luo, Hunjin, Lu, Qin, and Bao, Zhengjun

Subjects

*GENETIC mutation, *NONSENSE mutation, *MISSENSE mutation, *FAMILIAL spastic paraplegia, *PEOPLE with paraplegia, *PHENOTYPES, *GENE families

Abstract

Background. Spastic paraplegia type 4 (SPG4) is the most common type of hereditary spastic paraplegia (HSP) caused by mutations in the SPAST gene. Case Presentation. We report the case of a 27-year-old pregnant Chinese woman with HSP in whom we identified a missense mutation in the SPAST gene (c.1496G>A, p.Arg499His) and a nonsense mutation in the NEFH gene (c.289G>T, p.Glu97 ∗) via whole-exome sequencing; this finding corroborated that of Sanger sequencing. The patient exhibited the pure SPG4 phenotype with onset during childhood. The SPAST mutation was absent in the parents and paternal relatives. However, the NEFH mutation was identified in five people with no clinical phenotype. Based on theoretical conjecture and the family gene segregation information, we concluded that the SPAST mutation, but not the NEFH mutation, accounted for the proband's phenotype. Eventually, the woman gave birth to a healthy baby girl with the NEFH mutation. Conclusion. In this report, we identified a missense mutation in the SPAST gene (p.Arg499His) in a 27-year-old pregnant Chinese woman with HSP. We believe that this study expands the knowledge about the clinical parameters and mutation spectrum of SPG4. [ABSTRACT FROM AUTHOR]

Published

2021

18. Investigating ABCD1 mutations in a Taiwanese cohort with hereditary spastic paraplegia phenotype.

Author

Hsu, Shao-Lun, Chen, Ying-Hao, Chou, Cheng-Ta, Chou, Ying-Tsen, Tsai, Yu-Shuen, Hsiao, Cheng-Tsung, Liao, Yi-Chu, and Lee, Yi-Chung

Subjects

*FAMILIAL spastic paraplegia, *PHENOTYPES, *GENETIC mutation, *SYMPTOMS, *PEROXISOMAL disorders, *TAIWANESE people

Abstract

Background: Adrenoleukodystrophy (ALD) is an X-linked peroxisomal disorder caused by mutations in the ABCD1 gene. The clinical manifestations of ALD vary widely with some patients presenting with adrenomyeloneuropathy (AMN) that resembles the phenotype of hereditary spastic paraplegia (HSP). The aim of this study is to investigate the frequency, spectrum, and clinical features of ABCD1 mutations in Taiwanese patients with HSP phenotype.Methods: Mutational analysis of the ABCD1 gene was performed in 230 unrelated Taiwanese patients with clinically suspected HSP by targeted resequencing. Clinical, electrophysiological, and neuroimaging features of the patients carrying an ABCD1 pathogenic mutation were characterized.Results: Ten different ABCD1 mutations were identified in eleven patients, including two novel mutations (p.Q177Pfs*17 and p.Y357*) and eight ever reported in ALD cases of other ethnicities. All patients were male and exhibited slowly progressive spastic paraparesis with onset ages ranging from 21 to 50 years. Most of them had additional non-motor symptoms, including autonomic dysfunction in nine patients, sensory deficits in seven, premature baldness in seven, skin hyperpigmentation in five, psychiatric symptoms in one and cerebellar ataxia in one. Seven of the ten patients who ever received nerve conduction studies showed axonal polyneuropathy. Magnetic resonance imaging (MRI) revealed diffuse spinal cord atrophy in seven patients, cerebral white matter hyperintensity in one patient, and cerebellar involvement in one patient.Conclusions: ABCD1 mutations account for 4.8% (11/230) of the cases with HSP phenotype in Taiwan. This study highlights the importance to consider ABCD1 mutations in patients with clinically suspected HSP of unknown genetic causes. [ABSTRACT FROM AUTHOR]

Published

2021

19. Genotype-phenotype correlations of KIF5A stalk domain variants.

Author

de Boer, Eva M. J., van Rheenen, Wouter, Goedee, H. Stephan, Kamsteeg, Erik-Jan, Brilstra, Eva H., Veldink, Jan H., van Den Berg, Leonard H., and van Es, Michael A.

Subjects

*FAMILIAL spastic paraplegia, *AMYOTROPHIC lateral sclerosis, *PATIENT-family relations, *PHENOTYPES, *MYOCLONUS, *POLYNEUROPATHIES

Abstract

The kinesin family member 5A (KIF5A) motor domain variants are typically associated with hereditary spastic paraplegia (HSP) or Charcot-Marie-Tooth 2 (CMT2), while KIF5A tail variants predispose to amyotrophic lateral sclerosis (ALS) and neonatal intractable myoclonus. Variants within the stalk domain of KIF5A are relatively rare. We describe a family of three patients with a complex HSP phenotype and a likely pathogenic KIF5A stalk variant. More family members were reported to have walking difficulties. When reviewing the literature on KIF5A stalk variants, we found 22 other cases. The phenotypes varied with most cases having (complex) HSP/CMT2 or ALS. Symptom onset varied from childhood to adulthood and common additional symptoms for HSP are involvement of the upper limbs, sensorimotor polyneuropathy, and foot deformities. We conclude that KIF5A variants lead to a broad clinical spectrum of disease. Phenotype distribution according to variants in specific domains occurs often in the motor and tail domain but are not definite. However, variants in the stalk domain are not bound to a specific phenotype. [ABSTRACT FROM AUTHOR]

Published

2021

20. Spastic paraplegia type 46: novel and recurrent GBA2 gene variants in a compound heterozygous Italian patient with spastic ataxia phenotype.

Author

Gatti, Marta, Magri, Stefania, Di Bella, Daniela, Sarto, Elisa, Taroni, Franco, Mariotti, Caterina, and Nanetti, Lorenzo

Subjects

*GENETIC variation, *FAMILIAL spastic paraplegia, *SPINOCEREBELLAR ataxia, *PHENOTYPES, *SYMPTOMS, *PARAPLEGIA, *ATAXIA

Abstract

Introduction: Spastic paraplegia type 46 (SPG46) is a rare autosomal recessive hereditary spastic paraplegia, caused by mutations in the non-lysosomal glucosylceramidase β2 (GBA2) gene. Worldwide, approximately twenty SPG46 families have been identified so far. Case report: We describe a compound heterozygous Italian patient carrying a novel (p.Arg879Gln) and a recurrent (p.Arg399 *) GBA2 gene variant. The patient presented unsteady gait at age 2, and progressively manifested spastic-ataxia, scoliosis, mild intellectual decline, and bilateral cataract. Discussion: Clinical manifestations associated with GBA2 gene variants encompass a spectrum of overlapping phenotypes including cerebellar ataxia, spastic paraplegia, and Marinesco-Sjogren-like syndrome. We review previously reported cases of SPG46 and discuss possible genetic differential diagnosis. [ABSTRACT FROM AUTHOR]

Published

2021

21. The Genotype and Phenotype Features in a Large Chinese MFN2 Mutation Cohort.

Author

Ma, Yan, Sun, Aping, Zhang, Yingshuang, Fan, Dongsheng, and Liu, Xiaoxuan

Subjects

PHENOTYPES, GENOTYPES, GAIT disorders, CHARCOT-Marie-Tooth disease, NUCLEOTIDE sequencing, FAMILIAL spastic paraplegia

Abstract

Introduction: Charcot–Marie–Tooth disease type 2A (CMT2A) is a group of clinically and genetically heterogeneous disorders, which is mostly caused by mutations of the mitofusin2 (MFN2) gene. As the genotype–phenotype characteristics of CMT2A were still incompletely understood, we further explored the spectrum of CMT2A variants in China and demonstrated their phenotypic diversities. Methods: A total of 402 index patients/families with CMT throughout Mainland China were enrolled in this study. Among them, we analyzed 20 unrelated index cases with CMT2A by Sanger sequencing, next-generation sequencing, or whole-exome sequencing. Detailed clinical and genetic features of CMT2A patients were collected and analyzed. Of note, de novo mutations were not rare in MFN2 gene; we compared the clinical features of patients from the de novo group with those from the non- de novo group. Results: We identified 20 MFN2 variants, occupying 5.0% of CMT. Most patients presented with early onset and moderate phenotype with abnormal gait and foot drop as the main complaints at onset. Pyramidal signs accounts for 31.6% (6/19) in all patients, which is not uncommon. Four novel variants (p.Tyr752*, c.475-2A>G, p.Val99Met, and p.Arg275_Gln276insArg) were identified in the cohort. Besides, de novo variants occupied 35.0% (7/20) in our study with a much earlier age at onset compared with those in the non- de novo group (p = 0.021). Conclusion: Chinese CMT2A is a predominant typical pure CMT2A, with early onset and mild to moderate phenotype. Given the high frequency of de novo MFN2 mutations, genetic study should be considered for patients with early onset and severe idiopathic axonal neuropathy. [ABSTRACT FROM AUTHOR]

Published

2021

22. Niemann-Pick Type C 1 (NPC1) and NPC2 Gene Variability in Demented Patients with Evidence of Brain Amyloid Deposition.

Author

Sorrentino, Federica, Arighi, Andrea, Serpente, Maria, Arosio, Beatrice, Arcaro, Marina, Visconte, Caterina, Rotondo, Emanuela, Vimercati, Roberto, Ferri, Evelyn, Fumagalli, Giorgio G., Pietroboni, Anna M., Carandini, Tiziana, Scarpini, Elio, Fenoglio, Chiara, and Galimberti, Daniela

Subjects

*AMYLOID plaque, *AMYLOID, *GENETIC variation, *DISEASE risk factors, *CEREBROSPINAL fluid, *ALZHEIMER'S disease, *CEREBRAL amyloid angiopathy, *FAMILIAL spastic paraplegia, *BRAIN, *RESEARCH, *SEQUENCE analysis, *RESEARCH methodology, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies, *DEMENTIA, *MEMBRANE proteins, *PEPTIDES, *PHENOTYPES

Abstract

Background: Variants in Niemann-Pick Type C genes (NPC1 and NPC2) have been suggested to play a role as risk or disease modifying factors for Alzheimer's disease (AD).Objective: The aim of this study was to analyze NPC1 and NPC2 variability in demented patients with evidence of brain amyloid-β 1-42 (Aβ) deposition and to correlate genetic data with clinical phenotypes.Methods: A targeted Next Generation Sequencing panel was customized to screen NPC1, NPC2, and main genes related to neurodegenerative dementias in a cohort of 136 demented patients with cerebrospinal fluid (CSF) low Aβ levels or positive PET with Aβ tracer and 200 non-demented geriatric subjects.Results: Seven patients were carriers of NPC variants in heterozygosis. Four of them displayed pathogenic variants previously found in NPC patients and one AD patient had a novel variant. The latter was absent in 200 non-demented elderly subjects. Five of seven patients (70%) exhibited psychiatric symptoms at onset or later as compared with 43%in non-carriers (p > 0.05).Conclusion: The frequency of NPC1 and NPC2 heterozygous variants in patients with CSF evidence of Aβ deposition is higher than in the general population. [ABSTRACT FROM AUTHOR]

Published

2021

23. Neurophysiological and ophthalmological findings of SPG7-related spastic ataxia: a phenotype study in an Irish cohort.

Author

Bogdanova-Mihaylova, Petya, Chen, Hongying, Plapp, Helena Maria, Gorman, Ciara, Alexander, Michael D., McHugh, John C., Moran, Sharon, Early, Anne, Cassidy, Lorraine, Lynch, Timothy, Murphy, Sinéad M., and Walsh, Richard A.

Subjects

*PHENOTYPES, *ATAXIA, *NEUROLOGY, *OPTICAL coherence tomography, *FAMILIAL spastic paraplegia, *SPASTICITY

Abstract

Background: Mutations in SPG7 are increasingly identified as a common cause of spastic ataxia. We describe a cohort of Irish patients with recessive SPG7-associated phenotype. Methods: Comprehensive phenotyping was performed with documentation of clinical, neurophysiological, optical coherence tomography (OCT) and genetic data from individuals with SPG7 attending two academic neurology units in Dublin, including the National Ataxia Clinic. Results: Thirty-two symptomatic individuals from 25 families were identified. Mean age at onset was 39.1 years (range 12–61), mean disease duration 17.8 years (range 5–45), mean disease severity as quantified with the scale for the assessment and rating of ataxia 9/40 (range 3–29). All individuals displayed variable ataxia and spasticity within a spastic-ataxic phenotype, and additional ocular abnormalities. Two had spasmodic dysphonia and three had colour vision deficiency. Brain imaging consistently revealed cerebellar atrophy (n = 29); neurophysiology demonstrated a length-dependent large-fibre axonal neuropathy in 2/27 studied. The commonest variant was c.1529C > T (p.Ala510Val), present in 21 families. Five novel variants were identified. No significant thinning of average retinal nerve fibre layer (RNFL) was demonstrated on OCT (p = 0.61), but temporal quadrant reduction was evident compared to controls (p < 0.05), with significant average and temporal RNFL decline over time. Disease duration, severity and visual acuity were not correlated with RNFL thickness. Conclusions: Our results highlight that recessive SPG7 mutations may account for spastic ataxia with peripheral neuropathy in only a small proportion of patients. RNFL abnormalities with predominant temporal RNFL reduction are common and OCT should be considered part of the routine assessment in spastic ataxia. [ABSTRACT FROM AUTHOR]

Published

2021

24. CAPN1 and hereditary spastic paraplegia: a novel variant in an Iranian family and overview of the genotype-phenotype correlation.

Author

Rahimi Bidgoli, Mohammad Masoud, Javanparast, Leila, Rohani, Mohammad, Najmabadi, Hossein, Zamani, Babak, and Alavi, Afagh

Subjects

*FAMILIAL spastic paraplegia, *IRANIANS, *NEURODEGENERATION, *DIAGNOSIS, *PHENOTYPES, *NEUROLOGICAL disorders

Abstract

SPG76 is one of the rare forms of hereditary spastic paraplegia (HSP) which causes by mutations in the CAPN1 gene. The mode of inheritance of SPG76 is autosomal recessive (AR) and so far, only 24 families and 25 mutations in this gene have been reported worldwide. These mutations have been associated with a spectrum of disorders from pure HSP to spastic ataxia. HSP genetically is one of the most heterogeneous neurological disorders and to date, 79 types of HSP (SPG1-SPG79) have been identified, however, it has been suggested that many HSP-genes, particularly in AR-HSPs, remained unknown. AR-HSPs clinically overlap with other neurodegenerative disorders, making an accurate diagnosis of the disease difficult. Therefore, in addition to clinical examination, a high throughout genetic method like whole exome sequencing (WES) may be necessary for the diagnosis of this type of neurodegenerative disorders. Herein, we present the clinical features and results of WES in the first Iranian family with a novel CAPN1 variant, c.C853T:p.R285* and pure HSP. Some of the previous studies have mentioned that the "spasticity-ataxia phenotype might be conducted to the diagnosis of SPG76" but recently the number of pure HSP patients with CAPN1 mutation is increasing. The present study also expands the mutation spectrum of pure CAPN1-related SPG76; emphasizing that CAPN1 screening is required in both pure HSP and spasticity-ataxia phenotypes. As noted in some other literature, we suggest the clinical spectrum of this disorder to be considered as "CAPN1-associated neurodegeneration". [ABSTRACT FROM AUTHOR]

Published

2021

25. A Complex Phenotype of a Patient with Spastic Paraplegia Type 4 Caused by a Novel Pathogenic Variant in the SPAST Gene.

Author

Akaba, Yuichi, Takeguchi, Ryo, Tanaka, Ryosuke, and Takahashi, Satoru

Subjects

*EPILEPSY, *PARTIAL epilepsy, *SEIZURES (Medicine), *FAMILIAL spastic paraplegia, *GENETIC variation, *PEOPLE with paraplegia, *PHENOTYPES

Abstract

Hereditary spastic paraplegias (HSPs) are rare neurological disorders caused by degeneration of the corticospinal tract. Among the 79 causative genes involved in HSPs, variants in SPAST on chromosome 2p22, which encodes the microtubule-severing protein spastin, are responsible for spastic paraplegia type 4 (SPG4), the most common form of HSPs. SPG4 is characterized by a clinically pure phenotype that is associated with restricted involvement of the corticospinal tract; however, it is often accompanied by additional neurological symptoms such as epilepsy and cognitive impairment. There are few reports regarding the clinical course and treatment of epilepsy associated with SPG4. We describe a 21-year-old male patient with progressive weakness and spasticity of the lower limbs since infancy, which was complicated by epilepsy and cognitive impairment. Magnetic resonance imaging of the brain showed right hippocampal atrophy before the onset of epilepsy. Genetic analysis revealed a novel missense variant (NM_014946.4:c.1330G>C, p.Asp444His) in the SPAST gene. At the age of 13, the patient developed focal epilepsy, characterized by focal onset seizures that were preceded by a sensation of chest tightness. Carbamazepine, levetiracetam, and zonisamide were ineffective in controlling the seizures; however, the use of lacosamide in combination with lamotrigine and valproate was highly effective in improving the seizure symptoms and led to the patient being seizure free for at least 2 years. In conclusion, the missense variant in SPAST may cause a complex SPG4 phenotype accompanied by epilepsy and cognitive impairment, suggesting that the clinical manifestations of this condition do not confine to the motor system. [ABSTRACT FROM AUTHOR]

Published

2021

26. GCH1 mutations in hereditary spastic paraplegia.

Author

Varghaei, Parizad, Yoon, Grace, Estiar, Mehrdad A., Veyron, Simon, Leveille, Etienne, Dupré, Nicolas, Trempe, Jean‐François, Rouleau, Guy A., and Gan‐Or, Ziv

Subjects

*FAMILIAL spastic paraplegia, *TWINS, *GENETIC variation, *PARKINSON'S disease, *PHENOTYPES, *TETRAHYDROBIOPTERIN

Abstract

GCH1 mutations have been associated with dopa‐responsive dystonia (DRD), Parkinson's disease (PD) and tetrahydrobiopterin (BH4)‐deficient hyperphenylalaninemia B. Recently, GCH1 mutations have been reported in five patients with hereditary spastic paraplegia (HSP). Here, we analyzed a total of 400 HSP patients (291 families) from different centers across Canada by whole exome sequencing (WES). Three patients with heterozygous GCH1 variants were identified: monozygotic twins with a p.(Ser77_Leu82del) variant, and a patient with a p.(Val205Glu) variant. The former variant is predicted to be likely pathogenic and the latter is pathogenic. The three patients presented with childhood‐onset lower limb spasticity, hyperreflexia and abnormal plantar responses. One of the patients had diurnal fluctuations, and none had parkinsonism or dystonia. Phenotypic differences between the monozygotic twins were observed, who responded well to levodopa treatment. Pathway enrichment analysis suggested that GCH1 shares processes and pathways with other HSP‐associated genes, and structural analysis of the variants indicated a disruptive effect. In conclusion, GCH1 mutations may cause HSP; therefore, we suggest a levodopa trial in HSP patients and including GCH1 in the screening panels of HSP genes. Clinical differences between monozygotic twins suggest that environmental factors, epigenetics, and stochasticity could play a role in the clinical presentation. [ABSTRACT FROM AUTHOR]

Published

2021

27. VPS13D: One Family, Same Mutations, Two Phenotypes.

Author

Petry‐Schmelzer, Jan Niklas, Keller, Natalie, Karakaya, Mert, Wirth, Brunhilde, Fink, Gereon R., and Wunderlich, Gilbert

Subjects

*MOVEMENT disorders, *FAMILIAL spastic paraplegia, *NEUROLOGICAL disorders, *GENETIC variation, *PHENOTYPES, *MEDICAL personnel

Abstract

Keywords: VPS13D; phenotype-genotype correlation EN VPS13D phenotype-genotype correlation 803 806 4 07/21/21 20210701 NES 210701 Here, we report two siblings with compound heterozygous variants in I VPS13D i but a considerable divergent phenotype highlighting the difficulties of phenotype-genotype correlation in this rare disease. In contrast, non-essential splice site/LOF mutations or other mutation type combinations might be associated with a broader and more severe spectrum of phenotypes.2 Given our siblings' identical compound heterozygous I VPS13D i variants and their unlike phenotypes, a specific phenotype-genotype correlation seems questionable. This makes it even more important to be aware of this gene, especially in patients presenting with childhood-onset ataxia-plus syndrome or suspected hereditary spastic paraplegia with or without mental disability. [Extracted from the article]

Published

2021

28. How many phenotypes for the FBXO11 related disease? Report on a new patient with a tricho-rhino-phalangeal like phenotype.

Author

Mégarbané, Andre, Mehawej, Cybel, Mahfoud, Daniel, Chouery, Eliane, Devriendt, Koenraad, Hijazi, Mariam, Ryu, Seung W., Kim, JiHye, and McNeill, Alisdair

Subjects

*PHENOTYPES, *PHALANGES, *RHINOCEROSES, *DEVELOPMENTAL delay, *EYEBROWS, *GENETIC mutation, *HIP joint, *FAMILIAL spastic paraplegia

Abstract

Here we report the case of a young boy with developmental delay, thin sparse hair, early closure of the anterior fontanel, bilateral choanal atresia, brachyturicephaly; and dysmorphic features closely resembling those seen in trichorhinophalangeal syndrome (TRPS). These features include sparse hair, sparse lateral eyebrows, a bulbous pear shaped nose, a long philtrum, thin lips, small/hypoplastic nails, pes planovalgus; bilateral cone-shaped epiphyses at the proximal 5th phalanx, slender long bones, coxa valga, mild scoliosis, and delayed bone age. Given that TRPS had been excluded by a thorough genetic analysis, whole exome sequencing was performed and a heterozygous likely pathogenic variant was identified in the FBXO11 gene (NM_001190274.2: c.1781A > G; p. His594Arg), confirming the diagnosis of the newly individualized IDDFBA syndrome: Intellectual Developmental Disorder, dysmorphic Facies, and Behavioral Abnormalities (OMIM# 618,089). Our findings further delineate the clinical spectrum linked to FBXO11 and highlight the importance of investigating further cases with mutations in this gene to establish a potential genotype-phenotype correlation. [ABSTRACT FROM AUTHOR]

Published

2024

29. Genotype–phenotype associations in hereditary spastic paraplegia: a systematic review and meta-analysis on 13,570 patients.

Author

Erfanian Omidvar, Maryam, Torkamandi, Shahram, Rezaei, Somaye, Alipoor, Behnam, Omrani, Mir Davood, Darvish, Hossein, and Ghaedi, Hamid

Subjects

*FAMILIAL spastic paraplegia, *AGE of onset, *PHENOTYPES, *GENDER, *NEURODEGENERATION

Abstract

Aims: The hereditary spastic paraplegias (HSPs) are a heterogeneous group of inherited neurodegenerative disorders. Although, several genotype–phenotype studies have carried out on HSPs, the association between genotypes and clinical phenotypes remain incomplete since most studies are small in size or restricted to a few genes. Accordingly, this study provides the systematic meta-analysis of genotype–phenotype associations in HSP. Methods and results: We retrieved literature on genotype–phenotype associations in patients with HSP and mutated SPAST, REEP1, ATL1, SPG11, SPG15, SPG7, SPG35, SPG54, SPG5. In total, 147 studies with 13,570 HSP patients were included in our meta-analysis. The frequency of mutations in SPAST (25%) was higher than REEP1 (3%), as well as ATL1 (5%) in AD-HSP patients. As for AR-HSP patients, the rates of mutations in SPG11 (18%), SPG15 (7%) and SPG7 (13%) were higher than SPG5 (5%), as well as SPG35 (8%) and SPG54 (7%). The mean age of AD-HSP onset for ATL1 mutation-positive patients was earlier than patients with SPAST, REEP1 mutations. Also, the tendency toward younger age at AR-HSP onset for SPG35 was higher than other mutated genes. It is noteworthy that the mean age at HSP onset ranged from infancy to adulthood. As for the gender distribution, the male proportion in SPG7-HSP (90%) and REEP1-HSP (78%) was markedly high. The frequency of symptoms was varied among patients with different mutated genes. The rates of LL weakness, superficial sensory abnormalities, neuropathy, and deep sensory impairment were noticeably high in REEP1 mutations carriers. Also, in AR-HSP patients with SPG11 mutations, the presentation of symptoms including pes cavus, Neuropathy, and UL spasticity was higher. Conclusion: Our comprehensive genotype–phenotype assessment of available data displays that the mean age at disease onset and particular sub-phenotypes are associated with specific mutated genes which might be beneficial for a diagnostic procedure and differentiation of the specific mutated genes phenotype among diverse forms of HSP. [ABSTRACT FROM AUTHOR]

Published

2021

30. Description of clinical features and genetic analysis of one ultra-rare (SPG64) and two common forms (SPG5A and SPG15) of hereditary spastic paraplegia families.

Author

Pashaei, Mahdieh, Davarzani, Atefeh, Hajati, Reza, Zamani, Babak, Nafissi, Shahriar, Larti, Farzaneh, Nilipour, Yalda, Rohani, Mohammad, and Alavi, Afagh

Subjects

*FAMILIAL spastic paraplegia, *PHENOTYPES, *FAMILIES, *GENETIC mutation, *NEURODEGENERATION

Abstract

Hereditary spastic paraplegia (HSP) is a clinically and genetically heterogeneous neurodegenerative disorder, characterized by lower-limb spasticity and weakness. To date, more than 82 loci/genes (SPG1-SPG82) have been identified that contribute to the cause of HSP. Despite the use of next-generation sequencing-based methods, genetic-analysis has failed in the finding of causative genes in more than 50% of HSP patients, indicating a more significant heterogeneity and absence of a given phenotype-genotype correlation. Here, we performed whole-exome sequencing (WES) to identify HSP-causing genes in three unrelated-Iranian probands. Candidate variants were detected and confirmed in the probands and co-segregated in the family members. The phenotypic data gathered and compared with earlier cases with the same sub-types of disease. Three novel homozygous variants, c.978delT; p.Q327Kfs*39, c.A1208G; p.D403G and c.3811delT; p.S1271Lfs*44, in known HSP-causing genes including ENTPD1, CYP7B1, and ZFYVE26 were identified, respectively. Intra and interfamilial clinical variability were observed among affected individuals. Mutations in CYP7B1 and ZFYVE26 are relatively common causes of HSP and associated with SPG5A and SPG15, respectively. However, mutations in ENTPD1 are related to SPG64 which is an ultra-rare form of HSP. The research affirmed more complexities of phenotypic manifestations and allelic heterogeneity in HSP. Due to these complexities, it is not feasible to show a clear phenotype-genotype correlation in HSP cases. Identification of more families with mutations in HSP-causing genes may help the establishment of this correlation, further understanding of the molecular basis of the disease, and would provide an opportunity for genetic-counseling in these families. [ABSTRACT FROM AUTHOR]

Published

2021

31. Clinical and genetic characterization of hereditary spastic paraplegia type 3A in Taiwan.

Author

Hsu, Shao-Lun, Hsueh, Hsueh-Wen, Chen, Shih-Ying, Chang, Yung-Yee, Tan, Shennie, Hong, Chien-Tai, Tsai, Yu-Shuen, Yu, Kai-Wei, Wu, Hsiu-Mei, Liao, Yi-Chu, Soong, Bing-Wen, Hu, Chaur-Jong, Lan, Min-Yu, and Lee, Yi-Chung

Subjects

*FAMILIAL spastic paraplegia, *SINGLE nucleotide polymorphisms, *PHENOTYPES, *DIAGNOSIS, *DISABILITIES, *TAIWANESE people, *RESEARCH, *GENETICS, *SEQUENCE analysis, *RESEARCH methodology, *EVALUATION research, *COMPARATIVE studies, *MEMBRANE proteins, *CARRIER proteins, *LONGITUDINAL method

Abstract

Aim: To investigate the clinical and genetic features of hereditary spastic paraplegia (HSP) type 3A (SPG3A) in Taiwan.Methods: Mutational analysis of the ATL1 gene was performed for 274 unrelated Taiwanese HSP patients. The diagnosis of SPG3A was ascertained by the presence of a heterozygous pathogenic mutation in ATL1. The SPG3A patients received clinical, electrophysiological, and neuroimaging evaluations. Disease severity was assessed by using Spastic Paraplegia Rating Scale (SPRS) and disability score. Nineteen single nucleotide polymorphism (SNP) markers flanking ATL1 were genotyped for haplotype analysis of ATL1 p.R416C mutation.Results: Eighteen SPG3A patients from 11 families were identified. They typically presented a pure form HSP phenotype with disease onset ranging from age 1-68 years. Five heterozygous ATL1 mutations were identified, including p.R239C, p.V253I, p.Y336H, p.P342R and p.R416C. ATL1 p.R416C was the most common mutation and presented in five SPG3A pedigrees. Haplotype analyses demonstrated a shared haplotype in the 12 individuals carrying a p.R416C allele.Conclusion: SPG3A accounts for 4% (11 out of 274) of HSP in the Taiwanese cohort. Patents with the ATL1 p.R416C mutation in Taiwan may descend from a common ancestor. This study defines the clinical and genetic features of SPG3A in Taiwan and provides useful information for the diagnosis and management, especially in patients of Han Chinese descent. [ABSTRACT FROM AUTHOR]

Published

2021

32. Cognitive dysfunction and psychosis: expanding the phenotype of SPG7.

Author

Soares, Izadora Fonseca Zaiden, Ciarlariello, Vinicius Boaratti, Feder, David, and Carvalho, Alzira Alves De Siqueira

Subjects

*FAMILIAL spastic paraplegia, *COGNITION disorders, *PHENOTYPES, *PSYCHOSES

Abstract

Spastic paraplegia type 7 (SPG7) is one of the most common forms of autosomal recessive hereditary spastic paraplegia, which can lead to a hybrid spastic-ataxic phenotype. Recently, novel complicated forms of SPG7, including cognitive and social impairment phenotypes, have been reported. We present a SPG7 case with two pathogenic variants in compound heterozygosity in the SPG7 gene, featuring a cerebellar cognitive affective syndrome with psychosis not yet described in the literature. [ABSTRACT FROM AUTHOR]

Published

2021

33. Pseudoxanthoma elasticum overlaps hereditary spastic paraplegia type 56.

Author

Legrand, A., Pujol, C., Durand, C. M., Mesnil, A., Rubera, I., Duranton, C., Zuily, S., Sousa, A. B., Renaud, M., Boucher, J. L., Pietrancosta, N., Adham, S., Orssaud, C., Marelli, C., Casali, C., Ziccardi, L., Villain, N., Ewenczyk, C., Durr, A., and Mignot, C.

Subjects

*FAMILIAL spastic paraplegia, *GENETIC testing, *PHENOTYPES, *FUNCTIONAL analysis, *RESEARCH, *GENETIC mutation, *SKIN, *RESEARCH methodology, *RETROSPECTIVE studies, *MEDICAL cooperation, *EVALUATION research, *CONNECTIVE tissue diseases, *EYE, *COMPARATIVE studies, *CALCINOSIS, *RESEARCH funding, *EPITHELIAL cells, *CARRIER proteins, *HEMOPROTEINS

Abstract

Purpose: Pseudoxanthoma elasticum (PXE) is a recessive disorder involving skin, eyes and arteries, mainly caused by ABCC6 pathogenic variants. However, almost one fifth of patients remain genetically unsolved despite extensive genetic screening of ABCC6, as illustrated in a large French PXE series of 220 cases. We searched for new PXE gene(s) to solve the ABCC6-negative patients.Methods: First, family-based exome sequencing was performed, in one ABCC6-negative PXE patient with additional neurological features, and her relatives. CYP2U1, involved in hereditary spastic paraplegia type 56 (SPG56), was selected based on this complex phenotype, and the presence of two candidate variants. Second, CYP2U1 sequencing was performed in a retrospective series of 46 additional ABCC6-negative PXE probands. Third, six additional SPG56 patients were evaluated for PXE skin and eye phenotype. Additionally, plasma pyrophosphate dosage and functional analyses were performed in some of these patients.Results: 6.4% of ABCC6-negative PXE patients (n = 3) harboured biallelic pathogenic variants in CYP2U1. PXE skin lesions with histological confirmation, eye lesions including maculopathy or angioid streaks, and various neurological symptoms were present. CYP2U1 missense variants were confirmed to impair protein function. Plasma pyrophosphate levels were normal. Two SPG56 patients (33%) presented some phenotypic overlap with PXE.Conclusion: CYP2U1 pathogenic variants are found in unsolved PXE patients with neurological findings, including spastic paraplegia, expanding the SPG56 phenotype and highlighting its overlap with PXE. The pathophysiology of ABCC6 and CYP2U1 should be explored to explain their respective role and potential interaction in ectopic mineralization. [ABSTRACT FROM AUTHOR]

Published

2021

34. SPG11 presenting with dystonic tremor in childhood.

Author

Innes, Emily A., Goetti, Robert, Mahant, Neil, Ho, Gladys, Williams, Laura, Gill, Deepak, Dale, Russell C., and Mohammad, Shekeeb S.

Subjects

*FAMILIAL spastic paraplegia, *MOVEMENT disorders, *TREMOR, *CORPUS callosum, *MOTOR neurons, *PROTEINS, *GENETIC mutation, *PHENOTYPES

Abstract

This is a unique case of SPG11 mutation presenting as childhood onset dystonic tremor without weakness or spastic paraplegia. Hereditary spastic paraplegia is the most common phenotype of SPG11 mutation though there are reports of an extended phenotype of SPG11 including dopa-responsive dystonia and tremor. [ABSTRACT FROM AUTHOR]

Published

2022

35. Case Series of Autosomal Recessive Hereditary Spastic Paraplegia in Adults.

Author

Chakor, Rahul T. and Patil, Neelam S.

Subjects

*SPINE radiography, *BRAIN, *GENETIC mutation, *GENETIC testing, *MAGNETIC resonance imaging, *FAMILIAL spastic paraplegia, *GENOTYPES, *PHENOTYPES, *SYMPTOMS, *ADULTS

Published

2021

36. Complex hereditary spastic paraplegia associated with episodic visual loss caused by ACO2 variants.

Author

Tozawa, Takenori, Nishimura, Akira, Ueno, Tamaki, Shikata, Akane, Taura, Yoshihiro, Yoshida, Takeshi, Nakagawa, Naoko, Wada, Takahito, Kosugi, Shinji, Uehara, Tomoko, Takenouchi, Toshiki, Kosaki, Kenjiro, and Chiyonobu, Tomohiro

Subjects

FAMILIAL spastic paraplegia, MUSCLE hypotonia, RETINAL degeneration, PHENOTYPES, GENETIC disorders

Abstract

Most patients with homozygous or compound heterozygous pathogenic ACO2 variants present with muscular hypotonia features, namely, infantile cerebellar-retinal degeneration. Recently, two studies reported rare familial cases of ACO2 variants presenting as complex hereditary spastic paraplegia (HSP) with broad clinical spectra. Here, we report the case of a 20-year-old Japanese woman with complex HSP caused by compound heterozygous ACO2 variants, revealing a new phenotype of episodic visual loss during febrile illness. [ABSTRACT FROM AUTHOR]

Published

2021

37. A hereditary spastic paraplegia predominant phenotype caused by variants in the NEFL gene.

Author

Mul, Karlien, Schouten, Meyke I., van der Looij, Erica, Dooijes, Dennis, Hennekam, Frederic A.M., Notermans, Nicolette C., Praamstra, Peter, van Gaalen, Judith, Kamsteeg, Erik-Jan, Verbeek, Nienke E., and van de Warrenburg, Bart P.C.

Subjects

*FAMILIAL spastic paraplegia, *CHARCOT-Marie-Tooth disease, *GENETIC testing, *PHENOTYPES, *GENES, *NUCLEOTIDE sequencing

Abstract

Introduction: This study reports a large series of patients with a clinical picture dominated by spastic paraplegia in whom variants in the NEFL gene, a known cause for Charcot-Marie-Tooth disease, were identified.Methods: Index patients referred for a suspicion of hereditary spastic paraplegia (HSP) were clinically assessed and genetic analysis by next-generation sequencing was undertaken. Additional family members were clinically examined and subjected to targeted testing.Results: We identified two different heterozygous dominant variants in the NEFL gene in 25 patients from 14 families. Most of them (21/25) had a clinical diagnosis of HSP, often with a concomitant clinical diagnosis of polyneuropathy (16/21). Two patients were identified with a polyneuropathy with a pyramidal reflex pattern, but without spasticity. Two patients had isolated polyneuropathy. Out of the 21 patients with a diagnosis of HSP, two had co-occurring cerebellar signs. The c.262A > C p.(Thr88Pro) variant was detected in 13 families. Genealogical analysis showed shared ancestors or a similar geographical origin in 12, suggesting a founder effect. The other variant, c.296A > C p.(Asp99Ala), was found in only one family, in which limited segregation analysis could be performed.Discussion: Variants in the NEFL gene can cause HSP, with or without co-existing polyneuropathy, and should be included in diagnostic testing strategies for HSP patients. [ABSTRACT FROM AUTHOR]

Published

2020

38. Bi-allelic variants in PNPLA6 possibly associated with Parkinsonian features in addition to spastic paraplegia phenotype.

Author

Sen, Kuntal, Finau, Melesilika, and Ghosh, Pritha

Subjects

*FAMILIAL spastic paraplegia, *PATHOLOGY, *PARAPLEGIA, *DOPAMINERGIC neurons, *SYMPTOMS, *PHENOTYPES

Abstract

Variants in the PNPLA6 gene are known to cause 4 distinct phenotypes. One known phenotype is Hereditary Spastic Paraplegia type 39 (HSP 39), a rare neurodegenerative condition characterized by variable onset of lower limb spasticity, weakness and ataxia. Little is known about complications of HSP 39 in adulthood. Here, we report a family of three siblings who presented with bilateral lower limb spasticity in childhood, consistent with HSP, with confirmed bi-allellic PNPLA6 mutations. Two siblings developed parkinsonian features in middle age, a novel finding in this sibship. The proband had a positive dopamine transporter scan, indicating degeneration in dopaminergic neurons, and dopa-responsive extrapyramidal symptoms. Testing for known genetic causes of Parkinsonism was negative. The PNPLA6 gene encodes neuropathy target esterase, an enzyme involved in lipid metabolism that is critical to the stability of cell membranes. We hypothesize that the development of Parkinsonism in these patients may be related to the PNPLA6 mutations, as lipid dysregulation has been implicated in the pathogenesis of Parkinson disease. [ABSTRACT FROM AUTHOR]

Published

2020

39. Paediatric-onset hereditary spastic paraplegias: a retrospective cohort study.

Author

Schiavoni, Silvia, Spagnoli, Carlotta, Rizzi, Susanna, Salerno, Grazia G, Frattini, Daniele, Pisani, Francesco, and Fusco, Carlo

Subjects

*FAMILIAL spastic paraplegia, *HUMAN chromosome abnormality diagnosis, *COHORT analysis, *NUCLEOTIDE sequencing, *RETROSPECTIVE studies, *GENETIC testing, *PHENOTYPES

Abstract

Aim: To describe the clinical and neurogenetic spectrum of paediatric-onset hereditary spastic paraplegias (HSPs) diagnosed in our unit.Method: We report on 47 patients (30 males, 17 females; mean [SD] age 12y 7mo [6y 2mo], range 4-34y) clinically diagnosed with an HSP at the Child Neurology Unit, IRCCS-ASMN (Reggio Emilia, Italy) between 1990 and 2018, who were genetically investigated by means of single-gene direct sequencing and/or next-generation sequencing technologies (targeted panels, whole-exome sequencing [WES]).Results: Complex forms prevailed slightly (n=26), autosomal dominant being the main inheritance pattern (n=11), followed by recessive (n=5) and X-linked (n=1). A definite genetic diagnosis was achieved in 17 patients. Spastic paraplegia 3A (n=4) was the most frequent cause of autosomal dominant HSP in our cohort, while no genetic variant prevailed in autosomal recessive forms and pathogenic/likely pathogenic variants were disclosed in a wide range of different genes.Interpretation: We found wide phenotypic and genetic heterogeneity. With increasing accessibility to WES, a higher number of patients receive a diagnosis, allowing detection of variants in ultra-rare disease-causing genes and refining genotype-phenotype correlations.What This Paper Adds: A genetic diagnosis of paediatric-onset hereditary spastic paraplegia was achieved in one-third of patients. Pathogenic/likely pathogenic variants in rare genes were found. Genotypic and phenotypic heterogeneity favours targeted panel/whole-exome sequencing for diagnosis. [ABSTRACT FROM AUTHOR]

Published

2020

40. Janus-faced spatacsin (SPG11): involvement in neurodevelopment and multisystem neurodegeneration.

Author

Pozner, Tatyana, Regensburger, Martin, Engelhorn, Tobias, Winkler, Jürgen, and Winner, Beate

Subjects

*FAMILIAL spastic paraplegia, *NEURAL development, *CORPUS callosum, *SYMPTOMS, *MOVEMENT disorders, *NEURODEGENERATION, *PROTEINS, *GENETIC mutation, *ANIMAL experimentation, *PHENOTYPES

Abstract

Hereditary spastic paraplegia (HSP) is a heterogeneous group of rare motor neuron disorders characterized by progressive weakness and spasticity of the lower limbs. HSP type 11 (SPG11-HSP) is linked to pathogenic variants in the SPG11 gene and it represents the most frequent form of complex autosomal recessive HSP. The majority of SPG11-HSP patients exhibit additional neurological symptoms such as cognitive decline, thin corpus callosum, and peripheral neuropathy. Yet, the mechanisms of SPG11-linked spectrum diseases are largely unknown. Recent findings indicate that spatacsin, the 280 kDa protein encoded by SPG11, may impact the autophagy-lysosomal machinery. In this update, we summarize the current knowledge of SPG11-HSP. In addition to clinical symptoms and differential diagnosis, our work aims to link the different clinical manifestations with the respective structural abnormalities and cellular in vitro phenotypes. Moreover, we describe the impact of localization and function of spatacsin in different neuronal systems. Ultimately, we propose a model in which spatacsin bridges between neurodevelopmental and neurodegenerative phenotypes of SPG11-linked disorders. [ABSTRACT FROM AUTHOR]

Published

2020

41. FARS2 Mutations: More Than Two Phenotypes? A Case Report.

Author

Hotait, Mostafa, Nasreddine, Wassim, El-Khoury, Riyad, Dirani, Maya, Nawfal, Omar, and Beydoun, Ahmad

Subjects

GENETIC mutation, STATUS epilepticus, SEIZURES (Medicine), OLDER women, PHENOTYPES, FAMILIAL spastic paraplegia

Abstract

FARS2, a nuclear gene, encodes the mitochondrial phenylalanyl-tRNA synthetase (mtPheRS). Previous reports have described two distinct phenotypes linked to FARS2 gene mutation: an early onset epileptic encephalopathy and spastic paraplegia. This report describes a distinctive phenotype of FARS2-linked, juvenile onset refractory epilepsy, caused by a hemizygous mutation in a compound heterozygous state (p.V197M and exon 2 microdeletion). A 17-year- old woman with normal development presented with a super refractory focal motor status epilepticus. Only an emergency life-saving surgery aborted her status after all therapeutic interventions, including anesthesia, failed to control her seizures. Pathological and biochemical activities on muscle biopsy showed mitochondrial proliferation with enhanced isolated activities of complexes II and IV, suggestive of a compensatory mechanism for the bioenergetic deficiency. Postoperatively, the patient started experiencing focal aware motor seizures originating from the contralateral hemisphere after being seizure free for a few months. This report suggests a third phenotypic manifestation of FARS2 gene mutation. [ABSTRACT FROM AUTHOR]

Published

2020

42. Neurological Phenotypes Associated with AAAS-Related Disorders: Spastic Ataxia and Complex Spastic Paraplegia.

Author

Lorea, Cláudia Fernandes, Tenório, Renata Barreto, Koenig, Michel, Huebner, Angela, Koehler, Katrin, Devos, David, Guissart, Claire, and Saute, Jonas Alex Morales

Subjects

*FAMILIAL spastic paraplegia, *PARAPLEGIA, *ATAXIA, *DISEASES, *PHENOTYPES

Abstract

Sir, Triple A syndrome (AAAS) is a rare autosomal recessive disorder caused by pathogenic variants in I AAAS i initially described as the triad achalasia, ACTH-resistant adrenal failure, and defective tear production [[1]]. In this report, we expand AAAS-related disorders spectrum by describing a Brazilian family with a complex hereditary spastic paraplegia (HSP) phenotype and a Moroccan family with spastic-ataxia and severe amyotrophy phenotype. [Extracted from the article]

Published

2020

43. Clinical and Molecular Diagnosis of Joubert Syndrome and Related Disorders.

Author

Radha Rama Devi, Akella, Naushad, Shaik Mohammad, and Lingappa, Lokesh

Subjects

*JOUBERT syndrome, *MOLECULAR diagnosis, *MOLARS, *RETINAL diseases, *DISEASES, *FAMILIAL spastic paraplegia, *CEREBELLUM abnormalities, *RETINA abnormalities, *PRENATAL diagnosis, *CELL cycle proteins, *CYTOSKELETAL proteins, *MULTIPLE human abnormalities, *EYE abnormalities, *CYSTIC kidney disease, *GENETIC techniques, *TUMOR antigens, *PHENOTYPES, *GENEALOGY

Abstract

Background: Joubert syndrome and related disorders are a group of ciliopathies characterized by mid-hindbrain malformation, developmental delay, hypotonia, oculomotor apraxia, and breathing abnormalities. Molar tooth sign in brain imaging is the hallmark for diagnosis. Joubert syndrome is a clinically and genetically heterogeneous disorder involving mutations in 35 ciliopathy-related genes. We present a large cohort of 59 patients with Joubert syndrome from 55 families. Molecular analysis was performed in 35 families (trio).Methods: Clinical exome analysis was performed to identify causal mutations, and genotype-phenotype correlations were evaluated.Results: All of the cases were stratified into pure Joubert syndrome (62.7%), Joubert syndrome with retinal disease (22.0%), polydactyly (8.5%), and liver (1.7%) and kidney (1.7%) involvement. Joubert syndrome-related disorders include Meckel-Gruber syndrome in 5.1% cases and Leber congenital amaurosis (1.7%). Of the 35 Joubert syndrome-related genes, 11 were identified in these patients, i.e., CEP290, C5ORF, TCTN1, CC2D2A, RPGRP1L, TCTN3, AHI1, INPP5E, TCTN2, NPHP1, and TMEM237. For the first time, we identified a ciliopathy gene, CCDC28B, as a causal gene in Joubert syndrome in one family. CEP290 accounted for 37.8% cases of pure Joubert syndrome, Joubert syndrome with retinal and renal disease, and Meckel-Gruber syndrome. The p.G1890∗ allele in CEP290 is highly recurrent. Of the six families with Joubert syndrome who had a prenatal diagnosis, one fetus was normal, two were carriers, and three were affected.Conclusions: This is the largest study of Joubert syndrome from India. Although a high degree of locus and allelic heterogeneity was observed, CEP290 variants were the most common among these patients. [ABSTRACT FROM AUTHOR]

Published

2020

44. POLR3A-related spastic ataxia: new mutations and a look into the phenotype.

Author

Infante, Jon, Serrano-Cárdenas, Karla M., Corral‐Juan, Marc, Farré, Xavier, Sánchez, Ivelisse, de Lucas, Enrique M., García, Antonio, Martín-Gurpegui, José Luis, Berciano, José, and Matilla-Dueñas, Antoni

Subjects

*FAMILIAL spastic paraplegia, *ATAXIA, *CEREBELLAR ataxia, *AFFERENT pathways, *PHENOTYPES, *HUMAN chromosome abnormality diagnosis

Abstract

Adolescent-onset spastic ataxia is a proposed novel phenotype in compound heterozygous carriers of an intronic mutation (c.1909 + 22G > A) in the POLR3A gene. Here, we present ten new cases of POLR3A-related spastic ataxia and discuss the genetic, clinical and imaging findings. Patients belonged to six pedigrees with hereditary spastic paraplegia or cerebellar ataxia of unknown origin. All affected subjects presented with compound heterozygous variants, comprising c.1909 + 22G > A in combination in each pedigree with one of the following novel mutations (Thr596Met, Tyr665LeufsTer11, Glu198Ter, c.646-687_1185 + 844del). The new mutations segregated with the phenotype in all families. The phenotype combined variable cerebellar ataxia, gait and lower limb spasticity, involvement of central sensory tracts and in some cases also intention tremor. The reportedly characteristic hyperintensity along the superior cerebellar peduncle on MRI was observed in ~ 80% of the cases. Our study extends the clinical and molecular phenotype further supporting the pathogenic role of the c.1909 + 22G4A intronic mutation and identifying four novel causative mutations in POLR3A-related spastic ataxia. Certain characteristic MRI features may be useful to guide genetic diagnosis. [ABSTRACT FROM AUTHOR]

Published

2020

45. Corrigendum to "NMNAT1 and hereditary spastic paraplegia (HSP): Expanding the phenotypic spectrum of NMNAT1 variants" [Neuromuscular Disorders, 33(2023) 295-301].

Author

Sadr, Zahra, Ghasemi, Aida, Rohani, Mohammad, and Alavi, Afagh

Subjects

*FAMILIAL spastic paraplegia, *NEUROMUSCULAR diseases, *PHENOTYPES

Published

2024

46. Symptomatic Female Spastic Paraplegia Patient with a Novel Heterozygous Variant of the PLP1 Gene.

Author

Ae Ryoung Kim, Yun-Jeong Lee, Mi Hee Kwack, and Jong-Mok Lee

Subjects

*DNA analysis, *PROTEINS, *X-linked genetic disorders, *SEQUENCE analysis, *GENETIC mutation, *GENETIC variation, *FAMILIAL spastic paraplegia, *GENETIC carriers, *GENE expression, *GENOTYPES, *POLYNEUROPATHIES, *NEUROGLIA, *PHENOTYPES

Abstract

A case study of a 47‑year‑old unmarried female presented with gait disturbance and voiding difficulty with a novel heterozygous variant of the PLP1 gene. Topics include somatosensory evoked potential tests showed a central conduction defect in the left median and bilateral tibial nerve stimulations; and using whole‑exome sequencing (WES), we identified a novel heterozygous duplication mutation in PLP1, causing the condition.

Published

2021

47. Parkinsonism and spastic paraplegia type 7: Expanding the spectrum of mitochondrial Parkinsonism.

Author

De la Casa‐Fages, Beatriz, Fernández‐Eulate, Gorka, Gamez, Josep, Barahona‐Hernando, Raúl, Morís, Germán, García‐Barcina, María, Infante, Jon, Zulaica, Miren, Fernández‐Pelayo, Uxoa, Muñoz‐Oreja, Mikel, Urtasun, Miguel, Olaskoaga, Ander, Zelaya, Victoria, Jericó, Ivonne, Saez‐Villaverde, Raquel, Catalina, Irene, Sola, Emma, Martínez‐Sáez, Elena, Pujol, Aurora, and Ruiz, Montserrat

Subjects

*COMPARATIVE studies, *DNA, *RESEARCH methodology, *MEDICAL cooperation, *MITOCHONDRIA, *MITOCHONDRIAL pathology, *GENETIC mutation, *PARAPLEGIA, *RESEARCH, *RESEARCH funding, *PHENOTYPES, *EVALUATION research, *PARKINSONIAN disorders, *FAMILIAL spastic paraplegia

Abstract

Background: Pathogenic variants in the spastic paraplegia type 7 gene cause a complicated hereditary spastic paraplegia phenotype associated with classical features of mitochondrial diseases, including ataxia, progressive external ophthalmoplegia, and deletions of mitochondrial DNA.Objectives: To better characterize spastic paraplegia type 7 disease with a clinical, genetic, and functional analysis of a Spanish cohort of spastic paraplegia type 7 patients.Methods: Genetic analysis was performed in patients suspecting hereditary spastic paraplegia and in 1 patient with parkinsonism and Pisa syndrome, through next-generation sequencing, whole-exome sequencing, targeted Sanger sequencing, and multiplex ligation-dependent probe analysis, and blood mitochondrial DNA levels determined by quantitative polymerase chain reaction.Results: Thirty-five patients were found to carry homozygous or compound heterozygous pathogenic variants in the spastic paraplegia type 7 gene. Mean age at onset was 40 years (range, 12-63); 63% of spastic paraplegia type 7 patients were male, and three-quarters of all patients had at least one allele with the c.1529C>T (p.Ala510Val) mutation. Eighty percent of the cohort showed a complicated phenotype, combining ataxia and progressive external ophthalmoplegia (65% and 26%, respectively). Parkinsonism was observed in 21% of cases. Analysis of blood mitochondrial DNA indicated that both patients and carriers of spastic paraplegia type 7 pathogenic variants had markedly lower levels of mitochondrial DNA than control subjects (228 per haploid nuclear DNA vs. 176 vs. 573, respectively; P < 0.001).Conclusions: Parkinsonism is a frequent finding in spastic paraplegia type 7 patients. Spastic paraplegia type 7 pathogenic variants impair mitochondrial DNA homeostasis irrespective of the number of mutant alleles, type of variant, and patient or carrier status. Thus, spastic paraplegia type 7 supports mitochondrial DNA maintenance, and variants in the gene may cause parkinsonism owing to mitochondrial DNA abnormalities. Moreover, mitochondrial DNA blood analysis could be a useful biomarker to detect at risk families. © 2019 International Parkinson and Movement Disorder Society. [ABSTRACT FROM AUTHOR]

Published

2019

48. VPS53 gene is associated with a new phenotype of complicated hereditary spastic paraparesis.

Author

Hausman-Kedem, Moran, Ben-Shachar, Shay, Menascu, Shay, Geva, Karen, Sagie, Liora, and Fattal-Valevski, Aviva

Subjects

RECESSIVE genes, FAMILIAL spastic paraplegia, MAGNETIC resonance imaging, PHENOTYPES, GENES, LEG, MUSCLE tone

Abstract

Hereditary spastic paraparesis (HSP) is a progressive neurodegenerative disorder, characterized by progressive lower limb weakness and spasticity. Multiple genes are associated with both the pure and complicated HSP types. Our study is aimed at seeking for novel genetic basis of HSP in a family with two affected siblings. Genetic analysis using whole exome sequencing was conducted in a family quartet with two female siblings, who presented with complicated HSP featuring slowly progressive paraparesis, mild-moderate intellectual disability, normal head circumference (HC), and normal magnetic resonance imaging (MRI). A homozygous pathogenic variant was identified in both siblings in the VPS53 gene (c.2084A>G: c.2084A>G, p.Gln695Arg). This gene acts as a component of the Golgi-associated retrograde protein (GARP) complex that is involved, among others, in intracellular cholesterol transport and sphingolipid homeostasis in lysosomes and was previously associated with progressive cerebello-cerebral atrophy (PCCA) type 2. This is the first description of the VPS53 gene as a cause of autosomal recessive complicated HSP. Lysosomal dysfunction as a result of impaired cholesterol trafficking can explain the neurodegenerative processes responsible for the HSP. Our finding expands the phenotype of VPS53-related disease and warrants the addition of VPS53 analysis to the genetic investigation in patients with autosomal recessive HSP. The exact role of GARP complex in neurodegenerative processes should be further elucidated. [ABSTRACT FROM AUTHOR]

Published

2019

49. Late-onset phenotype associated with a homozygous GJC2 missense mutation in a Turkish family.

Author

Kuipers, Demy J.S., Tufekcioglu, Zeynep, Bilgiç, Başar, Olgiati, Simone, Dremmen, Marjolein H.G., van IJcken, Wilfred F.J., Breedveld, Guido J., Mancini, Grazia M.S., Hanagasi, Haşmet A., Emre, Murat, and Bonifati, Vincenzo

Subjects

*MISSENSE mutation, *GTPASE-activating protein, *PHENOTYPES, *LEUKODYSTROPHY, *PARKINSONIAN disorders, *FAMILIES, *FAMILIAL spastic paraplegia, *AGE factors in disease, *ATAXIA, *BRAIN, *COMPARATIVE studies, *GENEALOGY, *GENETIC techniques, *MAGNETIC resonance imaging, *RESEARCH methodology, *MEDICAL cooperation, *MEMBRANE proteins, *GENETIC mutation, *RESEARCH, *EVALUATION research

Abstract

Objective: Recessive mutations in the Gap Junction Protein Gamma 2 (GJC2) gene cause Pelizaeus-Merzbacher-like disease type 1, a severe infantile-onset hypomyelinating leukodystrophy. Milder, late-onset phenotypes including complicated spastic paraplegia in one family (SPG44), and mild tremor in one case, were reported associated to GJC2 homozygous missense mutations. Here, we report a new family with two siblings carrying a different homozygous GJC2 mutation, presenting with late-onset ataxic and pyramidal disturbances, and parkinsonism in one of them.Methods: Two affected siblings were studied by neurological examination and brain MRI. Genetic analyses included genome-wide homozygosity mapping in both siblings, and whole exome sequencing in one sib. The resulting candidate gene variant was validated by Sanger sequencing.Results: The affected siblings share a novel homozygous GJC2 missense mutation (c.820G>C, p.Val274Leu), predicted as pathogenic by all used in-silico tools. Brain MRI showed hyperintense signal in T2-weighted images in the internal capsule and subcortical and periventricular white matter, consistent with hypomyelination.Conclusions: Our findings confirm and further expand the late-onset phenotypes of GJC2 mutations, to include prominent ataxia, pyramidal disturbances and mild parkinsonism, and confirm the distinctive associated MRI pattern. [ABSTRACT FROM AUTHOR]

Published

2019

50. Novel Compound Heterozygous SACS Mutations in a Case with a Spasticity-Lacking Phenotype of Sacsin-Related Ataxia.

Author

Chen, You, Cen, Zhidong, Zheng, Xiaosheng, Chen, Si, Xie, Fei, and Luo, Wei

Subjects

*PHENOTYPES, *ATAXIA, *SPINOCEREBELLAR ataxia, *MUSCULAR atrophy, *GENETIC testing, *FAMILIAL spastic paraplegia, *RESEARCH, *GENETIC mutation, *RESEARCH methodology, *MEDICAL cooperation, *EVALUATION research, *SPASTICITY, *COMPARATIVE studies

Abstract

Dear Editors, Autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS, MIM#270550) is an inherited neurodegenerative disorder first described among French Canadians in the Charlevoix-Saguenay region of Quebec, with a homogeneous clinical picture characterized by a triad of early-onset cerebellar ataxia, peripheral neuropathy, and lower limb spasticity.[1] Here, we report a case caused by novel compound heterozygous SACS mutations, presenting without lower limb spasticity, usually a core feature of ARSACS. Cosegregation analysis [Figure 1]a suggests that the two mutations were located in trans.{Table 1} Our case does not present with lower limb spasticity, usually a core feature of ARSACS. Whole exome sequencing identified two novel heterozygous mutations in the gene SACS (NM 014363) - one frameshift mutation (c.10685 10689del, p.F3562*) and one missense mutation (c.8000T>C, p.F2667S) [Figure 1]b. [Extracted from the article]

Published

2021