Your search keyword '"FAMILIAL spastic paraplegia"' showing total 41 results

1. A case report of concurrent occurrence of two inherited axonopathies within a family: the benefit of whole-exome sequencing.

Author

Sadr, Zahra, Rohani, Mohammad, Jamali, Payman, and Alavi, Afagh

Subjects

*FAMILIAL spastic paraplegia, *GENETIC variation, *NERVE conduction studies, *GENETIC counseling, *SYMPTOMS

Abstract

Mutations in ERLIN2 and MFN2 lead to the development of spastic paraplegia-18 (SPG18) and Charcot–Marie–Tooth type-2A (CMT2A), respectively. These disorders are unified by the fact that both can be termed inherited axonopathies. With whole-exome sequencing (WES), more patients of neurological disorders with clinical overlaps receive a genetic result than ever before. This study describes an Iranian family who harbor mutations in ERLIN2 and MFN2, simultaneously. The proband was a 73-year old man who has experienced weakness and spasticity of lower limbs since late childhood. He was diagnosed with hereditary spastic paraplegia (HSP). His WES identified a novel homozygous variant in ERLIN2 as well as a known heterozygous variant in MFN2. These variants were cosegregated with the phenotypes among the family members. His sister with a similar phenotype just carried the homozygous ERLIN2 variant, whereas, his asymptomatic brother and daughter carried the heterozygous variant of MFN2. Re-evaluation of the MFN2 variant carriers by nerve conduction study revealed that only the proband's daughter has peripheral neuropathy. Herein, using WES two distinct disease-causing variants with different modes of inheritance in ERLIN2 and MFN2 were detected in the proband. As expected, individuals with a defined MFN2 variant, p.Arg468His, were asymptomatic or had a mild phenotype. The co-occurrence of such diseases, SPG18 and CMT2A, may result in the milder phenotype to be overlooked or its features considered as a part of the symptoms of other disease. Certainly, providing genetic counseling in such cases can be challenging. These cases reveal the importance of WES. [ABSTRACT FROM AUTHOR]

Published

2024

2. DDHD2 promotes lipid droplet catabolism by acting as a TAG lipase and a cargo receptor for lipophagy.

Author

Gao, Kun, Jia, Fei, Li, Yao, and Wang, Chenji

Subjects

FAMILIAL spastic paraplegia, NEURODEGENERATION, CATABOLISM, THERAPEUTICS, PARAPLEGIA, LIPASES

Abstract

Mutations in the DDHD2 (DDHD domain containing 2) gene cause autosomal recessive spastic paraplegia type 54 (SPG54), a rare neurodegenerative disorder characterized by the early childhood onset of progressive spastic paraplegia. DDHD2 is reported as the principal brain triacylglycerol (TAG) lipase whose dysfunction causes massive lipid droplet (LD) accumulation in the brains of SPG54 patients. However, the precise functions of DDHD2 in regulating LD catabolism are not yet fully understood. In a recent study, we demonstrate that DDHD2 interacts with multiple members of the Atg8-family proteins (MAP1LC3/LC3s, GABARAPs), which play crucial roles in lipophagy. DDHD2 possesses two LC3-interacting region (LIR) motifs that contribute to its LD-eliminating activity. Moreover, DDHD2 enhances the colocalization between LC3B and LDs to promote lipophagy. LD·ATTEC, a compound that tethers LC3 to LDs to enhance their macroautophagic/autophagic clearance, effectively counteracts DDHD2 deficiency-induced LD accumulation. These findings provide insights into the dual functions of DDHD2 as a TAG lipase and cargo receptor for lipophagy in neuronal LD catabolism, and also suggest a potential therapeutic approach for treating SPG54 patients. [ABSTRACT FROM AUTHOR]

Published

2024

3. Multimodal and longitudinal evaluation of novel phenotype-genotype correlation of CLN3 isolated retinal degeneration in an hispanic female with heterozygous mutations c.944dup and c.1305C>G.

Author

Garza-Garza, Lucas A., Villarreal-Martinez, Priscila, Villafuerte-de la Cruz, Rocio, and Garza-Leon, Manuel

Subjects

*HISPANIC American women, *RETINAL degeneration, *RETINAL diseases, *GENETIC variation, *VISUAL fields, *FAMILIAL spastic paraplegia, *NEMALINE myopathy

Abstract

Inherited retinal disorders (IRDs) are a complex group of heritable diseases which are characterized by rod, cone, retinal pigment epithelium, or optic nerve dysfunction. Recently, mutations in CLN3 have also been associated with isolated IRDs. Herein, a case with heterozygous CLN3 variations that had not been previously linked to a CLN3-isolated retinal degeneration (CLN3IRD) phenotype in a Hispanic female and its multimodal imaging findings across a 10-year follow-up are presented. An observational, prospective, case report on a hispanic female with CLN3IRD is presented. Patients underwent genetic testing and color fundus photography (CFC) and autofluorescence (FAF), fluorescein angiography (FA), Spectral domain optical coherence tomography (OCT) of the macular area, electroretinogram (ERG) and 30–2 visual field examination through automated perimetry. A female, aged 24, affected by CLN3IRD phenotype from c.944dup and c.1305C>G compound heterozygous variants, presented with bilateral hypopigmentary changes in the macular area of OU with that corresponded to hyporautofluorescent deposits in the macular area on FAF. An atrophic maculopathy was evident on structural OCT, and FA disclosed a symmetrical macular hyperflourescence with staining in the early and late stages in OU. Humphrey visual field testing showed a marked reduction of the central visual field in OU. Electrophysiological testing revealed an ERG with markedly decreased a and b waves in OU. In ten years follow up developed of bone spiculae in the midperipheral retina. We reported a patient with a novel CLN3IRD severe phenotype associated with the variants c.944dup and c.1305C>G, which had previously only been associated with JCNL. [ABSTRACT FROM AUTHOR]

Published

2024

4. Epigenetic regulation of autophagy-related genes: Implications for neurodevelopmental disorders.

Author

Lewerissa, Elly I., Nadif Kasri, Nael, and Linda, Katrin

Subjects

CYTOSINE, GENETIC regulation, HISTONES, INDUCED pluripotent stem cells, FAMILIAL spastic paraplegia, TUBULINS, EPIGENETICS, HOMEOBOX genes, EPIGENOMICS

Abstract

Macroautophagy/autophagy is an evolutionarily highly conserved catabolic process that is important for the clearance of cytosolic contents to maintain cellular homeostasis and survival. Recent findings point toward a critical role for autophagy in brain function, not only by preserving neuronal health, but especially by controlling different aspects of neuronal development and functioning. In line with this, mutations in autophagy-related genes are linked to various key characteristics and symptoms of neurodevelopmental disorders (NDDs), including autism, micro-/macrocephaly, and epilepsy. However, the group of NDDs caused by mutations in autophagy-related genes is relatively small. A significant proportion of NDDs are associated with mutations in genes encoding epigenetic regulatory proteins that modulate gene expression, so-called chromatinopathies. Intriguingly, several of the NDD-linked chromatinopathy genes have been shown to regulate autophagy-related genes, albeit in non-neuronal contexts. From these studies it becomes evident that tight transcriptional regulation of autophagy-related genes is crucial to control autophagic activity. This opens the exciting possibility that aberrant autophagic regulation might underly nervous system impairments in NDDs with disturbed epigenetic regulation. We here summarize NDD-related chromatinopathy genes that are known to regulate transcriptional regulation of autophagy-related genes. Thereby, we want to highlight autophagy as a candidate key hub mechanism in NDD-related chromatinopathies. Abbreviations: ADNP: activity dependent neuroprotector homeobox; ASD: autism spectrum disorder; ATG: AutTophaGy related; CpG: cytosine-guanine dinucleotide; DNMT: DNA methyltransferase; EHMT: euchromatic histone lysine methyltransferase; EP300: E1A binding protein p300; EZH2: enhancer of zeste 2 polycomb repressive complex 2 subunit; H3K4me3: histone 3 lysine 4 trimethylation; H3K9me1/2/3: histone 3 lysine 9 mono-, di-, or trimethylation; H3K27me2/3: histone 3 lysine 27 di-, or trimethylation; hiPSCs: human induced pluripotent stem cells; HSP: hereditary spastic paraplegia; ID: intellectual disability; KANSL1: KAT8 regulatory NSL complex subunit 1; KAT8: lysine acetyltransferase 8; KDM1A/LSD1: lysine demethylase 1A; MAP1LC3B: microtubule associated protein 1 light chain 3 beta; MTOR: mechanistic target of rapamycin kinase; MTORC1: mechanistic target of rapamycin complex 1; NDD: neurodevelopmental disorder; PHF8: PHD finger protein 8; PHF8-XLID: PHF8-X linked intellectual disability syndrome; PTM: post-translational modification; SESN2: sestrin 2; YY1: YY1 transcription factor; YY1AP1: YY1 associated protein 1 [ABSTRACT FROM AUTHOR]

Published

2024

5. Atl (atlastin) regulates mTor signaling and autophagy in Drosophila muscle through alteration of the lysosomal network.

Author

Srivastav, Saurabh, van der Graaf, Kevin, Singh, Pratibha, Utama, Alloysius Budi, Meyer, Matthew D., McNew, James A., and Stern, Michael

Subjects

FAMILIAL spastic paraplegia, GREEN fluorescent protein, AUTOPHAGY, DROSOPHILA, FLUORESCENT proteins, UBIQUITINATION

Abstract

The hereditary spastic paraplegias (HSPs) represent a family of genetic disorders comprising at least 72 different genes with the common pathology of progressive locomotor deficits and spasticity. ATL1/SPG3A (atlastin GTPase 1) encodes an ER fusion protein that controls ER morphology, which implicates ER structure as a causal factor in HSP. Here we use Drosophila to study effects of decreased atl (atlastin) on properties of the larval body wall muscle. We found that muscle atl loss causes accumulation of aggregates containing polyubiquitin (polyUB), mostly bound to the autophagy receptor ref(2)P/SQSTM1/p62. Muscle atl loss also decreased volume and complexity of the endolysosomal network and decreased lysosome number. To determine effects of these lysosomal deficits on progression through the basal autophagy pathway, we expressed Atg8a tagged with both GFP and mCherry in a wild-type and atl mutant background. We found numerous structures containing mCherry but not GFP fluorescence in wild type, indicating that Atg8a was found mostly in mature autolysosomes. In contrast, muscles lacking atl exhibited significant amounts of GFP signal, indicating failure of autophagosome maturation with acidic lysosomes. Many of these GFP-positive puncta contained the late-endosome marker Rab7 but not Lamp1, indicating that some autophagy cargo was accumulating within amphisomes. We also found that this autophagy block was accompanied by an inability to activate the mTor kinase. Our results provide mechanistic insights into the role of atl in maintaining proper function of the autophagy pathway and suggests that certain pathologies in patients with mutations in ATL1/SPG3A might result from altered MTOR signaling. atl atlastin; ALR autophagic lysosome reformation; ER endoplasmic reticulum; GFP green fluorescent protein; HSP hereditary spastic paraplegia; Lamp1 lysosomal associated membrane protein 1 PolyUB polyubiquitin; RFP red fluorescent protein; spin spinster; mTor mechanistic Target of rapamycin; VCP valosin containing protein [ABSTRACT FROM AUTHOR]

Published

2024

6. Disrupted endoplasmic reticulum-mediated autophagosomal biogenesis in a Drosophila model of C9-ALS-FTD.

Author

Sung, Hyun and Lloyd, Thomas E.

Subjects

TRP channels, MOTOR neuron diseases, AMYOTROPHIC lateral sclerosis, FRONTOTEMPORAL dementia, FAMILIAL spastic paraplegia, DROSOPHILA, ENDOPLASMIC reticulum, MOTOR neurons

Abstract

Macroautophagy/autophagy is a major pathway for the clearance of protein aggregates and damaged organelles, and multiple intracellular organelles participate in the process of autophagy, from autophagosome formation to maturation and degradation. Dysregulation of the autophagy pathway has been implicated in the pathogenesis of neurodegenerative diseases including amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD), however the mechanisms underlying autophagy impairment in these diseases are incompletely understood. Since the expansion of GGGGCC (G4C2) repeats in the first intron of the C9orf72 gene is the most common inherited cause of both ALS and FTD (C9-ALS-FTD), we investigated autophagosome dynamics in Drosophila motor neurons expressing 30 G4C2 repeats (30 R). In vivo imaging demonstrates that expression of expanded G4C2 repeats markedly impairs biogenesis of autophagosomes at synaptic termini, whereas trafficking and maturation of axonal autophagosomes are unaffected. Motor neurons expressing 30 R display marked disruption in endoplasmic reticulum (ER) structure and dynamics in the soma, axons, and synapses. Disruption of ER morphology with mutations in Rtnl1 (Reticulon-like 1) or atl (atlastin) also impairs autophagosome formation in motor neurons, suggesting that ER integrity is critical for autophagosome formation. Furthermore, live imaging demonstrates that autophagosomes are generated from dynamic ER tubules at synaptic boutons, and this process fails to occur in a C9-ALS-FTD model. Together, these findings suggest that dynamic ER tubules are required for formation of autophagosomes at the neuromuscular junction, and that this process is disrupted by expanded G4C2 repeats that cause ALS-FTD. 3R: UAS construct expressing 3 G4C2 repeats (used as control); 3WJ: three-way junction; 12R: UAS construct expressing leader sequence and 12 G4C2 repeats; 30R: UAS construct expressing 30 G4C2 repeats; 36R: UAS construct expressing 36 G4C2 repeats; 44R: UAS construct expressing leader sequence and 44 G4C2 repeats; ALS: amyotrophic lateral sclerosis; Atg: autophagy related; atl: atlastin; C9-ALS-FTD: ALS or FTD caused by hexanuleotide repeat expansion in C9orf72; ER: endoplasmic reticulum; FTD: frontotemporal dementia; HRE: GGGGCC hexanucleotide repeat expansion; HSP: hereditary spastic paraplegia; Lamp1: lysosomal associated membrane protein 1; MT: microtubule; NMJ: neuromuscular junction; Rab: Ras-associated binding GTPase; RAN: repeat associated non-AUG (RAN) translation; RO-36: UAS construct expression "RNA-only" version of 36 G4C2 repeats in which stop codons in all six reading frames are inserted.; Rtnl1: Reticulon-like 1; SN: segmental nerve; TFEB/Mitf: transcription factor EB/microphthalmia associated transcription factor (Drosophila ortholog of TFEB); TrpA1: transient receptor potential cation channel A1; VAPB: VAMP associated protein B and C; VNC: ventral nerve cord (spinal cord in Drosophila larvae) [ABSTRACT FROM AUTHOR]

Published

2024

7. Expanding the spectrum of KIF5A mutations—case report of a large kindred with familial ALS and overlapping syndrome.

Author

Dulski, JarosŁaw, Strongosky, Audrey J., Al-Shaikh, Rana Hanna, and Wszolek, Zbigniew K.

Subjects

*CHARCOT-Marie-Tooth disease, *FAMILIAL spastic paraplegia, *SPASTICITY, *AMYOTROPHIC lateral sclerosis, *FRIEDREICH'S ataxia, *FRONTOTEMPORAL dementia, *GENETIC testing

Abstract

This paper presents the first report of amyotrophic lateral sclerosis (ALS) kindred due to the KIF5A p.Arg1007Lys, a splice-altering variant. An index case was a 54-year-old male who developed progressive gait difficulty and imbalance followed by mild parkinsonism, spasticity, neuropathy, ataxia, and cognitive impairment with predominant subcortical frontal involvement. Brain MRI showed marked bilateral parietal lobes atrophy. Electromyography demonstrated chronic diffuse neurogenic changes. Due to the positive history of similar symptoms in his father and the diagnosis of ALS in 10 other family members, extensive genetic testing was pursued. Genetic screening for GRN, C9orf72, TARDBP, SOD1, FUS, MAPT mutations, and hereditary ataxia panel, was unremarkable. Whole-exome sequencing revealed c.3020G > A (p.Arg1007Lys) mutation in the KIF5A gene, later confirmed in two affected relatives. Similar to previous reports on KIF5A-related ALS, our index case, had a mild disease course with prolonged survival. However, as the rate of progression and survival time differed even among the same family members, other factors were probably at play. Additionally, our index case and his father displayed features overlapping ALS, spastic paraplegia, Charcot-Marie-Tooth disease type 2, and frontotemporal dementia. Therefore, we suggest considering KIF5A mutations in the differential diagnosis, particularly in the presence of overlapping features of spasticity, neuropathy, cerebellar ataxia, and dementia. [ABSTRACT FROM AUTHOR]

Published

2023

8. Autophagic lysosome reformation in health and disease.

Author

Nanayakkara, Randini, Gurung, Rajendra, Rodgers, Samuel J., Eramo, Matthew J., Ramm, Georg, Mitchell, Christina A., and McGrath, Meagan J.

Subjects

LYSOSOMES, FAMILIAL spastic paraplegia, REFORMATION, MUSCULAR dystrophy, CHARCOT-Marie-Tooth disease, URODYNAMICS, PARKINSON'S disease

Abstract

Lysosomes are the primary degradative compartment within cells and there have been significant advances over the past decade toward understanding how lysosome homeostasis is maintained. Lysosome repopulation ensures sustained autophagy function, a fundamental process that protects against disease. During macroautophagy/autophagy, cellular debris is sequestered into phagophores that mature into autophagosomes, which then fuse with lysosomes to generate autolysosomes in which contents are degraded. Autophagy cannot proceed without the sufficient generation of lysosomes, and this can be achieved via their de novo biogenesis. Alternatively, during autophagic lysosome reformation (ALR), lysosomes are generated via the recycling of autolysosome membranes. During this process, autolysosomes undergo significant membrane remodeling and scission to generate membrane fragments, that mature into functional lysosomes. By utilizing membranes already formed during autophagy, this facilitates an efficient pathway for re-deriving lysosomes, particularly under conditions of prolonged autophagic flux. ALR dysfunction is emerging as an important disease mechanism including for neurodegenerative disorders such as hereditary spastic paraplegia and Parkinson disease, neuropathies including Charcot-Marie-Tooth disease, lysosome storage disorders, muscular dystrophy, metabolic syndrome, and inflammatory and liver disorders. Here, we provide a comprehensive review of ALR, including an overview of its dynamic spatiotemporal regulation by MTOR and phosphoinositides, and the role ALR dysfunction plays in many diseases. [ABSTRACT FROM AUTHOR]

Published

2023

9. Clinical, electrophysiological, and genetic characteristics of cerebrotendinous xanthomatosis in South Korea.

Author

Kim, Sunyoung, Park, Jin-Sung, Lee, Jae-Hyeok, Shin, Ha-Young, Yang, Hui-Jun, and Shin, Jin-Hong

Subjects

*LIPIDOSES, *DELAYED diagnosis, *NEURODEGENERATION, *ELECTROPHYSIOLOGY, *AGE of onset, *RECESSIVE genes, *FAMILIAL spastic paraplegia

Abstract

Cerebrotendinous xanthomatosis (CTX) is an autosomal recessive lipid storage disorder caused by 27-hydroxylase deficiency. We report the clinical characteristics of six Korean CTX patients. The median age of onset was 22.5 years, the median age at diagnosis was 42 years, and the diagnostic delay was 18.1 years. The most common clinical symptoms were tendon xanthoma and spastic paraplegia. Four of five patients exhibited latent central conduction dysfunction. All patients carried the same mutation in CYP27A1 (c.1214 G>A [p.R405Q]). CTX is a treatable neurodegenerative disorder; however, our results revealed that patients with CTX in Korea might receive the diagnosis after a prolonged delay. [ABSTRACT FROM AUTHOR]

Published

2022

10. Theme 02 - Genetics and Genomics.

Author

Becattini, L., Bianchi, F., Fontanelli, L., Fogli, A., Siciliano, G., Bombaci, A., Manera, U., Canosa, A., Grassano, M., Palumbo, F., De Marco, G., Casale, F., Salamone, P. P., Fuda, G., Marchese, G., Moglia, C., Chiò, A., Gallone, S., Calvo, A., and Brown, F.

Subjects

*GENETICS, *AMYOTROPHIC lateral sclerosis, *GENOMICS, *NICOTINIC acetylcholine receptors, *NEUROTROPHIN receptors, *MEDICAL genetics, *FAMILIAL spastic paraplegia

Abstract

Rare missense variants of neuronal nicotinic acetylcholine receptor altering receptor function are associated with sporadic amyotrophic lateral sclerosis. 1996; 47 (2): 535 - 40. 33 Okada Y, Yamazaki H, Sekine-Aizawa Y, Hirokawa N. The neuron-specific kinesin superfamily protein KIF1A is a unique monomeric motor for anterograde axonal transport of synaptic vesicle precursors. Common and rare variant association analyses in amyotrophic lateral sclerosis identify 15 risk loci with distinct genetic architectures and neuron-specific biology. [Extracted from the article]

Published

2022

11. A de novo c.113 T > C: p.L38R mutation of SPTLC1: case report of a girl with sporadic juvenile amyotrophic lateral sclerosis.

Author

Liu, Xiaoxuan, He, Ji, Yu, Weiyi, and Fan, Dongsheng

Subjects

*AMYOTROPHIC lateral sclerosis, *FAMILIAL spastic paraplegia, *GENETIC variation, *SYMPTOMS, *GENETIC mutation, *METABOLIC disorders

Abstract

SPTLC1 has been implicated in hereditary sensory and autonomic neuropathy type 1 (HSAN1) and macular telangiectasia type2. Recent studies have reported mutations in SPLTC1 may cause juvenile amyotrophic lateral sclerosis (JALS), especially in the first transmembrane domain of SPTLC1(exon 2). In this study, we identified a novel heterozygous variant in exon 2, c.113 T > C: p. Leu38Arg, of SPTLC1 in a 12-year-old girl with sporadic JALS who experienced early-childhood-onset lower extremity spasticity followed by slowly progressive lower motor weakness and atrophy without sensory symptoms or signs. SPLTC1 is the first monogenic lipid metabolic disturbance that has been linked to ALS. The variant in exon 2 may impact on negative regulation of sphingolipid biosynthesis. [ABSTRACT FROM AUTHOR]

Published

2022

12. Clinical and molecular characterization of hereditary spastic paraplegia in a spanish Southern region.

Author

Salas, P. Carrasco, Fernández, E. Martínez, Méndez del Barrio, C., Mira, A. Serrano, Moreno, N. Guerrero, Royo, I., Delgado, M., Oropesa, J. M., and Vázquez Rico, I.

Subjects

*FAMILIAL spastic paraplegia, *SCIENTIFIC knowledge, *GENETIC variation, *GENE families, *TECHNOLOGICAL innovations, *SYMPTOMS

Abstract

Introduction: Spastic paraplegia (SPG) is a syndrome characterised by lower limb spasticity, occurring alone or in association with other neurological manifestations. Despite of the new molecular technologies, many patients remain yet undiagnosed. Objective: The purpose of this study was to describe the clinical presentation and molecular characteristics of a cohort of 27 patients from 18 different families with SPG in the south of Spain. Methods: We used a targeted next-generation sequencing (NGS) approach to study a proband from each family. Results: Variants in SPG11 gene were the most common cause of SPG in our area. We made a genetic diagnosis in 52% of cases, identified 3 novel variants and reclassified one uncertain variant in SPG11 gene as pathogenic variant. We identified a patient with two truncanting mutations in SPG11 gene and late onset disease and report another missense mutation outside of motor domain of KIF1A gene in a family with pure SPG. Conclusion: Our study contributes to enhance the scientific knowledge of SPG. It is important to note the large group of cases (48%) that were not genetically diagnosed in our cohort. Therefore NGS approach is an efficient diagnostic tool, but it still large the number of non-diagnosed subjects, suggesting further genetic heterogeneity. [ABSTRACT FROM AUTHOR]

Published

2022

13. SPG11: clinical and genetic features of seven Czech patients and literature review.

Author

Doleckova, Kristyna, Roth, Jan, Stellmachova, Julia, Gescheidt, Tomas, Sigut, Vladimir, Houska, Pavel, Jech, Robert, Zech, Michael, Vyhnalek, Martin, Vyhnalkova, Emilie, Seeman, Pavel, and Meszarosova, Anna Uhrova

Subjects

FAMILIAL spastic paraplegia, CZECHS, LITERATURE reviews, MISSENSE mutation, CORPUS callosum, AGE of onset, WALKING speed

Abstract

SPG11 is one of the most frequent autosomal recessively inherited types of hereditary spastic paraplegias (HSP or SPG). We describe the first seven patients from the Czech Republic with biallelic pathogenic variants in the SPG11. The typical HSP neurological findings are present in all the described patients in that the signs of a complicated phenotype develop slowly. The speed of disease progression, and the severity of gait impairment, was fast in all patients but the phenotype varied from patient to patient. Thin corpus callosum was not observed in two patients. Two Czech SPG11 patients had unusual late onset of disease and both were compound heterozygotes for the c.5381T>C variant. Therefore, we looked for a potential ralationship between the type of variant in the SPG11 gene and the age of disease onset. By reviewing all described SPG11 patients carrying at least one missense pathogenic variant in the SPG11 gene we did not found any relationship between the age of onset and the type of variant. Together twelve pathogenic variants, including gross deletions, were found in the SPG11 gene the Czech SPG11 patients, the c.3454-2A>G variant is novel. [ABSTRACT FROM AUTHOR]

Published

2022

14. Novel insights into the genetic profile of hereditary spastic paraplegia in India.

Author

Narendiran, Sundarapandian, Debnath, Monojit, Shivaram, Sumanth, Kannan, Ramakrishnan, Sharma, Shivani, Christopher, Rita, Seshagiri, Doniparthi V., Jain, Sanjeev, Purushottam, Meera, Mangalore, Sandhya, Bharath, Rose Dawn, Bindu, Parayil Sankaran, Sinha, Sanjib, Taly, Arun B., and Nagappa, Madhu

Subjects

*FAMILIAL spastic paraplegia, *GENETIC profile, *CEREBRAL atrophy, *CORPUS callosum, *GENETIC variation, *PYRAMIDAL tract

Abstract

The Hereditary Spastic Paraplegias (HSPs) are a group of clinically and genetically heterogeneous disorders characterized by length dependent degeneration of the corticospinal tracts. Genetic data related to HSPs are limited from India. We aimed to comprehensively analyse the phenotypic characteristics and genetic basis of a large cohort of HSP from India. Patients with HSP phenotype were evaluated for their clinical features, electrophysiological and radiological abnormalities. Genetic analyses were carried out by clinical exome sequencing (n = 52) and targeted sequencing (n = 5). The cohort comprised of 57 probands (M:F 40:17, age: 3.5–49 years). Based on the phenotype, the cohort could be categorized as 'pure' (n = 15, 26.3%) and 'complicated' (n = 42, 73.7%) HSP. Brain MRI showed thin corpus callosum (n = 10), periventricular hyperintensities (n = 20), cerebral atrophy (n = 3), cerebellar atrophy (n = 3) and diffuse atrophy (n = 4). Sixty-seven variants representing 40 genes were identified including 47 novel variants. Forty-eight patients (84.2%) had variants in genes previously implicated in HSP and other spastic paraplegia syndromes (SPG genes = 24, non-SPG genes = 24); among these 13 had variations in more than one gene and 12 patients (21.0%) had variations in genes implicated in potentially treatable/modifiable metabolic disorders (MTHFR = 8, MTRR = 1, ARG1 = 2 and ABCD1 = 1). In nine patients, no genetic variants implicated in spastic paraplegia phenotype were identified. Thus, the present study from India highlights the phenotypic complexities and spectrum of genetic variations in patients with HSP including those implicated in metabolically modifiable disorders. It sets a platform for carrying out functional studies to validate the causal role of the novel variants and variants of uncertain significance. [ABSTRACT FROM AUTHOR]

Published

2022

15. Maternal Germline Mosaicism of a de Novo TUBB2B Mutation Leads to Complex Cortical Dysplasia in Two Siblings.

Author

Çitli, Şenol and Serdaroglu, Esra

Subjects

*MOSAICISM, *SIBLINGS, *GERM cells, *DNA analysis, *SINGLE nucleotide polymorphisms, *PARTIAL epilepsy, *FAMILIAL spastic paraplegia

Abstract

Introduction: Complex cortical dysplasia with other brain malformations-7 (a.k.a. polymicrogyria) caused by mutations in TUBB2B gene is a clinically heterogeneous condition. Case report: We report two siblings with polymicrogyria. Brain MRI showed polymicrogyria, small brainstem, thin corpus callosum and fused basal ganglia. Karyotypes and chromosomal microarray analysis were normal. By whole exome sequencing, there were a de novo variant of c.728C > T (p.P243L) in both siblings and a common single nucleotide polymorphism (SNP) (c.718C > T) in both siblings and the mother. Seminal DNA analysis obtained from father was normal. Conclusion: Maternal germline mosaicism was considered because the sequencing result of the father's sperm was normal, two siblings had the same disease, and both patients and mother had the same SNP. [ABSTRACT FROM AUTHOR]

Published

2022

16. Corticospinal tract and motor cortex degeneration in pure hereditary spastic paraparesis type 4 (SPG4).

Author

Navas-Sánchez, Francisco J., Martín De Blas, Daniel, Fernández-Pena, Alberto, Alemán-Gómez, Yasser, Lage-Castellanos, Agustín, Marcos-Vidal, Luis, Guzmán-De-Villoria, Juan A., Catalina, Irene, Lillo, Laura, Muñoz-Blanco, José L., -Ugalde, Andrés Ordoñez, Quintáns, Beatriz, Sobrido, María-Jesús, Carmona, Susanna, Grandas, Francisco, and Desco, Manuel

Subjects

*FAMILIAL spastic paraplegia, *EFFERENT pathways, *PYRAMIDAL tract, *MOTOR cortex, *MOTOR neurons, *WHITE matter (Nerve tissue)

Abstract

Objective: SPG4 is an autosomal dominant pure form of hereditary spastic paraplegia (HSP) caused by mutations in the SPAST gene. HSP is considered an upper motor neuron disorder characterized by progressive retrograde degeneration, or "dying-back" phenomenon, of the corticospinal tract's longest axons. Neuroimaging studies mainly focus on white matter changes and, although previous studies reported cortical thinning in complicated HSP forms, cortical changes remain unclear in SPG4 patients. This work aimed to compare changes in white matter microstructure and cortical thickness between 12 SPG4 patients and 22 healthy age-matched controls. We also explore whether white matter alterations are related to cortical thickness and their correlation with clinical symptoms. Methods: we used fixel-based analysis, an advanced diffusion-weighted imaging technique, and probabilistic tractography of the corticospinal tracts. We also analyzed cortical morphometry using whole-brain surface-based and atlas-based methods in sensorimotor areas. Results: SPG4 patients showed bilateral involvement in the corticospinal tracts; this was more intense in the distal portion than in the upper segments and was associated with the degree of clinical impairment. We found a significant correlation between disease severity and fiber density and cross-section of the corticospinal tracts. Furthermore, corticospinal tract changes were significantly correlated with bilateral cortical thinning in the precentral gyrus in SPG4 patients. Conclusions: Our data point to axonal damage of the corticospinal motor neurons in SPG4 patients might be related to cortical thinning in motor regions. [ABSTRACT FROM AUTHOR]

Published

2022

17. The expanding clinical and genetic spectrum of alsin-related disorders: the first cohort of Brazilian patients.

Author

Alves De Siqueira Carvalho, Alzira, Antônio Troccoli Chieia, Marco, Braga Farias, Igor, Bulle Oliveira, Acary Souza, Pinto, Wladimir Bocca Vieira De Rezende, and Souza, Paulo Victor Sgobbi De

Subjects

*FAMILIAL spastic paraplegia, *AMYOTROPHIC lateral sclerosis, *MOTOR neurons, *NEURODEGENERATION, *MOVEMENT disorders, *AGE of onset

Abstract

There are three types of autosomal recessive disorders involving pathogenic variants in the ALS2 gene (OMIM*606352), infantile ascending hereditary spastic paraplegia (IAHSP), juvenile primary lateral sclerosis (JPLS) and juvenile amyotrophic lateral sclerosis (JALS), which are rare and related to retrograde degeneration of motor neurons. ALS2 pathogenic variants are distributed widely across the entire coding sequence and mostly result in a loss of protein function. Rarely, patients with JALS have been reported with lower motor neuron involvement. Here, we report the first Brazilian cohort (six patients) of JPLS with novel ALS2 pathogenic variants, and we propose an expanding clinical and genetic spectrum of alsin-related disorders. A review of the literature in PubMed from 2001 to September 2020 allowed us to identify 26 publications about the three different phenotypes caused by ALS2 variants (only case reports or families), encompassing 35 nonrelated families. We compiled data (sex, age, age at onset, first symptoms, atypical clinical features, molecular data, and clinical evolution (improvement or death)) from these studies and analyzed them in a general context on the basis of demographic features. [ABSTRACT FROM AUTHOR]

Published

2022

18. 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

19. Mouse models for hereditary spastic paraplegia uncover a role of PI4K2A in autophagic lysosome reformation.

Author

Khundadze, Mukhran, Ribaudo, Federico, Hussain, Adeela, Stahlberg, Henry, Brocke-Ahmadinejad, Nahal, Franzka, Patricia, Varga, Rita-Eva, Zarkovic, Milena, Pungsrinont, Thanakorn, Kokal, Miriam, Ganley, Ian G., Beetz, Christian, Sylvester, Marc, and Hübner, Christian A.

Subjects

FAMILIAL spastic paraplegia, LABORATORY mice, GREEN fluorescent protein, FLUORESCENT proteins, PHYSIOLOGIC salines, MEMBRANE proteins, PHOSPHOINOSITIDES, ANAPLASTIC lymphoma kinase

Abstract

Hereditary spastic paraplegia (HSP) denotes genetically heterogeneous disorders characterized by leg spasticity due to degeneration of corticospinal axons. SPG11 and SPG15 have a similar clinical course and together are the most prevalent autosomal recessive HSP entity. The respective proteins play a role for macroautophagy/autophagy and autophagic lysosome reformation (ALR). Here, we report that spg11 and zfyve26 KO mice developed motor impairments within the same course of time. This correlated with enhanced accumulation of autofluorescent material in neurons and progressive neuron loss. In agreement with defective ALR, tubulation events were diminished in starved KO mouse embryonic fibroblasts (MEFs) and lysosomes decreased in neurons of KO brain sections. Confirming that both proteins act in the same molecular pathway, the pathologies were not aggravated upon simultaneous disruption of both. We further show that PI4K2A (phosphatidylinositol 4-kinase type 2 alpha), which phosphorylates phosphatidylinositol to phosphatidylinositol-4-phosphate (PtdIns4P), accumulated in autofluorescent deposits isolated from KO but not WT brains. Elevated PI4K2A abundance was already found at autolysosomes of neurons of presymptomatic KO mice. Immunolabelings further suggested higher levels of PtdIns4P at LAMP1-positive structures in starved KO MEFs. An increased association with LAMP1-positive structures was also observed for clathrin and DNM2/dynamin 2, which are important effectors of ALR recruited by phospholipids. Because PI4K2A overexpression impaired ALR, while its knockdown increased tubulation, we conclude that PI4K2A modulates phosphoinositide levels at autolysosomes and thus the recruitment of downstream effectors of ALR. Therefore, PI4K2A may play an important role in the pathogenesis of SPG11 and SPG15. Abbreviations: ALR: autophagic lysosome reformation; AP-5: adaptor protein complex 5; BFP: blue fluorescent protein; dKO: double knockout; EBSS: Earle's balanced salt solution; FBA: foot base angle; GFP: green fluorescent protein; HSP: hereditary spastic paraplegia; KO: knockout; LAMP1: lysosomal-associated membrane protein 1; MAP1LC3B/LC3: microtubule-associated protein 1 light chain 3 beta; MEF: mouse embryonic fibroblast; SQSTM1/p62: sequestosome 1; PI4K2A: phosphatidylinositol 4-kinase type 2 alpha; PtdIns3P: phosphatidylinositol-3-phosphate; PtdIns4P: phosphatidylinositol-4-phosphate; RFP: red fluorescent protein; SPG: spastic paraplegia gene; TGN: trans-Golgi network; WT: wild type [ABSTRACT FROM AUTHOR]

Published

2021

20. 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

21. Lysosomal targeting of autophagosomes by the TECPR domain of TECPR2.

Author

Fraiberg, Milana, Tamim-Yecheskel, Bat-Chen, Kokabi, Kamilya, Subic, Nemanja, Heimer, Gali, Eck, Franziska, Nalbach, Karsten, Behrends, Christian, Ben-Zeev, Bruria, Shatz, Oren, and Elazar, Zvulun

Subjects

AUTOPHAGY, LYSOSOMES, MEMBRANE proteins, CHIMERIC proteins, FAMILIAL spastic paraplegia, FIBROBLASTS, NEURODEGENERATION

Abstract

TECPR2 (tectonin beta-propeller repeat containing 2) is a large, multi-domain protein comprised of an amino-terminal WD domain, a middle unstructured region and a carboxy-terminal TEPCR domain comprises of six TECPR repeats followed by a functional LIR motif. Human TECPR2 mutations are linked to spastic paraplegia type 49 (SPG49), a hereditary neurodegenerative disorder. Here we show that basal macroautophagic/autophagic flux is impaired in SPG49 patient fibroblasts in the form of accumulated autophagosomes. Ectopic expression of either full length TECPR2 or the TECPR domain rescued autophagy in patient fibroblasts in a LIR-dependent manner. Moreover, this domain is recruited to the cytosolic leaflet of autophagosomal and lysosomal membranes in a LIR- and VAMP8-dependent manner, respectively. These findings provide evidence for a new role of the TECPR domain in particular, and TECPR2 in general, in lysosomal targeting of autophagosomes via association with Atg8-family proteins on autophagosomes and VAMP8 on lysosomes. Abbreviations: HOPS: homotypic fusion and vacuole protein sorting; LIR: LC3-interacting region; SPG49: spastic paraplegia type 49; STX17: syntaxin 17; TECPR2: tectonin beta-propeller repeat containing 2; VAMP8: vesicle associated membrane protein 8 [ABSTRACT FROM AUTHOR]

Published

2021

22. 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

23. 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

24. Gait parameters as tools for analyzing phenotypic alterations of a mouse model of Charcot-Marie-Tooth disease.

Author

Hwang, Sun Hee, Chang, Eun Hyuk, Kwak, Geon, Jeon, Hyeonjin, Choi, Byung-Ok, and Hong, Young Bin

Subjects

*PHENOTYPIC plasticity, *CHARCOT-Marie-Tooth disease, *ANIMAL disease models, *PERIPHERAL nervous system, *PROGNOSIS, *ANATOMICAL planes, *FAMILIAL spastic paraplegia

Abstract

Charcot-Marie-Tooth disease (CMT), a genetically heterogeneous group of diseases in the peripheral nervous system, is characterized by progressive and symmetrical distal weakness resulting in gait abnormality. The necessity of the diagnostic and prognostic biomarkers has been raised for both basic research and clinical practice in CMT. Since biomarkers for animal study of CMT are limited, we evaluated the feasibility of gait parameters as tool for measuring disease phenotype of CMT mouse model. Using a Trembler-J (Tr-J) mouse, a CMT type 1 (CMT1) mouse model, we analyzed kinematic parameters such as angles of hip, knee and ankle (sagittal plane), and spatial parameters including step width and stride length (transverse plane). Regarding of kinematic parameters, Tr-J mice exhibited less plantarflexed ankle during the swing phase and more dorsiflexed ankle at the terminal stance compared to control mice. The range of motion in ankle angle of Tr-J mice was significantly greater than that of control mice. In spatial parameter, Tr-J mice exhibited wider step width compared to control mice. These results are similar to previously reported gait patterns of CMT1 patients. In comparison with other markers such as nerve conduction study and rotarod test, gait parameters dynamically reflected the disease progression of CMT1 mice. Therefore, these data imply that gait parameters can be used as useful tools to analyzed the disease phenotype and progression during preclinical study of peripheral neuropathy such as CMT. [ABSTRACT FROM AUTHOR]

Published

2021

25. Exome sequencing of a Pakistani family with spastic paraplegia identified an 18 bp deletion in the cytochrome B5 domain of FA2H.

Author

Abbas, Safdar, Brugger, Beatrice, Zubair, Muhammad, Gul, Sana, Blatterer, Jasmin, Wenninger, Julian, Rehman, Khurram, Tatrai, Benjamin, Khan, Muzammil Ahmad, and Windpassinger, Christian

Subjects

FAMILIAL spastic paraplegia, PAKISTANIS, FREE fatty acids, PARAPLEGIA, MUSCLE weakness

Abstract

Hereditary spastic paraplegias (HSPs) are a diverse class of neurodegenerative disorders that mainly affect the corticospinal tract of the body and result in various clinical conditions such as lower limb spasticity and muscle weakness in the lower extremities. Worldwide, more than 70 chromosomal loci/genes have been reported to be associated with HSPs, out of which, six genes viz., ATL1, FA2H, GJC2, AP4E1, ALDH18A1 and ATP13A2 have been mapped in Pakistani families. In the present genetic study, we report on a large consanguineous Pakistani family with a complex form of HSP segregating with a 18 bp deletion in the first exon of the Fatty Acid 2-Hydroxylase (FA2H) gene (NM_024306.5:c.159_176del). The identified in-frame deletion results in loss of six amino acids (p.Arg53_Ile58del) within the cytochrome B5 domain of the protein. FA2H is required for alpha-hydroxylation of free fatty acids to form alpha-hydroxylated sphingolipids. Its cytochrome b5-like heme-binding domain, which spans from residues 15 to 85, imparts the redox activity to FA2H. This mutation has previously been reported in a Pakistani family presenting with a similar form of complex HSP. Together with our findings the pathogenic role of the observed variant is further supported. Mutation studies on additional Pakistani families for FA2H will further elucidate its mutational spectrum, which may help in developing a prenatal diagnostic test for Khyber Pakhtunkhwa resident Pakistani families. [ABSTRACT FROM AUTHOR]

Published

2021

26. Bio-efficacy of organic selenium compounds in broiler chickens.

Author

De Marco, Michele, Conjat, Anne-Sophie, Briens, Mickaël, Hachemi, Mohammed Amine, and Geraert, Pierre-André

Subjects

*BROILER chickens, *ORGANIC compounds, *SELENOMETHIONINE, *SODIUM selenite, *SELENOCYSTEINE, *FAMILIAL spastic paraplegia

Abstract

This study is aimed at comparing the bio-efficacy of different inorganic and organic Se compounds. Three broiler experiments (Exp1 = Ross PM3; Exp2 = Ross 308; and Exp3 = Ross 308) were performed, on the basis of Se tissue accretion, to define the bio-efficacy of Se sources. Birds were fed a control diet (negative control [NC]; no supplemental Se) and, depending on the study, the NC was supplemented with sodium selenite (SS), Se-yeast (35%, 56%, 65% or 72% of Se as selenomethionine (SeMet); SY35, SY56, SY65 and SY72), pure forms of selenocysteine (SeCys) (methylselenocysteine [MSeCys]; L-selenocystine [L-SeCys]), or pure form of organic Se (L-selenomethionine, L-SeMet or hydroxy-selenomethionine, OH-SeMet) at 0.3 mg Se/kg. In Exp 2, an additional treatment of SY65 + L-SeCys was also fed, with both sources added at 0.3 mg Se/kg. In Exp3, L-SeMet and OH-SeMet, were supplemented at 0.15, 0.30, 0.45 and 0.60 mg Se/kg. The results of Exp 1 (mg Se/kg muscle DM) were: NC, 0.56; SS, 0.73; MSeCys, 0.68; L-SeCys, 0.70; SY65, 1.52; OH-SeMet, 1.85 (p <.001); Exp 2 were: NC, 0.34; SS, 0.52; SY35, 0.84; SY65, 1.18; SY65 + L-SeCys, 1.22; OH-SeMet: 1.33 (p <.001); Exp 3 were: NC, 0.10; SS, 0.31; SY56, 0.88; SY72, 1.03; L-SeMet, 1.33; OH-SeMet, 1.33 (p <.01). The results of these three studies demonstrate that the bio-efficacy of organic Se supplements for chickens depends upon the proportion of SeMet, while dietary SeCys sources showed similar bio-efficacy as SS. Moreover, these data showed the high bio-efficacy of the pure form of organic Se and the bioequivalence between L-SeMet and OH-SeMet. Updated knowledge on the bioavailability of different Se compounds in broiler. Direct L-selenomethionine and hydroxy-selenomethionine comparison. [ABSTRACT FROM AUTHOR]

Published

2021

27. Familiarity with Hereditary Spastic Paraplegia (HSP) and Differentiation of Upper Body Gait Characteristics between Children with HSP and Spastic Diplegic Cerebral Palsy.

Author

Bickley, Christina, Mitchell, Katy, Scott, Allison, Bury, Meredith, and Oyelami, Mayowa

Subjects

*CEREBRAL palsy, *DIAGNOSIS, *PHILOSOPHY of education, *GAIT in humans, *LONGITUDINAL method, *QUESTIONNAIRES, *SURVEYS, *SYMPTOMS, *DATA analysis software, *FAMILIAL spastic paraplegia

Abstract

The aim of this two-part, prospective study was to determine therapist familiarity with HSP and examine diagnostic accuracy between individuals with HSP and those with Spastic Diplegic Cerebral Palsy (SD-CP). Part-one surveyed physical therapists (PT) and physical therapist assistants (PTA) throughout Texas to determine familiarity with HSP and its gait deviations. Part-two examined accuracy in differential diagnosis of HSP versus SD-CP using gait analysis and the effects of an educational module on upper body gait deviations observed in individuals with HSP. Both PTs and PTAs indicated a high degree (≥73.2%) of unfamiliarity with HSP. While a majority of respondents (≥88.7%) indicated use of observational gait analysis in clinical practice, ≥92.5% indicated never receiving instruction on HSP or its associated gait deviations. Whole group analysis revealed diagnostic accuracy increased 21.7% post educational module. In addition, individual case diagnostic accuracy yielded significant improvement in 14 out of 20 cases. Physical and occupational therapists are in a unique position to assist with the identification and distinction of HSP from CP. This study demonstrated that brief instruction on common upper body gait deviations seen in individuals with HSP may improve a clinician's ability to distinguish SD-CP from HSP via gait analysis. [ABSTRACT FROM AUTHOR]

Published

2021

28. The neuroradiology of upper motor neuron degeneration: PLS, HSP, ALS.

Author

Li Hi Shing, Stacey and Bede, Peter

Subjects

*NEURODEGENERATION, *MOTOR neurons, *AMYOTROPHIC lateral sclerosis, *LEUKODYSTROPHY, *CORPUS callosum, *FAMILIAL spastic paraplegia

Abstract

While correlations between CST metrics and motor disability are confounded by co-existing lower motor neuron degeneration in ALS ([8]), these are pertinent to upper motor neuron predominant disorders such as PLS and HSP ([9]). In this edition of Amyotrophic Lateral Sclerosis and Frontotemporal Degeneration, Navas-Sánchez et al. present an intriguing study of motor cortex and corticospinal tract (CST) degeneration in hereditary spastic paraparesis type 4 (SPG4) ([7]). Curr Opin Neurol. 2018; 31: 431 - 8. 16 Schuster C, Elamin M, Hardiman O, Bede P. The segmental diffusivity profile of amyotrophic lateral sclerosis associated white matter degeneration. The neuroimaging literature of motor neuron diseases is dominated by studies in ALS ([1],[2]). [Extracted from the article]

Published

2022

29. Stumbling, struggling, and shame due to spasticity: a qualitative study of adult persons with hereditary spastic paraplegia.

Author

Kerstens, Hans C. J. W., Satink, Ton, Nijkrake, Maarten J., De Swart, Bert J. M., Van Lith, Bas J. H., Geurts, Alexander C. H., and Nijhuis-van der Sanden, Maria W. G.

Subjects

*ADAPTABILITY (Personality), *AUTOMOBILE driving, *POSTURAL balance, *FATIGUE (Physiology), *FEAR, *FRUSTRATION, *GAIT disorders, *HELP-seeking behavior, *THEORY of knowledge, *NEUROLOGICAL disorders, *HEALTH outcome assessment, *PAIN, *SHAME, *SPASTICITY, *QUALITATIVE research, *SOCIAL constructionism, *ACTIVITIES of daily living, *SOCIAL support, *WELL-being, *INFORMATION-seeking behavior, *THEMATIC analysis, *PHYSICAL activity, *DATA analysis software, *PATIENTS' attitudes, *FAMILIAL spastic paraplegia, *ADULTS

Abstract

Purpose: Little is known concerning the impact of chronic spasticity on physical activities, social participation, and well-being, and whether patients' needs are addressed by current treatments. This study aims to investigate these lacunas in persons with a pure form of hereditary spastic paraplegia (HSP), in whom spasticity is a prominent symptom. Methods: Fourteen patients with a pure form of HSP were interviewed. These interviews were recorded, verbally transcribed, and thematically analyzed. Results: Four themes were identified which can be reflected by the phrases: (1) 'I stumble', (2) 'I struggle', (3) 'I feel ashamed', and (4) 'I need support'. Balance and gait problems led to limitations in domestic activities, employment, and recreation. 'Stumbling' also occurred due to pain, stiffness, and fatigue. Struggling was related to the continuous need for adaptation strategies, including the abandonment of some activities. Participants further reported feelings of shame, fear, and frustration. Lastly, they needed more support in daily activities than currently provided. Conclusion: Besides treating spasticity-related motor impairments, patients with HSP need practical support for optimizing their physical activities and social participation. They also seek attention for the non-motor consequences of their chronic spasticity to improve their well-being. Patient-reported outcomes might help to address these needs. According to patients with hereditary spastic paraplegia, interventions for spasticity should not only be aimed at reducing motor impairments, but also on reducing pain and fatigue, improving nighttime rest and general well-being, and optimizing the performance of relevant personal activities. Medical, role and emotional management in patients with hereditary spastic paraplegia can be improved only when individual needs are identified and monitored over the course of the disease. Besides assessment of bodily functions and physical capacities, systematic evaluation of patient-reported outcomes will help both patients and professionals to monitor the functional impact of disease progression and to evaluate the effects of interventions aimed at retarding this progression. [ABSTRACT FROM AUTHOR]

Published

2020

30. Pseudoxanthoma elasticum and retinitis pigmentosa: dual diagnosis of recessive conditions with ophthalmological consequences.

Author

Katiyar, Disha, Davies, Peter, and Goel, Himanshu

Subjects

*RETINITIS pigmentosa, *DUAL diagnosis, *SYMPTOMS, *RECESSIVE genes, *CARDIOVASCULAR system, *FAMILIAL spastic paraplegia

Abstract

5.2% of people are carriers for at least two recessive diseases; it can be concluded that a much smaller proportion develop these conditions as two mutated copies of a gene must be present for the disease to manifest clinically. We present a 38-year-old Caucasian female affected by two autosomal recessive disorders which can affect the eyes, pseudoxanthoma elasticum (PXE) and retinitis pigmentosa (RP). PXE is an autosomal recessive disorder caused by mutations in ABCC6, affecting 1:25 000 to 1:100 000 people; its classical features involve the dermatological, ophthalmological and cardiovascular systems. Our patient presented with dermatological features of PXE and ophthalmological features of RP. RP presents with significant locus heterogeneity; our patient had biallelic mutations in USH2A. This report highlights an interesting case of two unrelated autosomal recessive diseases presenting in one person, both of which have the potential to manifest with ophthalmological symptoms and signs. Though it is likely that only one condition has caused the ophthalmological findings in this case, it raises the question of how we can distinguish the causative disease when two conditions are present that have a shared target organ. [ABSTRACT FROM AUTHOR]

Published

2020

31. A case of spastic paraplegia-15 with a novel pathogenic variant in ZFYVE26 gene.

Author

Özdemir, Taha Reşid, Gençpınar, Pınar, Arıcan, Pınar, Öztekin, Özgür, Dündar, Nihal Olgaç, and Özyılmaz, Berk

Subjects

*GENETIC disorders, *CORPUS callosum, *PEDIATRIC neurology, *HUMAN chromosome abnormality diagnosis, *LEG, *FAMILIAL spastic paraplegia

Abstract

Hereditary spastic paraplegia (HSP) is a group of rare neurodegenerative disorder with genetic and clinical heterogeneity. It has autosomal dominant (AD), autosomal recessive (AR) and X-linked forms. HSPs are clinically classified into 'pure' and 'complicated' (complex) forms. SPG11 (KIAA1840) and SPG15 (ZFYVE26) are the most common ARHSPs with thin corpus callosum (TCC). They typically present with early cognitive impairment in childhood followed by gait impairment and spasticity in the second and third decades of life. Here, we present a patient girl, born to a couple who were first cousins, was admitted to the pediatric neurology outpatient clinic at 14 years of age because of walking with help, dysarthria and forgetfulness. Her examination revealed a motor mental retardation, bilateral leg spasticity, increased deep tendon reflexes in lower limbs, bilateral pigmentary retinopathy; TCC and white matter hyperintensities on brain MRI, sensorimotor axonal polyneuropathy findings in lower limbs on electromyography. Based on the clinical features and the imaging studies, the diagnosis of HSP was suspected. Targeted next generation sequencing (NGS) was performed using Inherited NGS Panel that consists of 579 gene associated with Mendelian disorders. Analysis of the patient revealed a c.6398_6401delGGGA(p.Arg2133Asnfs*15)(Exon35) homozygous novel change in ZFYVE26 gene. Genotype-phenotype correlation of HSP is complicated due to heterogeneity. The clinical similarity of HSP types increases the importance of genetic diagnosis. There are few reports about pathogenic variants in ZFYVE26 gene in the literature. This case report is one of the few studies that revealed a novel pathogenic variant in ZFYVE26 gene using NGS. [ABSTRACT FROM AUTHOR]

Published

2019

32. A patient with juvenile-onset refractory status epilepticus caused by two novel compound heterozygous mutations in FARS2 gene.

Author

Chen, Zhongyun and Zhang, Yan

Subjects

*STATUS epilepticus, *TRANSFER RNA, *FAMILIAL spastic paraplegia, *PROTEIN structure, *PROTEIN stability, *NUCLEOTIDE sequence

Abstract

FARS2 encodes mitochondrial phenylalanyl transfer ribonucleic acid (RNA) synthetase and is implicated in autosomal recessive combined oxidative phosphorylation deficiency 14. The clinical manifestation can be divided into early onset epileptic phenotype and spastic paraplegia phenotype. The purpose of this study was to report a case of juvenile manifesting refractory epilepsy caused by two novel compound heterozygous mutations in the FARS2 gene. Microscopic and histochemical examination as well as next‐generation sequencing and reconstruction of the three-dimensional structure of FARS2 protein were performed. A 17-year-old man with no developmental delays suffered from generalized tonic-clonic convulsion since 12 years of age and developed refractory status epilepticus 5 years later. No specific etiology was found following brain imaging, muscle biopsy and metabolic studies. DNA sequencing identified two novel compound heterozygous mutations in FARS2, (p.V197M and p.F402S), derived from each parents, respectively. These mutations affected the structure or thermodynamic stability of the protein. This is a case report of juvenile-onset refractory epilepsy caused by two novel compound heterozygous mutations in the FARS2 gene. This case confirms and expands the clinicalphenotype and the genotypic spectrum of the FARS2 gene. [ABSTRACT FROM AUTHOR]

Published

2019

33. ALSUntangled no. 49: resveratrol.

Subjects

*FAMILIAL spastic paraplegia, *PGC-1 protein

Abstract

Three research groups have reported that resveratrol extends the lifespan of the mutant SOD1 mouse model of ALS (mice SB G93A sb ) when the resveratrol was given by an intraperitoneal injection (i.e., into the abdominal cavity). Some manufacturers claim that combining resveratrol with the natural flavanol called quercetin may increase resveratrol's bioavailability; however, data from a pharmacokinetic study in humans indicated that quercetin has no substantial effect on resveratrol blood levels ([62]). These are interesting mechanisms that may potentially alter the progression of ALS and do confer benefit in animal models of one type of familial ALS; however, to-date, there have been no trials of resveratrol in PALS. Given the unknown benefit of resveratrol in PALS and the possible risks, we cannot recommend resveratrol as an ALS treatment at this time. [Extracted from the article]

Published

2019

34. A neuropsychological and behavioral study of PLS.

Author

de Vries, Bálint S., Spreij, Lauriane A., Rustemeijer, Laura M.M., Bakker, Leonhard A., Veldink, Jan H., van den Berg, Leonard H., Nijboer, Tanja C.W., and van Es, Michael A.

Subjects

*SPASTICITY, *BEHAVIORAL assessment, *MOTOR neuron diseases, *BEHAVIOR, *FAMILIAL spastic paraplegia, *NEUROPSYCHOLOGICAL tests, *AMYOTROPHIC lateral sclerosis

Abstract

Background: Primary lateral sclerosis (PLS) is a rare motor neuron disease characterized by progressive degeneration of upper motor neurons, resulting in spasticity and disability. There is, however, mounting evidence that the disease is not limited to upper motor neurons alone and that cognitive and behavioral changes within the spectrum of frontotemporal dementia (FTD) are part of the clinical phenotype. Objectives: To provide an in-depth classification of the cognitive and behavioral profiles of PLS by using the golden standard, a full neuropsychological evaluation, as well as a comprehensive behavioral assessment in a cohort of 30 cases. Results: Only 7 out of 30 PLS patients scored within normal range on all of the tests within our battery. The neuropsychological profile of PLS consists of deficits in social cognition (affective theory of mind (ToM) in particular), fluency, executive functions and memory. Using the revised Strong criteria, we could classify 57% of patients within the FTD spectrum (of which 17% had behavioral variant FTD). An additional 20% of patients had deficits which were not characteristic of FTD. Conclusions: This study confirms that PLS is not a restricted phenotype (only affecting upper motor neurons) and that behavioral and cognitive changes are common. Therefore, clinicians treating PLS patients should routinely assess cognition and behavior as part of routine care as cognitive and behavioral changes impact management, decision-making and care-giver burden. This assessment should be sensitive to the neuropsychological profile of PLS (social cognition (affective ToM in particular), fluency, executive functions and memory) and behavioral changes. [ABSTRACT FROM AUTHOR]

Published

2019

35. High diagnostic yield and novel variants in very late-onset spasticity.

Author

Almomen, Momen, Martens, Kristina, Quadir, Asfia, Pontifex, Carly Sabine, Hanson, Alexandra, Korngut, Lawrence, and Pfeffer, Gerald

Subjects

*FAMILIAL spastic paraplegia, *SPASTICITY, *GENOTYPE-environment interaction, *AMYOTROPHIC lateral sclerosis

Abstract

Hereditary spastic paraplegias (HSPs) are a diverse group of genetic conditions with variable severity and onset age. From a neurogenetic clinic, we identified 14 patients with very late-onset HSP, with symptoms starting after the age of 35. In this cohort, sequencing of known genetic causes was performed using clinically available HSP sequencing panels. We identified 4 patients with mutations in SPG7 and 3 patients with SPAST mutations, representing 50% of the cohort and indicating a very high diagnostic yield. In the SPG7 group, we identified novel variants in two patients. We have also identified two novel mutations in the SPAST group. We present sequencing data from cDNA and RT-qPCR to support the pathogenicity of these variants, and provide observations regarding the poor genotype-phenotype correlation in these conditions that should be the subject of future study. [ABSTRACT FROM AUTHOR]

Published

2019

36. Hereditary and idiopathic spastic paraparesis: preliminary findings of a single center experience.

Author

Cui, Fang, Sun, Liuqing, Qiao, Jie, Xiong, Jianmei, Zhao, Yangang, Li, Jianyong, Li, Mao, Chen, Siyu, and Huang, Xusheng

Subjects

FAMILIAL spastic paraplegia, NEUROLOGIC manifestations of general diseases, MUSCLE strength, TENDON reflex, GENETIC disorders

Abstract

Objectives: Hereditary spastic paraplegias (HSP) is a heterogeneous group of inherited neurologic disorders with diversified clinical manifestations. The purpose of this study was to summarize the clinical manifestations of HSP by analyzing the clinical data of 56 HSP patients. Methods: A total of 56 HSP patients treated in our hospital from January 2014 to March 2016 were included. Demographic and clinical characteristics of patients were collected. The severity of HSP was assessed by disease severity score. Results: The patients included 40 males and 16 females. The mean onset age was 17.86 ± 12.56 years (range: 1-47). The mean disease duration was 13.46 ± 12.82 years (range: 1-63). There were 29 pure (51.8%) forms and 27 complicated (48.2%) HSP. The common manifestations included increased deep tendon reflexes in the lower extremities (94.6%), positive Babinski sign (94.6%), increased muscle tone of lower extremities (91.1%), scissors gait (83.9%), ankle clonus (69.6%), reduced muscle strength in the lower extremities (48.2%) and skeletal deformities (37.5%). Reduced cognitive function was the most common manifestation (55.6%) of the complicated HSP patients. The mean disease severity score was significantly higher in males than in females (2.75 ± 0.55 vs. 2.18 ± 1.13, P = 0.013). Patients with a disease duration >30 years had a significantly higher disease severity score than those with disease duration of 1-10 and 21-30 years. Discussion: We reported the clinical features of HSP from 56 patients in our hospital. Our findings should be helpful for better understanding of clinical features of HSP. [ABSTRACT FROM AUTHOR]

Published

2018

37. Autosomal dominant hereditary spastic paraplegia with axonal sensory motor polyneuropathy maps to chromosome 21q 22.3.

Author

Peddareddygari, Leema Reddy, Hanna, Philip A., Igo, Robert P., Luo, Yuqun A., Won, Sungho, Hirano, Michio, and Grewal, Raji P.

Subjects

*FAMILIAL spastic paraplegia, *POLYCYSTIC kidney disease, *MICROSATELLITE repeats, *HAPLOTYPES, *AUTOSOMAL recessive polycystic kidney

Abstract

Aim:Hereditary spastic paraplegia (HSP) are a genetically and clinically heterogeneous group of disorders. At present, 19 autosomal dominant loci for HSP have been mapped. We ascertained an American family of European descent segregating an autosomal dominant HSP associated with peripheral neuropathy.Methods:A genome wide scan was performed with 410 microsatellite repeat marker (Weber lab screening set 16) and following linkage and haplotype analysis, fine mapping was performed. Established genes or loci for HSP were excluded by direct sequencing or haplotype analysis.Results:All established loci for HSP were excluded. Fine mapping suggested a locus on chromosome 21q22.3 flanked by markers D21S1411 and D21S1446 with a maximum logarithm of odds score of 2.05 and was supported by haplotype analysis. A number of candidate genes in this region were analyzed and no disease-producing mutations were detected.Conclusion:We present the clinical and genetic analysis of an American family with autosomal dominant HSP with axonal sensory motor polyneuropathy mapping to a novel locus on chromosome 21q22.3 designated SPG56. [ABSTRACT FROM AUTHOR]

Published

2016

38. South African Teachers’ Attitudes toward the Inclusion of Learners with Different Abilities in Mainstream Classrooms.

Author

Donohue, Dana K. and Bornman, Juan

Subjects

*TEACHERS, *ACADEMIC achievement, *ANALYSIS of variance, *AUTISM, *BLINDNESS, *CONFIDENCE, *EMPLOYEES, *EXPERIENCE, *FACTOR analysis, *LEARNING disabilities, *MAINSTREAMING in special education, *CASE studies, *STATISTICAL sampling, *SCALE analysis (Psychology), *SOCIAL skills, *STATISTICS, *T-test (Statistics), *DATA analysis, *SOCIAL attitudes, *DOWN syndrome, *DATA analysis software, *DESCRIPTIVE statistics, *FAMILIAL spastic paraplegia, RESEARCH evaluation

Abstract

This research sought to examine South African teachers’ attitudes toward the inclusion of learners with different abilities in their hypothetical mainstream classrooms. Participants were 93 South African teachers who responded to the Teachers’ Attitudes and Expectations Scale, a measure developed for this study, regarding four vignettes depicting learners with different types of impairments. Overall, teachers reported that inclusion would benefit learners’ social development (mean scores from 2.57 to 3.35) more than their intellectual development (mean scores from 2.14 to 2.83). It also was found that teachers overwhelmingly were more confident about including learners with Down syndrome into their hypothetical mainstream classes when compared with the inclusion of learners with other disabilities,F(3, 90) = 9.59,p < 0.01. The results suggest that providing teachers with sufficient resources within the classroom and training that includes hands-on experience with children with disabilities could positively influence their attitudes toward the inclusion of learners with disabilities in their classrooms. [ABSTRACT FROM AUTHOR]

Published

2015

39. Social Competence and Temperament in Children with Chronic Orthopaedic Disability.

Author

Yagmurlu, Bilge and Yavuz, H. Melis

Subjects

*HUMAN abnormalities, *ANALYSIS of variance, *ATTENTION, *CARING, *STATISTICAL correlation, *HEALTH status indicators, *MOTHERS, *PARENT-child relationships, *PARENTING, *PSYCHOLOGY of children with disabilities, *POLYNEUROPATHIES, *SELF-management (Psychology), *SOCIAL skills, *SPINA bifida, *OPERATIVE surgery, *TEMPERAMENT, *SOCIOECONOMIC factors, *SEVERITY of illness index, *DESCRIPTIVE statistics, *FAMILIAL spastic paraplegia

Abstract

The aim of the study was to investigate social competence in children with orthopaedic disability and its concurrent relations to child’s temperament, health condition, and maternal warmth. Participants were 68 Turkish children (mean = 5.94 years) with chronic orthopaedic disability and their mothers coming from disadvantaged backgrounds. Mother ratings were used to measure social competence, temperament, general health condition, and parental warmth. The attending physician rated the severity of orthopaedic disability. Attentional focusing, emotional reactivity, and child’s sex significantly predicted social competence. Age at first operation was slightly negatively associated with reactivity. The findings revealed the importance of emotional and attentional regulation for social functioning in children with orthopaedic disability, and pointed to the susceptibility of reactivity to environmental conditions. The study suggested that social functioning of youth with orthopaedic disability might benefit from temperament-based intervention and prevention programmes. [ABSTRACT FROM AUTHOR]

Published

2015

40. Clinical variability and female penetrance in X-linked familial FTD/ALS caused by a P506S mutation in UBQLN2.

Author

Vengoechea, Jaime, David, Marjorie P., Yaghi, Shadi R., Carpenter, Lori, and Rudnicki, Stacy A.

Subjects

*MOTOR neuron diseases, *FRONTOTEMPORAL dementia, *AMYOTROPHIC lateral sclerosis, *FAMILIAL spastic paraplegia, *DEGLUTITION disorders, *MILD cognitive impairment

Abstract

Amyotrophic lateral sclerosis (ALS) is a degenerative motor neuron disease leading to progressive paralysis that is generally fatal. Only 10% of cases are familial, a subset of which overlaps with frontotemporal dementia (FTD). Up to half of ALS patients have cognitive impairment, with 15% meeting the criteria for FTD. Clinical sequencing of UBQLN2 in a family with X-linked FTD/ALS with suspected incomplete penetrance, manifesting in both genders, revealed a P506S mutation in. Affected individuals were diagnosed with various conditions including hereditary spastic paraplegia (HSP), bulbar palsy and multiple sclerosis. The mutation in UBQLN2 was first identified in a 35-year-old female who presented with one year of progressive dysarthria, dyspnea, dysphagia, and cognitive decline. EMG suggested early motor neuron disease with prominent bulbar involvement. Her cognition declined rapidly and she developed extremity weakness. Her brother, initially diagnosed with HSP, and her second cousin, with primary lateral sclerosis, also have a P506S mutation in UBQLN2. In conclusion, the P506S mutation in UBQLN2 can affect both males and females and displays great phenotypic variability within the same family. Females can potentially have a more severe and rapidly progressive presentation than their male relatives. Additionally, the P506S mutation can also cause an FTD phenotype. [ABSTRACT FROM AUTHOR]

Published

2013

41. Complicated SPG4 presenting with recurrent urinary tract infection.

Author

Oberoi, Kinsi, Grewal, Kabir S., and Reddy Peddareddygari, Leema

Subjects

*URINARY tract infections, *FAMILIAL spastic paraplegia, *NEUROLOGICAL disorders, *NEUROGENIC bladder, *GENETIC disorder diagnosis, *BLADDER, *BETA lactamases

Abstract

We present a 62-year-old woman who developed recurrent urinary tract infections in her early fifties and, after an evaluation by an infectious disease physician, was referred for a neurological consultation. Her history and neurological examination were consistent with spastic paraparesis and there was significant family history of a variety of neurological diagnoses suggesting a genetic disorder. Whole exome genetic testing revealed a novel change, a c.508 C > T variant in the SPAST gene. Our genetic and protein modeling analysis suggest that this is a disease-producing mutation confirming the diagnosis of hereditary spastic paraplegia type 4 (SPG4). This patient expands the spectrum of mutations that can cause this disorder and demonstrate the importance of recognizing the role of neurological disorders in causing neurogenic bladder and recurrent urinary tract infections. [ABSTRACT FROM AUTHOR]

Published

2020