Your search keyword '"leukodystrophy"' showing total 4,865 results

101. Autosomal Recessive NOTCH3-Related Leukodystrophy in Two Siblings and Review of the Literature.

Author

Al-Amrani, Fatema, Al-Maawali, Almundher, Al-Thihli, Khalid, Al-Ajmi, Eiman, Ganesh, Anuradha, and Al Futaisi, Amna

Subjects

*LITERATURE reviews, *LEUKODYSTROPHY, *SYMPTOMS, *GENETIC disorders, *SIBLINGS, *EPILEPSY

Abstract

NOTCH3, a large type I transmembrane receptor expressed on arterial smooth muscle cells and capillary pericytes, features a diverse extracellular domain with 34 epidermal growth factor-like repeats. It exhibits distinct phenotypes due to variant zygosity and type; missense mutations cause CADASIL with cerebral vasculopathy, while null mutations lead to severe congenital manifestations. This report describes two cases with homozygous loss- of- function variants in NOTCH3 along with their clinical manifestations. These patients presented with a severe congenital phenotype, including eye misalignment, visual impairment, epilepsy, global developmental delay, and subsequent development of pyramidal signs. Biallelic nonsense variants were discovered in both the cases (NM_000435.3:c.2203 C > T (p. [Arg735Ter]). Livedo reticularis was not reported in our cases, although it was present in previously reported patients. Autosomal recessive NOTCH3 -related leukodystrophy is usually caused by biallelic null mutations in NOTCH3. The phenotype of biallelic null variants is associated with a more severe phenotype than the dominantly inherited form of the disease. [ABSTRACT FROM AUTHOR]

Published

2023

102. Gene and Cellular Therapies for Leukodystrophies.

Author

Aerts-Kaya, Fatima and van Til, Niek P.

Subjects

*DUCHENNE muscular dystrophy, *GENE therapy, *LEUKODYSTROPHY, *HEMATOPOIETIC stem cell transplantation, *CELLULAR therapy, *CORD blood

Abstract

Leukodystrophies are a heterogenous group of inherited, degenerative encephalopathies, that if left untreated, are often lethal at an early age. Although some of the leukodystrophies can be treated with allogeneic hematopoietic stem cell transplantation, not all patients have suitable donors, and new treatment strategies, such as gene therapy, are rapidly being developed. Recent developments in the field of gene therapy for severe combined immune deficiencies, Leber's amaurosis, epidermolysis bullosa, Duchenne's muscular dystrophy and spinal muscular atrophy, have paved the way for the treatment of leukodystrophies, revealing some of the pitfalls, but overall showing promising results. Gene therapy offers the possibility for overexpression of secretable enzymes that can be released and through uptake, allow cross-correction of affected cells. Here, we discuss some of the leukodystrophies that have demonstrated strong potential for gene therapy interventions, such as X-linked adrenoleukodystrophy (X-ALD), and metachromatic leukodystrophy (MLD), which have reached clinical application. We further discuss the advantages and disadvantages of ex vivo lentiviral hematopoietic stem cell gene therapy, an approach for targeting microglia-like cells or rendering cross-correction. In addition, we summarize ongoing developments in the field of in vivo administration of recombinant adeno-associated viral (rAAV) vectors, which can be used for direct targeting of affected cells, and other recently developed molecular technologies that may be applicable to treating leukodystrophies in the future. [ABSTRACT FROM AUTHOR]

Published

2023

103. Evaluation of Pediatric Leukodystrophies using Magnetic Resonance Imaging: A Prospective Study from North India.

Author

Malgotra, Sugandhi, Kumar, Ashna, and Mahajan, Manik

Subjects

*MAGNETIC resonance imaging, *LEUKODYSTROPHY, *NUCLEAR magnetic resonance spectroscopy, *DIAGNOSTIC imaging, *LONGITUDINAL method, *CHILD patients, *HOSPITAL care of children

Abstract

Background: Leukodystrophies are rare genetically determined disorders affecting the process of myelination of the central nervous system that primarily occur in the pediatric age group. These disorders are associated with significant morbidity and mortality. Detailed clinical evaluation, neuroimaging, biochemical studies, and genetic analysis have a pivotal role in their evaluation. Aim: The aim of this study is to assess the spectrum and distinctive magnetic resonance imaging (MRI) patterns of various pediatric leukodystrophies from North India. Materials and Methods: This prospective observational study was carried over a period of 1 year in a tertiary care center in North India. All children with suspected leukodystrophies referred to the Department of Radiology for MRI were included in the study. The findings were recorded in detail and a probable diagnosis of the type of leukodystrophy was made. Biochemical evaluation was performed wherever possible and correlated with MRI diagnosis. Results: Thirty patients formed the material of the study with an age range of 2.5 months to 17 years. Developmental delay was the commonest presenting complaint (66.67%) followed by abnormal muscle tone and gait disturbances. Different subtypes of leukodystrophies were seen in our study with metachromatic leukodystrophy being the commonest one (30%). Magnetic resonance spectroscopy was found to be a promising sequence in certain leukodystrophies. Conclusions: Varied spectrum of pediatric leukodystrophies was observed in North India. MRI is an accurate modality in determining the presence and assessing the severity of abnormalities in patients with leukodystrophies. [ABSTRACT FROM AUTHOR]

Published

2023

104. Diffusion-based structural connectivity patterns of multiple sclerosis phenotypes.

Author

Martinez-Heras, Eloy, Solana, Elisabeth, Vivó, Francesc, Lopez-Soley, Elisabet, Calvi, Alberto, Alba-Arbalat, Salut, Schoonheim, Menno M., Strijbis, Eva M., Vrenken, Hugo, Barkhof, Frederik, Rocca, Maria A., Filippi, Massimo, Pagani, Elisabetta, Groppa, Sergiu, Fleischer, Vinzenz, Dineen, Robert A., Bellenberg, Barbara, Lukas, Carsten, Pareto, Deborah, and Rovira, Alex

Subjects

MULTIPLE sclerosis, MAGNETIC resonance imaging, LEUKODYSTROPHY, MACHINE learning, PHENOTYPES

Published

2023

105. A Case of Multiple Mitochondrial Dysfunctions Syndrome 4 with Novel ISCA2 Variants, Mimicking Post-Infectious Encephalitis.

Author

Chin, Hyungjin, Cho, Jaeso, Kim, Woo Joong, Kim, Soo Yeon, Lim, Byung Chan, Kim, Ki Joong, and Chae, Jong Hee

Abstract

ISCA2 loss of function leads to leukodystrophy and developmental regression (multiple mitochondrial dysfunctions syndrome 4 (MMDS4)). We present a first Korean case of MMDS4 presenting with rapid developmental regression and leukodystrophy after febrile episode, mimicking post-infectious encephalitis. The patient had displayed normal development until 12 months of age. At 13 months of age, one month after experiencing a post-vaccination fever, she quickly progressed to being unable to sit unassisted nor speak any words. Analysis of the cerebrospinal fluid (CSF) revealed lympho-dominant pleocytosis. Amino acid analysis of both the serum and CSF demonstrated elevated glycine exclusively in the CSF. Diffuse leukodystrophy was noted in the brain magnetic resonance image. Whole exome sequencing revealed compound heterozygous ISCA2 variants of c.166T>G, p.C56G and c.422A>C, p.Q141P. No evidence of mitochondrial disease other than bilateral optic atrophy was noted. In cases of early onset rapid developmental regression with leukodystrophy, MMDS4 should be considered. [ABSTRACT FROM AUTHOR]

Published

2023

106. Biallelic pathogenic variants in POLR3D alter tRNA transcription and cause a hypomyelinating leukodystrophy: A case report.

Author

Macintosh, Julia, Perrier, Stefanie, Pinard, Maxime, Tran, Luan T., Guerrero, Kether, Prasad, Chitra, Prasad, Asuri N., Pastinen, Tomi, Thiffault, Isabelle, Coulombe, Benoit, and Bernard, Geneviève

Subjects

TRANSFER RNA, RNA polymerases, MISSENSE mutation, MOLECULAR spectra, LEUKODYSTROPHY, DYSARTHRIA, GENETIC variation

Abstract

RNA polymerase III-related leukodystrophy (POLR3-related leukodystrophy) is a rare, genetically determined hypomyelinating disease arising from biallelic pathogenic variants in genes encoding subunits of RNA polymerase III (Pol III). Here, we describe the first reported case of POLR3-related leukodystrophy caused by biallelic pathogenic variants in POLR3D, encoding the RPC4 subunit of Pol III. The individual, a female, demonstrated delays in walking and expressive and receptive language as a child and later cognitively plateaued. Additional neurological features included cerebellar signs (e.g., dysarthria, ataxia, and intention tremor) and dysphagia, while non-neurological features included hypodontia, hypogonadotropic hypogonadism, and dysmorphic facial features. Her MRI was notable for diffuse hypomyelination with myelin preservation of early myelinating structures, characteristic of POLR3-related leukodystrophy. Exome sequencing revealed the biallelic variants in POLR3D, a missense variant (c.541C > T, p.P181S) and an intronic splice site variant (c.656-6G > A, p.?). Functional studies of the patient's fibroblasts demonstrated significantly decreased RNA-level expression of POLR3D, along with reduced expression of other Pol III subunit genes. Notably, Pol III transcription was also shown to be aberrant, with a significant decrease in 7SK RNA and several distinct tRNA genes analyzed. Affinity purification coupled to mass spectrometry of the POLR3D p.P181S variant showed normal assembly of Pol III subunits yet altered interaction of Pol III with the PAQosome chaperone complex, indicating the missense variant is likely to alter complex maturation. This work identifies biallelic pathogenic variants in POLR3D as a novel genetic cause of POLR3-related leukodystrophy, expanding the molecular spectrum associated with this disease, and proposes altered tRNA homeostasis as a factor in the underlying biology of this hypomyelinating disorder. [ABSTRACT FROM AUTHOR]

Published

2023

107. Description of the Hamburg Alexander Leukodystrophy Cohort.

Author

Kokaly, N., Volk, A., and Bley, A.

Subjects

*LEUKODYSTROPHY, *DISEASE progression, *APNEA, *PERIODICAL publishing

Abstract

This article, published in the journal Neuropediatrics, provides a description of the Hamburg Alexander Leukodystrophy Cohort. Alexander disease (AxD) is a rare and severe leukodystrophy that currently has no cure. The study analyzed the disease courses of 10 AxD patients and classified them according to existing classification systems. The analysis also revealed a heterogeneous need for care and support among the patients, with apnea being a common occurrence. The authors conclude that the disease courses are highly variable and that awareness of potential apnea is important for clinical management. [Extracted from the article]

Published

2023

108. Mutation in the β‐tubulin gene TUBB4A results in epileptic encephalopathy associated with hypomyelinated leucodystrophy: Unexpected findings reveal genetic mosaicism.

Author

Ben Jdila, Marwa, Kammoun, Fatma, Abdelmaksoud‐Dammak, Rania, Triki, Chahnez, and Fakhfakh, Faiza

Subjects

*GAIN-of-function mutations, *EPILEPSY, *MOSAICISM, *LEUKODYSTROPHY, *VOLTAGE-gated ion channels, *PEOPLE with epilepsy, *GENETIC mutation

Abstract

Introduction: Epileptic encephalopathies (EEs) are a group of heterogeneous epileptic syndromes characterized by early‐onset refractory seizures, specific EEG abnormalities, developmental delay or regression and intellectual disability. The genetic spectrum of EE is very wide with mutations in a number of genes having various functions, such as those encoding AMPA ionotropic and glutamate receptors as well as voltage‐gated ion channels. However, the list of EE‐responsible genes could certainly be enlarged by next‐generation sequencing. Patients and methods: The present study reports a clinical investigation and a molecular analysis by the whole exome sequencing (WES) and pyrosequencing of a patient's family affected by epileptic spasms and severe psychomotor delay. Results: Clinical and radiological investigations revealed that the patient presented clinical features of severe and drug‐resistant EE‐type infantile epileptic spasm syndrome that evolved to Lennox Gastaut syndrome with radiological findings of hypomyelinated leukodystrophy. The results of WES revealed the presence of a novel heterozygous c.466C>T mutation in exon 4 of the TUBB4A gene in the patient. This transition led to the replacement of arginine by cysteine at position 156 (p.R156C) of the conserved helix 4 among the N‐terminal domain of the TUBB4A protein. Bioinformatic tools predicted its deleterious effects on the structural arrangement and stability of the protein. The presence of the mutation in the asymptomatic father suggested the hypothesis of somatic mosaicism that was tested by pyrosequencing of DNA from two tissues of the patient and her father. The obtained results showed a lower rate of mutated alleles in the asymptomatic father compared with the affected daughter in both lymphocytes and buccal mucosa cells, confirming the occurrence of paternal mosaicism. The phenotypic features of the patient were also compared with those of previously described patients presenting TUBB4A mutations. Conclusions: Our study is the first to report a disease‐causing variant in the TUBB4A gene in a patient with EE associated with hypomyelinated leucodystrophy. In addition, we expanded the phenotypic spectrum associated with the TUBB4A gene. [ABSTRACT FROM AUTHOR]

Published

2023

109. High genetic heterogeneity of leukodystrophies in Iranian children: the first report of Iranian Leukodystrophy Registry.

Author

Ashrafi, Mahmoudreza, Kameli, Reyhaneh, Hosseinpour, Sareh, Razmara, Ehsan, Zamani, Zahra, Rezaei, Zahra, Mashayekhi, Raziyeh, Pak, Neda, Barzegar, Mohammad, Azizimalamiri, Reza, Kashani, Morteza Rezvani, Khosroshahi, Nahideh, Rasulinezhad, Maryam, Heidari, Morteza, Amanat, Man, Abdi, Alireza, Mohammadi, Bahram, Mohammadi, Mahmoud, Zamani, Gholam Reza, and Badv, Reza Shervin

Subjects

IRANIANS, PEROXISOMAL disorders, MYELIN proteins, MAGNETIC resonance imaging, CENTRAL nervous system, LEUKODYSTROPHY, GLYCOGEN storage disease type II

Abstract

Leukodystrophies (LDs) are a heterogeneous group of progressive neurological disorders and characterized by primary involvement of white matter of the central nervous system (CNS). This is the first report of the Iranian LD Registry database to describe the clinical, radiological, and genomic data of Persian patients with leukodystrophies. From 2016 to 2019, patients suspicious of LDs were examined followed by a brain magnetic resonance imaging (MRI). A single gene testing or whole-exome sequencing (WES) was used depending on the neuroradiologic phenotypes. In a few cases, the diagnosis was made by metabolic studies. Based on the MRI pattern, diagnosed patients were divided into cohorts A (hypomyelinating LDs) versus cohort B (Other LDs). The most recent LD classification was utilized for classification of diagnosed patients. For novel variants, in silico analyses were performed to verify their pathogenicity. Out of 680 registered patients, 342 completed the diagnostic evaluations. In total, 245 patients met a diagnosis which in turn 24.5% were categorized in cohort A and the remaining in cohort B. Genetic tests revealed causal variants in 228 patients consisting of 213 variants in 110 genes with 78 novel variants. WES and single gene testing identified a causal variant in 65.5% and 34.5% cases, respectively. The total diagnostic rate of WES was 60.7%. Lysosomal disorders (27.3%; GM2-gangliosidosis-9.8%, MLD-6.1%, KD-4.5%), amino and organic acid disorders (17.15%; Canavan disease-4.5%, L-2-HGA-3.6%), mitochondrial leukodystrophies (12.6%), ion and water homeostasis disorders (7.3%; MLC-4.5%), peroxisomal disorders (6.5%; X-ALD-3.6%), and myelin protein disorders (3.6%; PMLD-3.6%) were the most commonly diagnosed disorders. Thirty-seven percent of cases had a pathogenic variant in nine genes (ARSA, HEXA, ASPA, MLC1, GALC, GJC2, ABCD1, L2HGDH, GCDH). This study highlights the most common types as well as the genetic heterogeneity of LDs in Iranian children. [ABSTRACT FROM AUTHOR]

Published

2023

110. Adult-onset Alexander disease among patients of Jewish Syrian descent.

Author

Anis, Saar, Fay-Karmon, Tsvia, Lassman, Simon, Shbat, Fadi, Lesman-Segev, Orit, Mor, Nofar, Barel, Ortal, Dominissini, Dan, Chorin, Odelia, Pras, Elon, Greenbaum, Lior, and Hassin-Baer, Sharon

Subjects

FAMILY counseling, SYMPTOMS, CERVICAL cord, SPINAL cord, GENETIC counseling, DYSAUTONOMIA

Abstract

Alexander disease (AxD) is a rare autosomal dominant leukodystrophy caused by heterozygous mutations in the glial fibrillary acid protein (GFAP) gene. The age of symptoms onset ranges from infancy to adulthood, with variable clinical and radiological manifestations. Adult-onset AxD manifests as a chronic and progressive condition, characterized by bulbar, motor, cerebellar, and other clinical signs and symptoms. Neuroradiological findings typically involve the brainstem and cervical spinal cord. Adult-onset AxD has been described in diverse populations but is rare in Israel. We present a series of patients diagnosed with adult-onset AxD from three families, all of Jewish Syrian descent. Five patients (4 females) were diagnosed with adult-onset AxD due to the heterozygous mutation c.219G > A, p.Met73Ile in GFAP. Age at symptoms onset ranged from 48 to 61 years. Clinical characteristics were typical and involved progressive bulbar and gait disturbance, followed by pyramidal and cerebellar impairment, dysautonomia, and cognitive decline. Imaging findings included medullary and cervical spinal atrophy and mostly infratentorial white matter hyperintensities. A newly recognized cluster of adult-onset AxD in Jews of Syrian origin is presented. This disorder should be considered in differential diagnosis in appropriate circumstances. Genetic counselling for family members is required in order to discuss options for future family planning. [ABSTRACT FROM AUTHOR]

Published

2023

111. Molecular Pathogenic Mechanisms of Hypomyelinating Leukodystrophies (HLDs).

Author

Torii, Tomohiro and Yamauchi, Junji

Subjects

*LEUKODYSTROPHY, *CONGENITAL disorders, *GENETIC mutation, *CELL physiology, *RARE diseases

Abstract

Hypomyelinating leukodystrophies (HLDs) represent a group of congenital rare diseases for which the responsible genes have been identified in recent studies. In this review, we briefly describe the genetic/molecular mechanisms underlying the pathogenesis of HLD and the normal cellular functions of the related genes and proteins. An increasing number of studies have reported genetic mutations that cause protein misfolding, protein dysfunction, and/or mislocalization associated with HLD. Insight into the mechanisms of these pathways can provide new findings for the clinical treatments of HLD. [ABSTRACT FROM AUTHOR]

Published

2023

112. A novel variant of the POLR3A gene in a Chinese patient with POLR3-related leukodystrophy.

Author

Yang, Haojun, Wu, Zhongling, Li, Xiaolei, Huang, Yuanxin, Li, Jing, He, Fang, Feng, Li, Xiao, Bo, and Tang, Weiting

Subjects

*GENETIC variation, *CORPUS callosum, *CEREBRAL hemispheres, *CEREBRAL atrophy, *PITUITARY gland, *LEUKODYSTROPHY, *MULTIPLE system atrophy

Abstract

Background: POLR3-related leukodystrophy is a group of rare neurodegenerative disorders characterized by degeneration of the white matter with different combinations of major clinical features. Case: An 18-year-old lady was admitted for no menstruation since childhood. She gradually developed slight symptoms, such as choking after drinking water and unsteady walking in the last 2 years. Furthermore, her test scores and response capability were far lower than that of her peers. Physical examination revealed her to be of a slightly short stature, with stiff expressions and bilateral breast enlargement. She revealed clumsy movements when examined for ataxia, with an SARA score of 9. Findings: The laboratory data revealed a decreased level of estradiol, FSH, and LH, with a MoCA score of 7. Conventional karyotype analysis revealed a 46 XX 9qh + karyotype. Ultrasound indicated primordial uterus (19 × 11 × 10 mm). Brain MRI showed bilateral cerebral hemisphere myelin dysplasia, brain atrophy, thin corpus callosum, and small pituitary gland with uneven reinforcement and enlarged ventricles. Exome sequencing exhibited two missense mutations in the POLR3A gene (c.3013C > T and c.1757C > T), which were inherited from her mother and father, respectively. Conclusion: Collectively, we identified novel compound heterozygous mutations of the POLR3A gene that caused POLR3A-related hypomyelinating leukodystrophy with hypogonadism in the patient combined with the clinical presentation, MRI brain pattern, and medical exome sequencing. Teaching points: The complexity of clinical phenotypes and heterogeneity of genotypes raise new challenges in genetic diagnoses. This study will further aid our understanding of POLR3A-related leukodystrophy and promote further analysis of phenotype-genotype correlations of related diseases. [ABSTRACT FROM AUTHOR]

Published

2023

113. Adult-onset leukodystrophy with vanishing white matter: a case series of 19 patients.

Author

Benzoni, Chiara, Moscatelli, Marco, Farina, Laura, Magri, Stefania, Ciano, Claudia, Scaioli, Vidmer, Alverà, Sara, Cammarata, Gabriella, Bianchi-Marzoli, Stefania, Castellani, Massimo, Zito, Felicia Margherita, Marotta, Giorgio, Piacentini, Sylvie, Villacara, Alberto, Mantegazza, Renato, Gellera, Cinzia, Durães, João, Gouveia, Ana, Matos, Anabela, and do Carmo Macário, Maria

Subjects

*WHITE matter (Nerve tissue), *LEUKODYSTROPHY, *DIFFUSION magnetic resonance imaging, *EVOKED potentials (Electrophysiology), *SYMPTOMS, *MELAS syndrome

Abstract

Background: Leukodystrophy with vanishing white matter (LVWM) is an autosomal recessive disease with typical pediatric-onset caused by mutations in one of the five EIF2B genes. Adult-onset (AO) cases are rare. Methods: In this observational study, we reviewed clinical and laboratory information of the patients with AO-LVWM assessed at two referral centers in Italy and Portugal from Jan-2007 to Dec-2019. Results: We identified 18 patients (13 females) with AO-LVWM caused by EIF2B5 or EIF2B3 mutations. Age of neurological onset ranged from 16 to 60 years, with follow-ups occurring from 2 to 37 years. Crucial symptoms were cognitive and motor decline. In three patients, stroke-like events were the first manifestation; in another, bladder dysfunction remained the main complaint across decades. Brain MRI showed white matter (WM) rarefaction in all cases, except two. Diffusion-weighted imaging documented focal hyperintensity in the acute stage of stroke-like events. 1H-spectroscopy primarily showed N-acetyl-aspartate reduction; 18fluorodeoxyglucose-PET revealed predominant frontoparietal hypometabolism; evoked potential studies demonstrated normal-to-reduced amplitudes; neuro-ophthalmological assessment showed neuroretinal thinning, and b-wave reduction on full-field electroretinogram. Interestingly, we found an additional patient with LVWM-compatible phenotype and monoallelic variants in two distinct eIF2B genes, EIF2B1 and EIF2B2. Conclusions: AO-LVWM presents varying clinical manifestations at onset, including stroke-like events. WM rarefaction is the most consistent diagnostic clue even in the latest onset cases. Spectroscopy and electrophysiological features are compatible with axon, rather than myelin, damage. Cerebral glucose metabolic abnormalities and retinal alterations can be present. LVWM might also be caused by a digenic inheritance affecting the eIF2B complex. [ABSTRACT FROM AUTHOR]

Published

2023

114. Clinical, genetic, and molecular characteristics in a central‐southern Chinese cohort of genetic leukodystrophies.

Author

Li, Yingjie, Xu, Jiaming, Xu, Yan, Li, Chuanzhou, Wu, Yan, and Liu, Zhijun

Subjects

*MACROPHAGE colony-stimulating factor, *LEUKODYSTROPHY, *SPASTICITY, *CELL survival, *VISION disorders, *EPILEPSY, *CENTRAL nervous system

Abstract

Objective: Leukodystrophies are a diverse group of rare inherited disorders that affect the white matter of the central nervous system with a wide phenotypic spectrum. We aimed to characterize the clinical and genetic features of leukodystrophies in a central‐southern Chinese cohort. Methods: A cohort of 16 Chinese probands with leukodystrophy was recruited and performed genetic analysis by targeted panels or whole‐exome sequencing. Further functional analysis of identified mutations in the colony stimulating factor 1 receptor (CSF1R) gene was explored. Results: A total of eight pathogenic variants (3 novel, 5 documented) were identified in genes including AARS2, ABCD1, CSF1R, and GALC. Common symptoms of leukodystrophy such as cognitive decline, behavioral symptoms, bradykinesia, and spasticity were observed in mutation carriers as well as other rare features (e.g., seizure, dysarthric, and vision impairment). Overexpressing CSF1R mutants p.M875I and p.F971Sfs*7 in vitro showed pronounced cleavage CSF1R and suppressed protein expression, respectively, and reduced transcripts of both mutants were observed. CSF1 treatment revealed deficient and suppressed CSF1R phospho‐activation with the mutants. In contrast to the plasma membrane and endoplasmic reticulum (ER) localized wild‐type CSF1R, M875I mutant showed much less membrane association and greater detainment in the ER, whereas F971Sfs*7 mutation led to aberrant non‐ER localization. Both mutations caused suppressed cell viability, which was partially resulted from deficient/suppressed CSF1R‐ERK signaling. Interpretation: In summary, our findings expand the mutation spectrum of these genes in leukodystrophies. Supported by in vitro validation of the pathogenicity of heterozygous CSF1R mutations, our data also provide insights into the pathogenic mechanisms of CSF1R‐related leukodystrophy. [ABSTRACT FROM AUTHOR]

Published

2023

115. Metachromatic leukodystrophy: To screen or not to screen?

Author

Jonckheere, An I., Kingma, Sandra D.K., Eyskens, François, Bordon, Victoria, and Jansen, Anna C.

Subjects

GLYCOGEN storage disease type II, STEM cell transplantation, NEWBORN screening, AGE of onset, LEUKODYSTROPHY, LYSOSOMAL storage diseases

Abstract

Metachromatic leukodystrophy (MLD) is a neurodegenerative lysosomal storage disorder caused by biallelic pathogenic variants in the gene encoding arylsulfatase A. Disease onset is variable (with late infantile, early and late juvenile, and adult forms) and treatment options depend on age and disease symptoms at onset. In the past, allo-hematopoietic stem cell transplantation (allo-HSCT) has been the best treatment option, following strict selection criteria. The outcome however is variable and morbidity remains high. This paved the way to the development of new treatment options, some of them aiming to be curative. In the light of this changing therapeutic field, newborn screening is becoming a valuable option. This narrative review aims to describe the outcome of allo-HSCT in the different MLD disease forms, and, in addition, reviews new treatment options. Finally, the shift of the field towards newborn screening for MLD is discussed. • MLD is a neurodegenerative disease. • Allo-hematopoietic stem cell transplantation increases life span but morbidity remains high. • New therapeutic developments including gene therapy aim to be curative. • This shifts the field towards newborn screening. [ABSTRACT FROM AUTHOR]

Published

2023

116. Association of serum neurofilament light with microglial activation in multiple sclerosis.

Author

Saraste, Maija, Matilainen, Markus, Vuorimaa, Anna, Laaksonen, Sini, Sucksdorff, Marcus, Leppert, David, Kuhle, Jens, and Airas, Laura

Subjects

MULTIPLE sclerosis, GLATIRAMER acetate, TRANSLOCATOR proteins, CHRONIC wounds & injuries, CYTOPLASMIC filaments, MICROGLIA, LEUKODYSTROPHY, SEX factors in disease

Published

2023

117. Newborn Screening for Krabbe Disease and Identification of Minority Patients.

Author

Bonkowsky, Joshua L., Wilkes, Jacob, Baker, Monika, Grantham, Anna, Kurtzberg, Joanne, and Orsini, Joseph

Subjects

*NEWBORN screening, *MEDICAL screening, *MINORITIES

Published

2024

118. Recurrent Ischemic Strokes due to Monogenic COL4A1 Mutation: The First Case Report from Latin America.

Author

Wong-Valenzuela, Emilio Israel, San Juan, Daniel, Santos Zambrano, José, Camacho Molina, Alejandra, Morales-Morales, Miguel Angel, and Lopez-Landa, Alejandro

Subjects

*ISCHEMIC stroke, *GENETIC mutation, *YOUNG adults, *STROKE patients, *LEUKODYSTROPHY

Abstract

Introduction. Monogenic mutations as the cause of recurrent ischemic cerebral small-vessel disease with leukodystrophy are rare. COL4A1 gene mutations are a relatively new etiology of cerebrovascular lesions in young adults; however, any patient has been reported from Latin America. Case Presentation. We presented a Mexican young female with leukodystrophy and recurrent stroke secondary to COL4A1 monogenic mutation. Discussion/Conclusion. COL4A1 monogenic mutations are associated with cerebral small-vessel disease and other systemic manifestations. To date, there is little evidence to justify the treatment and prevention of recurrent strokes in patients with this mutation. [ABSTRACT FROM AUTHOR]

Published

2023

119. A systematic review of clinical effectiveness and safety for historical and current treatment options for metachromatic leukodystrophy in children, including atidarsagene autotemcel.

Author

Armstrong, Nigel, Olaye, Andrew, Noake, Caro, and Pang, Francis

Subjects

*HEMATOPOIETIC stem cell transplantation, *GRAFT versus host disease, *LEUKODYSTROPHY, *COGNITIVE ability

Abstract

Objective: To understand the benefit-risk profile for historical and current treatments for MLD. Methods: A systematic review was conducted on the effectiveness, safety, and costs of MLD treatments: allogeneic haematopoietic stem cell transplantation (HSCT) and atidarsagene autotemcel (arsa-cel) according to best practice. Results: A total of 6940 titles and abstracts were retrieved from the literature searches and 26 from other sources. From these, 35 manuscripts reporting on a total of 12 studies were selected for inclusion in the review. There were no controlled multi-armed trials. However, we provide observations comparing two interventional therapies (alloHSCT and arsa-cel) and each of these to standard/supportive care (natural history). There were no benefits for survival, gross motor function and cognitive function for LI patients receiving alloHSCT, as patients experienced disease progression similar to LI natural history. For juvenile patients receiving alloHSCT, no differences in survival were observed versus natural history, however stabilisation of cognitive and motor function were reported for some patients (particularly for pre- or minimally-symptomatic LJ patients), while others experienced disease progression. Furthermore, alloHSCT was associated with severe complications such as treatment-related mortality, graft versus host disease, and re-transplantation in both LI and EJ treated patients. Most LI and EJ patients treated with arsa-cel appeared to have normal development, preservation, or slower progression of gross motor function and cognitive function, in contrast to the rapid decline observed in natural history patients. A survival benefit for arsa-cel versus natural history and versus alloHSCT was observed in LI patients.LI and EJ patients treated with arsa-cel had better gross motor function and cognitive function compared to alloHSCT, which had limited effect on motor and cognitive decline. No data has been reported for arsa-cel treatment of LJ patients. Conclusions: Overall, this systematic review indicates that compared to NHx and HSCT, treatment with arsa-cel results in clinically relevant benefits in LI and EJ MLD patients by preserving cognitive function and motor development in most patients, and increased survival for LI patients. Nevertheless, further research is required to confirm these findings, given they are based on results from non-RCT studies. [ABSTRACT FROM AUTHOR]

Published

2023

120. Core protocol development for phase 2/3 clinical trials in the leukodystrophy vanishing white matter: a consensus statement by the VWM consortium and patient advocates.

Author

Schoenmakers, Daphne H., Leferink, Prisca S., Vanderver, Adeline, Bonkowsky, Joshua L., Krägeloh-Mann, Ingeborg, Bernard, Geneviève, Bertini, Enrico, Fatemi, Ali, Fogel, Brent L., Wolf, Nicole I., Skwirut, Donna, Buck, Allyson, Holberg, Brett, Saunier-Vivar, Elise F., Rauner, Robert, Dekker, Hanka, van Bokhoven, Pieter, Stellingwerff, Menno D., Berkhof, Johannes, and van der Knaap, Marjo S.

Subjects

*WHITE matter (Nerve tissue), *CONSORTIA, *CLINICAL trials, *LEUKODYSTROPHY, *RARE diseases

Abstract

Background: The leukodystrophy "Vanishing White Matter" (VWM) is an orphan disease with neurological decline and high mortality. Currently, VWM has no approved treatments, but advances in understanding pathophysiology have led to identification of promising therapies. Several investigational medicinal products are either in or about to enter clinical trial phase. Clinical trials in VWM pose serious challenges, as VWM has an episodic disease course; disease phenotype is highly heterogeneous and predictable only for early onset; and study power is limited by the small patient numbers. To address these challenges and accelerate therapy delivery, the VWM Consortium, a group of academic clinicians with expertise in VWM, decided to develop a core protocol to function as a template for trials, to improve trial design and facilitate sharing of control data, while permitting flexibility regarding other trial details. Overall aims of the core protocol are to collect safety, tolerability, and efficacy data for treatment assessment and marketing authorization. Methods: To develop the core protocol, the VWM Consortium designated a committee, including clinician members of the VWM Consortium, family and patient group advocates, and experts in statistics, clinical trial design and alliancing with industries. We drafted three age-specific protocols, to stratify into more homogeneous patient groups, of ages ≥ 18 years, ≥ 6 to < 18 years and < 6 years. We chose double‐blind, randomized, placebo-controlled design for patients aged ≥ 6 years; and open-label non-randomized natural-history-controlled design for patients < 6 years. The protocol describes study populations, age-specific endpoints, inclusion and exclusion criteria, study schedules, sample size determinations, and statistical considerations. Discussion: The core protocol provides a shared uniformity across trials, enables a pool of shared controls, and reduces the total number of patients necessary per trial, limiting the number of patients on placebo. All VWM clinical trials are suggested to adhere to the core protocol. Other trial components such as choice of primary outcome, pharmacokinetics, pharmacodynamics, and biomarkers are flexible and unconstrained by the core protocol. Each sponsor is responsible for their trial execution, while the control data are handled by a shared research organization. This core protocol benefits the efficiency of parallel and consecutive trials in VWM, and we hope accelerates time to availability of treatments for VWM. Trial registration: NA. From a scientific and ethical perspective, it is strongly recommended that all interventional trials using this core protocol are registered in a clinical trial register. [ABSTRACT FROM AUTHOR]

Published

2023

121. A novel IBA57 variant is associated with mitochondrial iron--sulfur protein deficiency and necrotizing myelopathy in dogs.

Author

Mandigers, Paul J. J., Stehling, Oliver, Vos-Loohuis, Manon, Van Steenbeek, Frank G., Lill, Roland, and Leegwater, Peter A.

Subjects

PROTEIN deficiency, IRON, MITOCHONDRIA, SULFUR, DOGS, SPINAL cord diseases, IRON clusters

Abstract

Introduction: Hereditary necrotizing myelopathy (HNM) in young Kooiker dogs is characterized by progressive ataxia and paralysis with autosomal recessive inheritance. The basic genetic defect is unknown. We investigated the possible cause by a genome-wide analysis using six affected and 17 unrelated unaffected Kooiker dogs and by functional follow-up studies. Method: The HNM locus was mapped by a case--control study using a dense SNP array and confirmed by linkage analysis of two pedigrees. The gene exons in the critical region were analyzed by next-generation sequencing. The functional effect of the candidate canine IBA57 pathogenic variant was biochemically examined in an established HeLa cell culture model in which the endogenous IBA75 gene product was depleted by RNAi. Results: The basic defect was localized in the centromeric 5 Mb region of canine chromosome 14. The most associated SNP co-segregated fully with HNM and reached an LOD score of 6.1. A candidate pathogenic mutation was found in the iron--sulfur cluster assembly gene IBA57 and led to the amino acid substitution R147W. The expression of human IBA57 harboring the canine R147W exchange could only partially restore the biochemical defects of several mitochondrial [4Fe-4S] proteins upon IBA57 depletion, showing that the mutant protein is functionally impaired. Discussion: Pathogenic variants in human IBA57 cause multiple mitochondrial dysfunction syndrome 3 (MMDS3), a neurodegenerative disorder with distant similarities to HNM. The incomplete functional complementation of IBA57- depleted human cells by IBA57-R147W identifies the DNA mutation in affected Kooiker dogs as the genetic cause of HNM. Our findings further expand the phenotypic spectrum of pathogenic IBA57 variants. [ABSTRACT FROM AUTHOR]

Published

2023

122. HDAC-6 inhibition ameliorates the early neuropathology in a mouse model of Krabbe disease.

Author

Braz, Sandra O., Morgado, Marlene M., Pereira, Marta I., Monteiro, Ana C., Golonzhka, Olga, Jarpe, Matthew, Brites, Pedro, Sousa, Monica M., and Nogueira-Rodrigues, Joana

Subjects

AXONAL transport, NEUROLOGICAL disorders, TUBULINS, LABORATORY mice, NERVOUS system, ANIMAL disease models

Abstract

Introduction: In Krabbe disease (KD), mutations in β-galactosylceramidase (GALC), a lysosomal enzyme responsible for the catabolism of galactolipids, leads to the accumulation of its substrates galactocerebroside and psychosine. This neurologic condition is characterized by a severe and progressive demyelination together with neuron-autonomous defects and degeneration. Twitcher mice mimic the infantile form of KD, which is the most common form of the human disease. The Twitcher CNS and PNS present demyelination, axonal loss and neuronal defects including decreased levels of acetylated tubulin, decreased microtubule stability and impaired axonal transport. Methods: We tested whether inhibiting the α-tubulin deacetylase HDAC6 with a specific inhibitor, ACY-738, was able to counteract the early neuropathology and neuronal defects of Twitcher mice. Results: Our data show that delivery of ACY-738 corrects the low levels of acetylated tubulin in the Twitcher nervous system. Furthermore, it reverts the loss myelinated axons in the sciatic nerve and in the optic nerve when administered from birth to postnatal day 9, suggesting that the drug holds neuroprotective properties. The extended delivery of ACY-738 to Twitcher mice delayed axonal degeneration in the CNS and ameliorated the general presentation of the disease. ACY-738 was effective in rescuing neuronal defects of Twitcher neurons, stabilizing microtubule dynamics and increasing the axonal transport of mitochondria. Discussion: Overall, our results support that ACY-738 has a neuroprotective effect in KD and should be considered as an add-on therapy combined with strategies targeting metabolic correction. [ABSTRACT FROM AUTHOR]

Published

2023

123. Optical genome mapping in an atypical Pelizaeus-Merzbacher prenatal challenge.

Author

Rogac, Mihael, Kovanda, Anja, Lovrečić, Luca, and Peterlin, Borut

Subjects

GENE mapping, GENETIC counseling, GENETIC variation, SYMPTOMS, LEUKODYSTROPHY

Abstract

Pathogenic genetic variants represent a challenge in prenatal counseling, especially when clinical presentation in familial carriers is atypical. We describe a prenatal case involving a microarray-detected duplication of PLP1 which causes X-linked Pelizaeus-Merzbacher disease, a progressive hypomyelinating leukodystrophy. Because of atypical clinical presentation in an older male child, the duplication was examined using a novel technology, optical genome mapping, and was found to be an inverted duplication, which has not been previously described. Simultaneously, segregation analysis identified another healthy adult male carrier of this unique structural rearrangement. The novel PLP1 structural variant was reclassified, and a healthy boy was delivered. In conclusion, we suggest that examining structural variants with novel methods is warranted especially in cases with atypical clinical presentation and may in these cases lead to improved prenatal and postnatal genetic counseling. [ABSTRACT FROM AUTHOR]

Published

2023

124. Adult-onset leukodystrophies: a practical guide, recent treatment updates, and future directions.

Author

Muthusamy, Karthik, Sivadasan, Ajith, Dixon, Luke, Sudhakar, Sniya, Thomas, Maya, Danda, Sumita, Wszolek, Zbigniew K., Wierenga, Klaas, Dhamija, Radhika, and Gavrilova, Ralitza

Subjects

LEUKODYSTROPHY, FAMILY counseling, MOLECULAR spectra, WHITE matter (Nerve tissue), DISEASE progression

Abstract

Adult-onset leukodystrophies though individually rare are not uncommon. This group includes several disorders with isolated adult presentations, as well as several childhood leukodystrophies with attenuated phenotypes that present at a later age. Misdiagnoses often occur due to the clinical and radiological overlap with common acquired disorders such as infectious, immune, inflammatory, vascular, metabolic, and toxic etiologies. Increased prevalence of non-specific white matter changes in adult population poses challenges during diagnostic considerations. Clinico-radiological spectrum and molecular landscape of adult-onset leukodystrophies have not been completely elucidated at this time. Diagnostic approach is less well-standardized when compared to the childhood counterpart. Absence of family history and reduced penetrance in certain disorders frequently create a dilemma. Comprehensive evaluation and molecular confirmation when available helps in prognostication, early initiation of treatment in certain disorders, enrollment in clinical trials, and provides valuable information for the family for reproductive counseling. In this review article, we aimed to formulate an approach to adult-onset leukodystrophies that will be useful in routine practice, discuss common adult-onset leukodystrophies with usual and unusual presentations, neuroimaging findings, recent advances in treatment, acquired mimics, and provide an algorithm for comprehensive clinical, radiological, and genetic evaluation that will facilitate early diagnosis and consider active treatment options when available. A high index of suspicion, awareness of the clinico-radiological presentations, and comprehensive genetic evaluation are paramount because treatment options are available for several disorders when diagnosed early in the disease course. [ABSTRACT FROM AUTHOR]

Published

2023

125. Clinical Significance of Diffusion Tensor Imaging in Metachromatic Leukodystrophy.

Author

Amedick, Lucas Bastian, Martin, Pascal, Beschle, Judith, Strölin, Manuel, Wilke, Marko, Wolf, Nicole, Pouwels, Petra, Hagberg, Gisela, Klose, Uwe, Naegele, Thomas, Kraegeloh-Mann, Ingeborg, and Groeschel, Samuel

Subjects

*DIFFUSION tensor imaging, *NATURAL history, *DIFFUSION magnetic resonance imaging, *LYSOSOMAL storage diseases, *LEUKODYSTROPHY, *GLYCOGEN storage disease type II

Abstract

Background Metachromatic leukodystrophy (MLD) is a lysosomal enzyme deficiency disorder leading to progressive demyelination and, consecutively, to cognitive and motor decline. Brain magnetic resonance imaging (MRI) can detect affected white matter as T2 hyperintense areas but cannot quantify the gradual microstructural process of demyelination more accurately. Our study aimed to investigate the value of routine MR diffusion tensor imaging in assessing disease progression. Methods MR diffusion parameters (apparent diffusion coefficient [ADC] and fractional anisotropy [FA]) were in the frontal white matter, central region (CR), and posterior limb of the internal capsule in 111 MR datasets from a natural history study of 83 patients (age: 0.5–39.9 years; 35 late-infantile, 45 juvenile, 3 adult, with clinical diffusion sequences of different scanner manufacturers) as well as 120 controls. Results were correlated with clinical parameters reflecting motor and cognitive function. Results ADC values increase and FA values decrease depending on disease stage/severity. They show region-specific correlations with clinical parameters of motor and cognitive symptoms, respectively. Higher ADC levels in CR at diagnosis predicted a disease course with more rapid motor deterioration in juvenile MLD patients. In highly organized tissues such as the corticospinal tract, in particular, diffusion MR parameters were highly sensitive to MLD-associated changes and did not correlate with the visual quantification of T2 hyperintensities. Conclusion Our results show that diffusion MRI can deliver valuable, robust, clinically meaningful, and easily obtainable/accessible/available parameters in the assessment of prognosis and progression of MLD. Therefore, it provides additional quantifiable information to established methods such as T2 hyperintensity. [ABSTRACT FROM AUTHOR]

Published

2023

126. Aquaporin-4 and GPRC5B: old and new players in controlling brain oedema.

Author

Passchier, Emma M J, Kerst, Sven, Brouwers, Eelke, Hamilton, Eline M C, Bisseling, Quinty, Bugiani, Marianna, Waisfisz, Quinten, Kitchen, Philip, Unger, Lucas, Breur, Marjolein, Hoogterp, Leoni, Vries, Sharon I de, Abbink, Truus E M, Kole, Maarten H P, Leurs, Rob, Vischer, Henry F, Brignone, Maria S, Ambrosini, Elena, Feillet, François, and Born, Alfred P

Subjects

*CEREBRAL edema, *AQUAPORINS, *G protein coupled receptors, *NEUROLOGICAL disorders, *GENETIC variation

Abstract

Brain oedema is a life-threatening complication of various neurological conditions. Understanding molecular mechanisms of brain volume regulation is critical for therapy development. Unique insight comes from monogenic diseases characterized by chronic brain oedema, of which megalencephalic leukoencephalopathy with subcortical cysts (MLC) is the prototype. Variants in MLC1 or GLIALCAM , encoding proteins involved in astrocyte volume regulation, are the main causes of MLC. In some patients, the genetic cause remains unknown. We performed genetic studies to identify novel gene variants in MLC patients, diagnosed by clinical and MRI features, without MLC1 or GLIALCAM variants. We determined subcellular localization of the related novel proteins in cells and in human brain tissue. We investigated functional consequences of the newly identified variants on volume regulation pathways using cell volume measurements, biochemical analysis and electrophysiology. We identified a novel homozygous variant in AQP4 , encoding the water channel aquaporin-4, in two siblings, and two de novo heterozygous variants in GPRC5B , encoding the orphan G protein-coupled receptor GPRC5B, in three unrelated patients. The AQP4 variant disrupts membrane localization and thereby channel function. GPRC5B, like MLC1, GlialCAM and aquaporin-4, is expressed in astrocyte endfeet in human brain. Cell volume regulation is disrupted in GPRC5B patient-derived lymphoblasts. GPRC5B functionally interacts with ion channels involved in astrocyte volume regulation. In conclusion, we identify aquaporin-4 and GPRC5B as old and new players in genetic brain oedema. Our findings shed light on the protein complex involved in astrocyte volume regulation and identify GPRC5B as novel potentially druggable target for treating brain oedema. [ABSTRACT FROM AUTHOR]

Published

2023

127. A homozygous POLR1A variant causes leukodystrophy and affects protein homeostasis.

Author

Misceo, Doriana, Lirussi, Lisa, Strømme, Petter, Sumathipala, Dulika, Guerin, Andrea, Wolf, Nicole I, Server, Andres, Stensland, Maria, Dalhus, Bjørn, Tolun, Aslıhan, Kroes, Hester Y, Nyman, Tuula A, Nilsen, Hilde L, and Frengen, Eirik

Subjects

*LEUKODYSTROPHY, *CATALYTIC RNA, *RIBOSOMAL proteins, *RNA polymerases, *HOMEOSTASIS

Abstract

RNA polymerase I transcribes ribosomal DNA to produce precursor 47S rRNA. Post-transcriptional processing of this rRNA generates mature 28S, 18S and 5.8S rRNAs, which form the ribosomes, together with 5S rRNA, assembly factors and ribosomal proteins. We previously reported a homozygous variant in the catalytic subunit of RNA polymerase I, POLR1A, in two brothers with leukodystrophy and progressive course. However, the disease mechanism remained unknown. In this report, we describe another missense variant POLR1A NM_015425.3:c.1925C>A; p.(Thr642Asn) in homozygosity in two unrelated patients. Patient 1 was a 16-year-old male and Patient 2 was a 2-year-old female. Both patients manifested neurological deficits, with brain MRIs showing hypomyelinating leukodystrophy and cerebellar atrophy; and in Patient 1 additionally with hypointensity of globi pallidi and small volume of the basal ganglia. Patient 1 had progressive disease course, leading to death at the age of 16.5 years. Extensive in vitro experiments in fibroblasts from Patient 1 documented that the mutated POLR1A led to aberrant rRNA processing and degradation, and abnormal nucleolar homeostasis. Proteomics data analyses and further in vitro experiments documented abnormal protein homeostasis, and endoplasmic reticulum stress responses. We confirm that POLR1A biallelic variants cause neurodegenerative disease, expand the knowledge of the clinical phenotype of the disorder, and provide evidence for possible pathological mechanisms leading to POLR1A-related leukodystrophy. [ABSTRACT FROM AUTHOR]

Published

2023

128. Unraveling the heterogeneous pathological substrates of relapse-onset multiple sclerosis: a multiparametric voxel-wise 3 T MRI study.

Author

Margoni, Monica, Pagani, Elisabetta, Preziosa, Paolo, Gueye, Mor, Azzimonti, Matteo, Rocca, Maria A., and Filippi, Massimo

Subjects

*MULTIPLE sclerosis, *CEREBRAL atrophy, *MAGNETIC resonance imaging, *MAGNETIZATION transfer, *WHITE matter (Nerve tissue), *LEUKODYSTROPHY

Abstract

Background: In multiple sclerosis (MS), pathological processes affecting brain gray (GM) and white matter (WM) are heterogeneous. Objective: To apply a multimodal MRI approach to investigate the regional distribution of the different pathological processes occurring in the brain WM and GM of relapse-onset MS patients. Methods: Fifty-seven MS patients (forty-two relapsing remitting [RR], fifteen secondary progressive [SP]) and forty-seven age- and sex-matched healthy controls (HC) underwent a multimodal 3 T MRI acquisition. Between-group voxel-wise differences of brain WM and GM volumes, magnetization transfer ratio (MTR), T1-weighted(w)/T2w ratio, intracellular volume fraction (ICV_f), and quantitative susceptibility mapping (QSM) maps were investigated. Results: Compared to HC, RRMS showed significant WM, deep GM and cortical atrophy, significantly lower MTR and T1w/T2w ratio of periventricular and infratentorial WM, deep GM and several cortical areas, lower ICV_f in supratentorial and cerebellar WM and in some cortical areas, and lower QSM values in bilateral periventricular WM (p < 0.001). Compared to RRMS, SPMS patients showed significant deep GM and widespread cortical atrophy, significantly lower MTR of periventricular WM, deep GM and cerebellum, lower T1w/T2w ratio of fronto-temporal WM regions, lower ICV_f of some fronto-tempo-occipital WM and cortical areas. They also had increased QSM and T1w/T2w ratio in the pallidum, bilaterally (p < 0.001). Conclusion: A periventricular pattern of demyelination and widespread GM and WM neuro-axonal loss are detectable in RRMS and are more severe in SPMS. Higher T1w/T2w ratio and QSM in the pallidum, possibly reflecting iron accumulation and neurodegeneration, may represent a relevant MRI marker to differentiate SPMS from RRMS. [ABSTRACT FROM AUTHOR]

Published

2023

129. Gross Motor Function in Pediatric Onset TUBB4A -Related Leukodystrophy: GMFM-88 Performance and Validation of GMFC-MLD in TUBB4A.

Author

Gavazzi, Francesco, Patel, Virali, Charsar, Brittany, Glanzman, Allan, Erler, Jacqueline, Sevagamoorthy, Anjana, McKenzie, Emma, Kornafel, Tracy, Ballance, Elizabeth, Pierce, Samuel R., Teng, Michelle, Formanowski, Brielle, Woidill, Sarah, Shults, Justine, Wassmer, Evangeline, Tonduti, Davide, Magrinelli, Francesca, Bernard, Geneviève, Van Der Knaap, Marjo, and Wolf, Nicole

Subjects

*LEUKODYSTROPHY, *AGE of onset, *RANK correlation (Statistics), *TEST validity, *MOLECULAR diagnosis

Abstract

TUBB4A pathogenic variants are associated with a spectrum of neurologic impairments including movement disorders and leukodystrophy. With the development of targeted therapies, there is an urgent unmet need for validated tools to measure mobility impairment. Our aim is to explore gross motor function in a pediatric-onset TUBB4A -related leukodystrophy cohort with existing gross motor outcome tools. Gross Motor Function Measure-88 (GMFM-88), Gross Motor Function Classification System (GMFCS-ER), and Gross Motor Function Classification-Metachromatic Leukodystrophy (GMFC-MLD) were selected through face validity. Subjects with a confirmed clinical and molecular diagnosis of TUBB4A -related leukodystrophy were enrolled. Participants' sex, age, genotype, and age at disease onset were collected, together with GMFM-88 and concurrent GMFCS-ER and GMFC-MLD. Performances on each measure were compared. GMFM-88 floor effect was defined as total score below 20%. A total of 35 subjects participated. Median performance by GMFM-88 was 16.24% (range 0-97.31), with 42.9% (n = 15) of individuals performing above the floor. GMFM-88 Dimension A (Lying and Rolling) was the best-performing dimension in the GMFM-88 (n = 29 above the floor). All levels of the Classification Scales were represented, with the exception of the GMFC-MLD level 0. Evaluation by GMFM-88 was strongly correlated with the Classification Scales (Spearman correlations: GMFCS-ER:GMFM-88 r = 0.90; GMFC-MLD:GMFM-88 r = 0.88; GMFCS-ER:GMFC-MLD: r = 0.92). Despite overall observation of a floor effect, the GMFM-88 is able to accurately capture the performance of individuals with attenuated phenotypes. GMFM-88 Dimension A shows no floor effect. GMFC-MLD shows a strong correlation with GMFCS-ER and GMFM-88, supporting its use as an age-independent functional score in TUBB4A -related leukodystrophy. [ABSTRACT FROM AUTHOR]

Published

2023

130. Fatal leukodystrophy in Costello syndrome: a case report.

Author

Failoc-Rojas, Virgilio E., Ugaz, Piero A. Quiroz, León, Dante A. Loconi, and Zeña-Ñañez, Sandra

Subjects

FETAL macrosomia, FETAL growth retardation, RAS oncogenes, LEUKODYSTROPHY, ENDOCRINE diseases, PHENOTYPIC plasticity

Abstract

Background: Costello syndrome (CS) is a rare genetic condition characterized by dysregulation of the signaling pathway, phenotypic alteration due to fetal macrosomia or growth retardation, facial abnormalities, loose skin, cardiovascular abnormalities, and a variable degree of intellectual disability. Case presentation: We describe the case of a 20-month-old male patient with fetal macrosomia and polyhydramnios, presenting psychomotor development delay and growth limitation during the first months of life. CS was diagnosed at four months of age after detecting a variant of the HRAS gene c.35G > C (p.G12A). A clinical description of his condition was recorded throughout his life, including cardiovascular diseases, endocrine disorders, and recurrent infections. At 20 months of age, after presenting events of marked hypotonia and generalized seizures, brain magnetic resonance revealed symmetrical lesions of the infra- and supratentorial white matter in both cerebral hemispheres, which resulted in the diagnosis of cerebral leukodystrophy. The patient had a rapid and progressive deterioration that eventually led to death. Conclusions: This is the first report of a case of CS in Peru. In addition, this is a case that presented with multisystemic conditions culminating in leukodystrophy, which is a rare event according to the literature. [ABSTRACT FROM AUTHOR]

Published

2023

131. Hypomyelination caused by a novel homozygous pathogenic variant in FOLR1: complete clinical and radiological recovery with oral folinic acid therapy and review of the literature.

Author

Potic, Ana, Perrier, Stefanie, Radovic, Tijana, Gavrilovic, Svetlana, Ostojic, Jelena, Tran, Luan T., Thiffault, Isabelle, Pastinen, Tomi, Schiffmann, Raphael, and Bernard, Geneviève

Subjects

*LITERATURE reviews, *FOLINIC acid, *DYSPLASIA, *MAGNETIC resonance imaging, *THERAPEUTICS, *DISEASE progression

Abstract

Background: Neurodegeneration due to cerebral folate transport deficiency is a rare autosomal recessive disorder caused by biallelic pathogenic variants in FOLR1. Onset typically occurs in late infancy and is characterized by psychomotor regression, epilepsy, and a hypomyelinating leukodystrophy on magnetic resonance imaging. If left untreated, progressive neurodegeneration occurs. However, early treatment with folinic acid has been shown to stabilize or reverse neurological features. Approximately thirty patients have been described worldwide. Here, we report the first two cases with genetically proven cerebral folate transport deficiency from South-Eastern Europe, describe the effect of oral folinic acid therapy on clinical and neuroradiological features and review the literature. Results: Two siblings presented in childhood with clinical and radiological findings consistent with a hypomyelinating leukodystrophy. Exome sequencing revealed a novel homozygous pathogenic variant in FOLR1 (c.465_466delinsTG; p.W156G), confirming the diagnosis of neurodegeneration due to cerebral folate transport deficiency. Folinic acid treatment was promptly initiated in both patients. The younger sibling was treated early in disease course at 2 years of age, and demonstrated complete recovery in clinical and MRI features. The older sibling, who was 8 years of age at the time of diagnosis and treatment, demonstrated partial but substantial improvements. Conclusion: We present the first account in the literature that early treatment initiation with oral folinic acid alone can result in complete neurological recovery of both clinical and radiological abnormalities in neurodegeneration due to cerebral folate deficiency. Moreover, through the report of these patients along with review of the literature, we provide information about the natural history of the disease with comparison of treatment effects at different stages of disease progression. This report also reinforces the importance of universal access to genetic testing to ensure prompt diagnoses for treatable disorders. [ABSTRACT FROM AUTHOR]

Published

2023

132. The Effect of Interleukin-1 Antagonists on Brain Volume and Cognitive Function in Two Patients With Megalencephalic Leukoencephalopathy With Subcortical Cysts.

Author

Sönmez, Hafize Emine, Savaş, Merve, Aliyeva, Bülbül, Deniz, Adnan, Güngör, Mesut, Anık, Yonca, and Kara, Bülent

Subjects

*LEUKOENCEPHALOPATHIES, *LEUKODYSTROPHY, *COGNITIVE ability, *INTERLEUKIN-1, *MAGNETIC resonance imaging, *CYSTS (Pathology), *WHITE matter (Nerve tissue)

Abstract

Megalencephalic leukoencephalopathy with subcortical cysts (MLC) is a rare leukodystrophy characterized by early-onset macrocephaly and progressive white matter vacuolation. The MLC1 protein plays a role in astrocyte activation during neuroinflammation and regulates volume decrease following astrocyte osmotic swelling. Loss of MLC1 function activates interleukin (IL)-1β-induced inflammatory signals. Theoretically, IL-1 antagonists (such as anakinra and canakinumab) can slow the progression of MLC. Herein, we present two boys from different families who had MLC due to biallelic MLC1 gene mutations and were treated with the anti-IL-1 drug anakinra. Two boys from different families presented with megalencephaly and psychomotor retardation. Brain magnetic resonance imaging findings in both patients were compatible with the diagnosis of MLC. The diagnosis of MLC was confirmed via Sanger analysis of the MLC1 gene. Anakinra was administered to both patients. Volumetric brain studies and psychometric evaluations were performed before and after anakinra treatment. After anakinra therapy, brain volume in both patients decreased significantly and cognitive functions and social interactions improved. No adverse effects were observed during anakinra therapy. Anakinra or other IL-1 antagonists can be used to suppress disease activity in patients with MLC; however, the present findings need to be confirmed via additional research. [ABSTRACT FROM AUTHOR]

Published

2023

133. Cortical interneuron development is affected in 4H leukodystrophy.

Author

Dooves, Stephanie, Kok, Liza M L, Holmes, Dwayne B, Breeuwsma, Nicole, Breur, Marjolein, Bugiani, Marianna, Wolf, Nicole I, and Heine, Vivi M

Subjects

*LEUKODYSTROPHY, *NEURAL circuitry, *KALLMANN syndrome, *GABA antagonists, *GENE expression, *PLURIPOTENT stem cells, *BRAIN abnormalities

Abstract

4H leukodystrophy is a rare genetic disorder classically characterized by hypomyelination, hypodontia and hypogonadotropic hypogonadism. With the discovery that 4H is caused by mutations that affect RNA polymerase III, mainly involved in the transcription of small non-coding RNAs, patients with atypical presentations with mainly a neuronal phenotype were also identified. Pathomechanisms of 4H brain abnormalities are still unknown and research is hampered by a lack of preclinical models. We aimed to identify cells and pathways that are affected by 4H mutations using induced pluripotent stem cell models. RNA sequencing analysis on induced pluripotent stem cell-derived cerebellar cells revealed several differentially expressed genes between 4H patients and control samples, including reduced ARX expression. As ARX is involved in early brain and interneuron development, we studied and confirmed interneuron changes in primary tissue of 4H patients. Subsequently, we studied interneuron changes in more depth and analysed induced pluripotent stem cell-derived cortical neuron cultures for changes in neuronal morphology, synaptic balance, network activity and myelination. We showed a decreased percentage of GABAergic synapses in 4H, which correlated to increased neuronal network activity. Treatment of cultures with GABA antagonists led to a significant increase in neuronal network activity in control cells but not in 4H cells, also pointing to lack of inhibitory activity in 4H. Myelination and oligodendrocyte maturation in cultures with 4H neurons was normal, and treatment with sonic hedgehog agonist SAG did not improve 4H related neuronal phenotypes. Quantitative PCR analysis revealed increased expression of parvalbumin interneuron marker ERBB4 , suggesting that the development rather than generation of interneurons may be affected in 4H. Together, these results indicate that interneurons are involved, possibly parvalbumin interneurons, in disease mechanisms of 4H leukodystrophy. [ABSTRACT FROM AUTHOR]

Published

2023

134. Clinical and radiological spectrum of anti-myelin oligodendrocyte glycoprotein (MOG) antibody encephalitis: single-center observational study.

Author

Salunkhe, Manish, Gupta, Pranjal, Singh, Rajesh K., Tayade, Kamalesh, Goel, Vinay, Agarwal, Ayush, Das, Animesh, Elavarasi, Arunmozhimaran, Pandit, Awadh K., Vibha, Deepti, Garg, Ajay, Sebastian, Leve Joseph Devarajan, Bhatia, Rohit, Tripathi, Manjari, Gaikwad, Shailesh, and Srivastava, MVPadma

Subjects

*MYELIN oligodendrocyte glycoprotein, *ENCEPHALITIS, *POSTVACCINAL encephalitis, *SCIENTIFIC observation, *LEUKODYSTROPHY, *DISEASE progression

Abstract

Objective : The objective was to describe the clinical presentations, radiologic features, and outcomes of patients with autoimmune encephalitis associated with myelin oligodendrocyte glycoprotein antibody (MOG). Background: During the past decade, the spectrum of the myelin oligodendrocyte glycoprotein antibody-associated diseases (MOGAD) has expanded. Recently, patients with MOG antibody encephalitis (MOG-E) who do not fulfill the criteria for ADEM have been reported. In this study, we aimed to describe the spectrum of MOG-E. Methods: Sixty-four patients with MOGAD were screened for encephalitis-like presentation. We collected the clinical, radiological, laboratory, and outcome data of the patients who presented with encephalitis and compared it with the non-encephalitis group. Results: We identified sixteen patients (nine males and seven females) with MOG-E. The median age of the encephalitis population was significantly lower than the non-encephalitis group (14.5 years (11.75–18) vs. 28 years (19.75–42), p = 0.0004). Twelve out of sixteen patients (75%) had fever at the time of encephalitis. Headache and seizure were present in 9/16 (56.2%) and 7/16 (43.75%) patients, respectively. FLAIR cortical hyperintensity was present in 10/16 (62.5%) patients. Supratentorial deep gray nuclei were involved in 10/16 (62.5%) patients. Three patients had tumefactive demyelination, and one patient had a leukodystrophy-like lesion. Twelve of 16 (75%) patients had a good clinical outcome. Patient with leukodystrophy pattern and other with generalized CNS atrophy showed a chronic progressive course. Conclusion: MOG-E can have heterogeneous radiological presentations. FLAIR cortical hyperintensity, tumefactive demyelination, and leukodystrophy-like presentations are novel radiological presentations associated with MOGAD. Though majority of MOG-E have a good clinical outcome, few patients can have chronic progressive disease even on immunosuppressive therapy. [ABSTRACT FROM AUTHOR]

Published

2023

135. Neurodegenerative disease after hematopoietic stem cell transplantation in metachromatic leukodystrophy.

Author

Al‐Saady, Murtadha, Beerepoot, Shanice, Plug, Bonnie C., Breur, Marjolein, Galabova, Hristina, Pouwels, Petra J. W., Boelens, Jaap‐Jan, Lindemans, Caroline, van Hasselt, Peter M., Matzner, Ulrich, Vanderver, Adeline, Bugiani, Marianna, van der Knaap, Marjo S., and Wolf, Nicole I.

Subjects

*HEMATOPOIETIC stem cell transplantation, *NEURODEGENERATION, *LYSOSOMAL storage diseases, *GRAY matter (Nerve tissue), *LEUKODYSTROPHY, *CEREBRAL atrophy, *GLYCOGEN storage disease type II

Abstract

Objective: Metachromatic leukodystrophy is a lysosomal storage disease caused by deficient arylsulfatase A. It is characterized by progressive demyelination and thus mainly affects the white matter. Hematopoietic stem cell transplantation may stabilize and improve white matter damage, yet some patients deteriorate despite successfully treated leukodystrophy. We hypothesized that post‐treatment decline in metachromatic leukodystrophy might be caused by gray matter pathology. Methods: Three metachromatic leukodystrophy patients treated with hematopoietic stem cell transplantation with a progressive clinical course despite stable white matter pathology were clinically and radiologically analyzed. Longitudinal volumetric MRI was used to quantify atrophy. We also examined histopathology in three other patients deceased after treatment and compared them with six untreated patients. Results: The three clinically progressive patients developed cognitive and motor deterioration after transplantation, despite stable mild white matter abnormalities on MRI. Volumetric MRI identified cerebral and thalamus atrophy in these patients, and cerebellar atrophy in two. Histopathology showed that in brain tissue of transplanted patients, arylsulfatase A expressing macrophages were clearly present in the white matter, but absent in the cortex. Arylsulfatase A expression within patient thalamic neurons was lower than in controls, the same was found in transplanted patients. Interpretation: Neurological deterioration may occur after hematopoietic stem cell transplantation in metachromatic leukodystrophy despite successfully treated leukodystrophy. MRI shows gray matter atrophy, and histological data demonstrate absence of donor cells in gray matter structures. These findings point to a clinically relevant gray matter component of metachromatic leukodystrophy, which does not seem sufficiently affected by transplantation. [ABSTRACT FROM AUTHOR]

Published

2023

136. Magnetic Resonance Imaging Characteristics of Autoimmune Glial Fibrillary Acidic Protein (GFAP) Astrocytopathy: A Pediatric Series in Southwest China.

Author

Cheng, Weiqin, He, Ling, Luo, Hechuan, Jiang, Yan, Tan, Chengbing, and Fan, Xiao

Subjects

*GLIAL fibrillary acidic protein, *MAGNETIC resonance imaging, *SPINAL cord, *BASAL ganglia, *WHITE matter (Nerve tissue), *NEUROMYELITIS optica, *LEUKODYSTROPHY

Abstract

Objective: To investigate and summarize the magnetic resonance imaging (MRI) manifestations of autoimmune glial fibrillary acidic protein (GFAP) astrocytopathy in children. Methods: We retrospectively analyzed data from 17 pediatric patients with autoimmune GFAP astrocytopathy confirmed by the detection of GFAP autoantibodies in cerebrospinal fluid in our single-center. Furthermore, we reviewed current literature and summarized previous findings on the MRI characteristics of this disease in children. Results: In these 17 patients, the clinical manifestations and results of CSF analysis were suggestive of autoimmune disorder, with a good improvement. The lesions on MRI were most commonly located in the bilateral basal ganglia (70.6%), thalamus (64.7%), cerebral white matter (29.4%). 93.3% of the cerebral lesions were relatively scattered and small, 80% of the spinal lesions presented as longitudinally extensive ones. Both periventricular radial linear (PVRL) (53.8%) and punctate or linear enhancement in basal ganglia and thalamus (53.8%) were commonly observed, followed by the leptomeningeal enhancement (46.2% in the brain and 62.5% in the spinal cord). We then included 55 pediatric patients with MRI data from current literature in our analysis (n = 72, 44 males). Our results revealed similar MRI findings but the enhancement pattern between our series and previously published cases, that is, leptomeningeal enhancement in the brain 46.2% vs 31.4%, in spinal cord 62.5% vs 18.4%, and PVRL enhancement 53.8% vs 11.2%. There were no detailed reports on punctate or linear enhancement. Conclusion: The MRI characteristics of autoimmune GFAP astrocytopathy in children could be suggestive. Scattered and small lesions (especially punctate or linear) in the bilateral thalamus, basal ganglia, and white matter, as well as longitudinally extensive spinal cord lesions (if present), with punctate, PVRL and leptomeningeal enhancement might be a distinct indication for the early diagnosis of this disorder. [ABSTRACT FROM AUTHOR]

Published

2023

137. Utility of genetic testing in children with leukodystrophy.

Author

Zerem, Ayelet, Libzon, Stephanie, Ben Sira, Liat, Meirson, Hadas, Hausman-Kedem, Moran, Haviv, Noam, Yosovich, Keren, Mory, Adi, Baris Feldman, Hagit, Lev, Dorit, Lerman-Sagie, Tally, Fattal-Valevski, Aviva, Hacohen, Yael, and Marom, Daphna

Subjects

LEUKODYSTROPHY, GENETIC testing, NUCLEOTIDE sequencing, PEDIATRIC clinics, CHILDREN'S hospitals, GENETIC disorder diagnosis, MOLECULAR diagnosis

Abstract

Leukodystrophies are monogenic disorders primarily affecting the white matter. We aimed to evaluate the utility of genetic testing and time-to-diagnosis in a retrospective cohort of children with suspected leukodystrophy. Medical records of patients who attended the leukodystrophy clinic at the Dana-Dwek Children's Hospital between June 2019 and December 2021 were retrieved. Clinical, molecular, and neuroimaging data were reviewed, and the diagnostic yield was compared across genetic tests. Sixty-seven patients (Female/Male ratio 35/32) were included. Median age at symptom onset was 9 months (interquartile range (IQR) 3–18 months), and median length of follow-up was 4.75 years (IQR 3–8.5). Time from symptom onset to a confirmed genetic diagnosis was 15months (IQR 11–30). Pathogenic variants were identified in 60/67 (89.6%) patients; classic leukodystrophy (55/67, 82.1%), leukodystrophy mimics (5/67, 7.5%). Seven patients (10.4%) remained undiagnosed. Exome sequencing showed the highest diagnostic yield (34/41, 82.9%), followed by single-gene sequencing (13/24, 54%), targeted panels (3/9, 33.3%) and chromosomal microarray (2/25, 8%). Familial pathogenic variant testing confirmed the diagnosis in 7/7 patients. A comparison between patients who presented before (n = 31) and after (n = 21) next-generation sequencing (NGS) became clinically available in Israel revealed that the time-to-diagnosis was shorter in the latter group with a median of 12months (IQR 3.5–18.5) vs. a median of 19 months (IQR 13–51) (p = 0.005). NGS carries the highest diagnostic yield in children with suspected leukodystrophy. Access to advanced sequencing technologies accelerates speed to diagnosis, which is increasingly crucial as targeted treatments become available. • NGS carries the highest diagnostic yield in leukodystrophy (LD). • CMA has low diagnostic yield in LD. • Access to next generation sequencing shortens time to diagnosis in LD patients. • LD frequencies differ between different geographical areas. [ABSTRACT FROM AUTHOR]

Published

2023

138. Chitinase dysregulation predicts disease aggressiveness in ALS: Insights from the D50 progression model.

Author

Gaur, Nayana, Steinbach, Robert, Plaas, Mario, Witte, Otto W., Brill, Monika S., and Grosskreutz, Julian

Subjects

AMYOTROPHIC lateral sclerosis, CHITINASE, LEUKODYSTROPHY

Published

2023

139. Two rare cases of myelin oligodendrocyte glycoprotein antibody-associated disorder in children with leukodystrophy-like imaging findings.

Author

Wang, Xin, Zhao, Ruibin, Yang, Huafang, Liu, Chong, and Zhao, Qing

Subjects

*MYELIN oligodendrocyte glycoprotein, *LEUKODYSTROPHY, *MAGNETIC resonance imaging, *DEMYELINATION, *SYMPTOMS, *WHITE matter (Nerve tissue)

Abstract

Background: Children with acquired demyelinating syndromes (ADS) whose sera are positive for myelin oligodendrocyte glycoprotein (MOG) immunoglobulin (IgG) can be diagnosed with MOG-IgG associated disorder (MOGAD). Cases with leukodystrophy-like imaging findings with recurrent MOGAD have rarely been reported. Case presentation: Two children with MOGAD, whose onset age was 6 months and 3 years, respectively, were admitted to the hospital due to fever and altered consciousness. In both children, MOG-IgG was detected in the serum using live cell-based assay. Brain magnetic resonance imaging (MRI) revealed leukodystrophy-like lesions with diffuse bilateral white matter. Cerebrospinal fluid (CSF) analysis showed mild pleocytosis with normal or slightly increased protein levels and no oligoclonal bands. Metabolic and inflammatory blood/CSF markers were all negative. Full exon gene testing revealed normal results, and nuclear and mitochondrial DNA were normal. Despite regular immunotherapy and reduction of lesions based on brain MRI results, the patients repeatedly relapsed and had residual neurological dysfunction at 3–4 years of follow-up. Conclusions: Although MOGAD is a monophasic and benign condition, certain MOGAD patients can experience multiple relapses and residual neurologic deficits. The spectrum of clinical manifestations in MOGAD is wider in children than in previously reported cases, including cases with leukodystrophy-like imaging findings. Such imaging findings along with MOG-IgG may occur recurrently and result in severe neurological prognosis. Patients with extensive and confluent white matter lesions should undergo early testing of MOG-IgG to ensure early therapy. In refractory cases, MOGAD treatment may need to be escalated beyond the current therapy, which means second-line immunotherapy should be performed as early as possible and hormone levels should not be rapidly reduced. Early diagnosis and appropriate treatment may improve the prognosis of children with MOGAD. [ABSTRACT FROM AUTHOR]

Published

2023

140. Regional vulnerability of brain white matter in vanishing white matter.

Author

Man, Jodie H.K., van Gelder, Charlotte A.G.H., Breur, Marjolein, Molenaar, Douwe, Abbink, Truus, Altelaar, Maarten, Bugiani, Marianna, and van der Knaap, Marjo S.

Subjects

*OXIDATIVE phosphorylation, *GENE ontology

Abstract

Vanishing white matter (VWM) is a leukodystrophy that primarily manifests in young children. In this disease, the brain white matter is differentially affected in a predictable pattern with telencephalic brain areas being most severely affected, while others remain allegedly completely spared. Using high-resolution mass spectrometry-based proteomics, we investigated the proteome patterns of the white matter in the severely affected frontal lobe and normal appearing pons in VWM and control cases to identify molecular bases underlying regional vulnerability. By comparing VWM patients to controls, we identified disease-specific proteome patterns. We showed substantial changes in both the VWM frontal and pons white matter at the protein level. Side-by-side comparison of brain region-specific proteome patterns further revealed regional differences. We found that different cell types were affected in the VWM frontal white matter than in the pons. Gene ontology and pathway analyses identified involvement of region specific biological processes, of which pathways involved in cellular respiratory metabolism were overarching features. In the VWM frontal white matter, proteins involved in glycolysis/gluconeogenesis and metabolism of various amino acids were decreased compared to controls. By contrast, in the VWM pons white matter, we found a decrease in proteins involved in oxidative phosphorylation. Taken together, our data show that brain regions are affected in parallel in VWM, but to different degrees. We found region-specific involvement of different cell types and discovered that cellular respiratory metabolism is likely to be differentially affected across white matter regions in VWM. These region-specific changes help explain regional vulnerability to pathology in VWM. [ABSTRACT FROM AUTHOR]

Published

2023

141. Early postnatal microglial ablation in the Ccdc39 mouse model reveals adverse effects on brain development and in neonatal hydrocephalus.

Author

Brown, Farrah N., Iwasawa, Eri, Shula, Crystal, Fugate, Elizabeth M., Lindquist, Diana M., Mangano, Francesco T., and Goto, June

Subjects

*NEURAL development, *MICROGLIA, *MACROPHAGE colony-stimulating factor, *HYDROCEPHALUS, *LABORATORY mice, *LEUKODYSTROPHY

Abstract

Background: Neonatal hydrocephalus is a congenital abnormality resulting in an inflammatory response and microglial cell activation both clinically and in animal models. Previously, we reported a mutation in a motile cilia gene, Ccdc39 that develops neonatal progressive hydrocephalus (prh) with inflammatory microglia. We discovered significantly increased amoeboid-shaped activated microglia in periventricular white matter edema, reduced mature homeostatic microglia in grey matter, and reduced myelination in the prh model. Recently, the role of microglia in animal models of adult brain disorders was examined using cell type-specific ablation by colony-stimulating factor-1 receptor (CSF1R) inhibitor, however, little information exists regarding the role of microglia in neonatal brain disorders such as hydrocephalus. Therefore, we aim to see if ablating pro-inflammatory microglia, and thus suppressing the inflammatory response, in a neonatal hydrocephalic mouse line could have beneficial effects. Methods: In this study, Plexxikon 5622 (PLX5622), a CSF1R inhibitor, was subcutaneously administered to wild-type (WT) and prh mutant mice daily from postnatal day (P) 3 to P7. MRI-estimated brain volume was compared with untreated WT and prh mutants P7-9 and immunohistochemistry of the brain sections was performed at P8 and P18-21. Results: PLX5622 injections successfully ablated IBA1-positive microglia in both the WT and prh mutants at P8. Of the microglia that are resistant to PLX5622 treatment, there was a higher percentage of amoeboid-shaped microglia, identified by morphology with retracted processes. In PLX-treated prh mutants, there was increased ventriculomegaly and no change in the total brain volume was observed. Also, the PLX5622 treatment significantly reduced myelination in WT mice at P8, although this was recovered after full microglia repopulation by P20. Microglia repopulation in the mutants worsened hypomyelination at P20. Conclusions: Microglia ablation in the neonatal hydrocephalic brain does not improve white matter edema, and actually worsens ventricular enlargement and hypomyelination, suggesting critical functions of homeostatic ramified microglia to better improve brain development with neonatal hydrocephalus. Future studies with detailed examination of microglial development and status may provide a clarification of the need for microglia in neonatal brain development. [ABSTRACT FROM AUTHOR]

Published

2023

142. Cryo-EM structures of ClC-2 chloride channel reveal the blocking mechanism of its specific inhibitor AK-42.

Author

Ma, Tao, Wang, Lei, Chai, Anping, Liu, Chao, Cui, Wenqiang, Yuan, Shuguang, Wing Ngor Au, Shannon, Sun, Liang, Zhang, Xiaokang, Zhang, Zhenzhen, Lu, Jianping, Gao, Yuanzhu, Wang, Peiyi, Li, Zhifang, Liang, Yujie, Vogel, Horst, Wang, Yu Tian, Wang, Daping, Yan, Kaige, and Zhang, Huawei

Subjects

CHLORIDE channels, CELL membranes, MOLECULAR dynamics, CHLORIDE ions, HYPERALDOSTERONISM, LEUKODYSTROPHY

Abstract

ClC-2 transports chloride ions across plasma membranes and plays critical roles in cellular homeostasis. Its dysfunction is involved in diseases including leukodystrophy and primary aldosteronism. AK-42 was recently reported as a specific inhibitor of ClC-2. However, experimental structures are still missing to decipher its inhibition mechanism. Here, we present cryo-EM structures of apo ClC-2 and its complex with AK-42, both at 3.5 Å resolution. Residues S162, E205 and Y553 are involved in chloride binding and contribute to the ion selectivity. The side-chain of the gating glutamate E205 occupies the putative central chloride-binding site, indicating that our structure represents a closed state. Structural analysis, molecular dynamics and electrophysiological recordings identify key residues to interact with AK-42. Several AK-42 interacting residues are present in ClC-2 but not in other ClCs, providing a possible explanation for AK-42 specificity. Taken together, our results experimentally reveal the potential inhibition mechanism of ClC-2 inhibitor AK-42. AK-42 was reported as a specific inhibitor of ClC-2 but its working mechanism is not clear. Here authors report cryo-EM structures of apo ClC-2 and in complex with AK-42, revealing how it inhibits ClC-2 specifically. [ABSTRACT FROM AUTHOR]

Published

2023

143. Case report: Treatment of advanced CSF1-receptor associated leukoencephalopathy with hematopoietic stem cell transplant.

Author

Bergner, Caroline G., Schäfer, Lisa, Vucinic, Vladan, Schetschorke, Birthe, Lier, Julia, Scherlach, Cordula, Rullmann, Michael, Sabri, Osama, Classen, Joseph, Platzbecker, Uwe, Kühl, Jörn-Sven, Barthel, Henryk, Köhler, Wolfgang, and Franke, Georg-Nikolaus

Subjects

HEMATOPOIETIC stem cells, STEM cell transplantation, WHITE matter (Nerve tissue), CENTRAL nervous system, LEUKOENCEPHALOPATHIES, GENETIC disorders, LEUKODYSTROPHY

Abstract

CSF1 receptor-related leukoencephalopathy is a rare genetic disorder presenting with severe, adult-onset white matter dementia as one of the leading symptoms. Within the central nervous system, the affected CSF1-receptor is expressed exclusively in microglia cells. Growing evidence implicates that replacing the defective microglia with healthy donor cells through hematopoietic stem cell transplant might halt disease progression. Early initiation of that treatment is crucial to limit persistent disability. However, which patients are suitable for this treatment is not clear, and imaging biomarkers that specifically depict lasting structural damage are lacking. In this study, we report on two patients with CSF1R-related leukoencephalopathy in whom allogenic hematopoietic stem cell transplant at advanced disease stages led to clinical stabilization. We compare their disease course with that of two patients admitted in the same timeframe to our hospital, considered too late for treatment, and place our cases in context with the respective literature. We propose that the rate of clinical progression might be a suitable stratification measure for treatment amenability in patients. Furthermore, for the first time we evaluate [18F] florbetaben, a PET tracer known to bind to intact myelin, as a novel MRI-adjunct tool to image white matter damage in CSF1R-related leukoencephalopathy. In conclusion, our data add evidence for allogenic hematopoietic stem cell transplant as a promising treatment in CSF1R-related leukoencephalopathy patients with slow to moderate disease progression. [ABSTRACT FROM AUTHOR]

Published

2023

144. Expanding the Spectrum of NUBPL -Related Leukodystrophy.

Author

Tonduti, Davide, Zambon, Alberto A., Ghezzi, Daniele, Lamantea, Eleonora, Izzo, Rossella, Parazzini, Cecilia, Baldoli, Cristina, van der Knaap, Marjo S., and Fumagalli, Francesca

Subjects

*LEUKODYSTROPHY, *CORPUS callosum, *LITERATURE reviews, *CEREBELLAR cortex, *WHITE matter (Nerve tissue), *MAGNETIC resonance imaging

Abstract

Mitochondrial leukodystrophies constitute a group of different conditions presenting with a wide range of clinical presentation but with some shared neuroradiological features. Genetic defects in NUBPL have been recognized as cause of a pediatric onset mitochondrial leukodystrophy characterized by onset at the end of the first year of life with motor delay or regression and cerebellar signs, followed by progressive spasticity. Early magnetic resonance imagings (MRIs) show white matter abnormalities with predominant involvement of frontoparietal regions and corpus callosum. A striking cerebellar involvement is usually observed. Later MRIs show spontaneous improvement of white matter abnormalities but worsening of the cerebellar involvement evolving to global atrophy and progressive involvement of brainstem. After the 7 cases initially described, 11 more subjects were reported. Some of them were similar to patients from the original series while few others broadened the phenotypic spectrum. We performed a literature review and report on a new patient who further expand the spectrum of NUBPL-related leukodystrophy. With our study we confirm that the association of cerebral white matter and cerebellar cortex abnormalities is a feature commonly observed in early stages of the disease but beside the original and so far prevalent presentation, there are also uncommon phenotypes: clinical onset can be earlier and more severe than previously thought and signs of extraneurological involvement can be observed. Brain white matter can be diffusely abnormal without anteroposterior gradient, can progressively worsen, and cystic degeneration can be present. Thalami can be involved. Basal ganglia can also become involved during disease evolution. [ABSTRACT FROM AUTHOR]

Published

2023

145. Long Noncoding RNAs in CNS Myelination and Disease.

Author

Zhang, Jing, Guan, Menglong, Zhou, Xianyao, Berry, Kalen, He, Xuelian, and Lu, Q. Richard

Subjects

*LINCRNA, *MYELINATION, *DEMYELINATION, *MYELIN sheath diseases, *NEUROLOGICAL disorders, *NON-coding RNA, *LEUKODYSTROPHY

Abstract

Myelination by oligodendrocytes is crucial for neuronal survival and function, and defects in myelination or failure in myelin repair can lead to axonal degeneration and various neurological diseases. At present, the factors that promote myelination and overcome the remyelination block in demyelinating diseases are poorly defined. Although the roles of protein-coding genes in oligodendrocyte differentiation have been extensively studied, the majority of the mammalian genome is transcribed into noncoding RNAs, and the functions of these molecules in myelination are poorly characterized. Long noncoding RNAs (lncRNAs) regulate transcription at multiple levels, providing spatiotemporal control and robustness for cell type–specific gene expression and physiological functions. lncRNAs have been shown to regulate neural cell–type specification, differentiation, and maintenance of cell identity, and dysregulation of lncRNA function has been shown to contribute to neurological diseases. In this review, we discuss recent advances in our understanding of the functions of lncRNAs in oligodendrocyte development and myelination as well their roles in neurological diseases and brain tumorigenesis. A more systematic characterization of lncRNA functional networks will be instrumental for a better understanding of CNS myelination, myelin disorders, and myelin repair. [ABSTRACT FROM AUTHOR]

Published

2023

146. The central role of the left inferior longitudinal fasciculus in the face‐name retrieval network.

Author

Burkhardt, Eléonor, Zemmoura, Ilyess, Hirsch, Fabrice, Lemaitre, Anne‐Laure, Deverdun, Jeremy, Moritz‐Gasser, Sylvie, Duffau, Hugues, and Herbet, Guillaume

Subjects

*NEUROLOGICAL disorders, *WHITE matter (Nerve tissue), *TEMPORAL lobe, *EPISODIC memory, *SEMANTIC memory, *LEUKODYSTROPHY

Abstract

Unsuccessful retrieval of proper names (PNs) is commonly observed in patients suffering from neurological conditions such as stroke or epilepsy. While a large body of works has suggested that PN retrieval relies on a cortical network centered on the left anterior temporal lobe (ATL), much less is known about the white matter connections underpinning this process. Sparse studies provided evidence for a possible role of the uncinate fasciculus, but the inferior longitudinal fasciculus (ILF) might also contribute, since it mainly projects into the ATL, interconnects it with the posterior lexical interface and is engaged in common name (CN) retrieval. To ascertain this hypothesis, we assessed 58 patients having undergone a neurosurgery for a left low‐grade glioma by means of a famous face naming (FFN) task. The behavioural data were processed following a multilevel lesion approach, including location‐based analyses, voxel‐based lesion‐symptom mapping (VLSM) and disconnection‐symptom mapping. Different statistical models were generated to control for sociodemographic data, familiarity, biographical knowledge and control cognitive performances (i.e., semantic and episodic memory and CN retrieval). Overall, VLSM analyses indicated that damage to the mid‐to‐anterior part of the ventro‐basal temporal cortex was especially associated with PN retrieval deficits. As expected, tract‐oriented analyses showed that the left ILF was the most strongly associated pathway. Our results provide evidence for the pivotal role of the ILF in the PN retrieval network. This novel finding paves the way for a better understanding of the pathophysiological bases underlying PN retrieval difficulties in the various neurological conditions marked by white matter abnormalities. [ABSTRACT FROM AUTHOR]

Published

2023

147. The genetic and phenotypic spectra of adult genetic leukoencephalopathies in a cohort of 309 patients.

Author

Wu, Chujun, Wang, Mengwen, Wang, Xingao, Li, Wei, Li, Shaowu, Chen, Bin, Niu, Songtao, Tai, Hongfei, Pan, Hua, and Zhang, Zaiqiang

Subjects

*MYELIN sheath diseases, *LEUKOENCEPHALOPATHIES, *DNA sequencing, *PHENOTYPES, *MITOCHONDRIAL DNA, *ADULTS, *GENETIC disorders

Abstract

Genetic leukoencephalopathies (gLEs) are a highly heterogeneous group of rare genetic disorders. The spectrum of gLEs varies among patients of different ages. Distinct from the relatively more abundant studies of gLEs in children, only a few studies that explore the spectrum of adult gLEs have been published, and it should be noted that the majority of these excluded certain gLEs. Thus, to date, no large study has been designed and conducted to characterize the genetic and phenotypic spectra of gLEs in adult patients. We recruited a consecutive series of 309 adult patients clinically suspected of gLEs from Beijing Tiantan Hospital between January 2014 and December 2021. Whole exome sequencing, mitochondrial DNA sequencing, and repeat analysis of NOTCH2NLC, FMR1, DMPK and ZNF9 were performed for patients. We describe the genetic and phenotypic spectra of the set of patients with a genetically confirmed diagnosis and summarize their clinical and radiological characteristics. A total of 201 patients (65%) were genetically diagnosed, while 108 patients (35%) remained undiagnosed. The most frequent diseases were NOTCH3 (25%), NOTCH2NLC (19%), ABCD1 (9%), CSF1R (7%), and HTRA1 (5%)-related leukoencephalopathies. Based on a previously proposed pathological classification, the gLEs in our cohort were divided into leukovasculopathies (35%), leuko-axonopathies (31%), myelin disorders (21%), microgliopathies (7%), and astrocytopathies (6%). Patients with NOTCH3 mutations accounted for 70% of the leukovasculopathies, followed by HTRA1 (13%) and COL4A1/2 (9%). The leuko-axonopathies contained the richest variety of associated genes, of which NOTCH2NLC comprised 62%. Among myelin disorders, demyelinating leukoencephalopathies (61%)-mainly adrenoleukodystrophy and Krabbe disease-accounted for the majority, while hypomyelinating leukoencephalopathies (2%) were rare. CSF1R was the only mutated gene detected in microgliopathy patients. Leukoencephalopathy with vanishing white matter disease due to mutations in EIF2B2-5 accounted for half of the astrocytopathies. We characterized the genetic and phenotypic spectra of adult gLEs in a large Chinese cohort. The most frequently mutated genes were NOTCH3, NOTCH2NLC, ABCD1, CSF1R, and HTRA1. [ABSTRACT FROM AUTHOR]

Published

2023

148. An approach to reporting paediatric leukoencephalopathy and leukodystrophies.

Author

Davies, A., Tolliday, A., Craven, I., and Connolly, D.J.A.

Subjects

*LEUKODYSTROPHY, *LEUKOENCEPHALOPATHIES, *PEDIATRICS, *NEURAL development, *SYMPTOMS

Abstract

The leukodystrophies (LD) and leukoencephalopathies (LE) are a diverse group of conditions involving the cerebral white and grey matter. There is heterogeneity in the clinical presentations, imaging features, and biochemical dysfunction. Given the number of conditions and varied imaging appearances, this topic can be difficult for non-specialist radiologists who do not routinely work in dedicated paediatric neuroradiology centres. This article will aim to provide a simplified and step-wise approach to assessing suspected LD/LE, focussing on the more common diagnoses you may encounter in the UK. Additionally, it will highlight important non-LD/LE differentials, which if considered early, may significantly alter treatment and prognosis. By the end of this review, we hope the reader will begin to develop an awareness of physiological paediatric brain development in terms of normal myelination; the ability to recognise and categorise the distribution of abnormal signal based on the established diagnostic framework outlined by Schiffmann & Van der Knapp; and be aware of potential non-LD/LE radiological mimics. [ABSTRACT FROM AUTHOR]

Published

2023

149. A p.Val412Serfs pathogenic variant associated with Wolfram-like syndrome and leukodystrophy

Author

Ayca Kocaaga, Sevgi Yimenicioglu, and Murat Bayav

Subjects

Dominant inheritance, Leukodystrophy, Optic atrophy, WFS1 (Wolframin) gene, Wolfram-like syndrome, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Abstract Background Wolfram syndrome is due to a mutation of the WFS1 gene that codes for the transmembrane protein wolframin. This protein is located in the endoplasmic reticulum and is expressed at higher concentrations in the beta cells of pancreatic islets and the brain. The term "Wolfram syndrome spectrum" is often used because of its genetic and clinical heterogeneity. Disorders associated with the WFS1 gene include Wolfram syndrome following an autosomal recessive inheritance pattern and Wolfram-like syndrome following an autosomal dominant inheritance pattern, and congenital cataract. Here, we report a case with Wolfram-like syndrome presented with bilateral congenital cataract, optic atrophy, nystagmus, ataxia, mild intellectual disability, epilepsy and leukodystrophy. Case report Magnetic resonance imaging (MRI) showed bilateral cerebral T2 and flair hyperintensities that causes diffusion restriction in some areas with hypoperfusion. Bilateral T2 cerebellar central white matter hyperintensities and atrophy of brain stem were revealed by the brain MRI. There was also found evidence of a proximal cervical cord lesion and syrinx cavity in the vertebral MRI. The heterozygous frame-shift (c.1230_1233delCTCT; p.Val412Serfs) mutation in the WFS1 gene. This heterozygous pathogenic variant in the WFS1 gene was identified in both the father and grandmother. Conclusions To our knowledge, this is a novel Wolfram-like syndrome-related phenotype. This case report broadens the currently known phenotypic presentations of Wolfram-like syndrome and suggests that the p.Val412Serfs variant in the WFS1 gene may be associated with syrinx cavity and leukodystrophy.

Published

2023

150. Cavitating leukodystrophy in a case of mitochondrial complex III deficiency due to LYRM7 mutation

Author

Rezaei, Mojtaba, Dourandish, Zahra, Kiani Mehr, Gilda, Ghorbani, Askar, and Fatehi, Farzad

Published

2024