Your search keyword '"Abreu, Nicolas J."' showing total 18 results

1. Severe neurodevelopmental phenotype, diagnostic, and treatment challenges in patients with SECISBP2 deficiency.

Author

Stoupa A, Franca MM, Abdulhadi-Atwan M, Fujisawa H, Korwutthikulrangsri M, Marchand I, Polak G, Beltrand J, Polak M, Kariyawasam D, Liao XH, Raimondi C, Steigerwald C, Abreu NJ, Bauer AJ, Carré A, Taneja C, Mekhoubad AB, and Dumitrescu AM

Abstract

Purpose: Defects in the gene encoding selenocysteine insertion sequence binding protein 2, SECISBP2, result in global impaired selenoprotein synthesis manifesting a complex syndrome with characteristic serum thyroid function tests due to impaired thyroid hormone metabolism. Knowledge about this multisystemic defect remains limited., Methods: Genetic and laboratory investigations were performed in affected members from 6 families presenting with short stature and failure to thrive., Results: Four probands presented a complex neurodevelopmental profile, including absent speech, autistic features, and seizures. Pediatric neurological evaluation prompted genetic investigations leading to the identification of SECISBP2 variants before knowing the characteristic thyroid tests in 2 cases. Thyroid hormone treatment improved motor development, whereas speech and intellectual impairments persisted. This defect poses great diagnostic and treatment challenges for clinicians, as illustrated by a case that escaped detection for 20 years because SECISBP2 was not included in the neurodevelopmental genetic panel, and his complex thyroid status prompted antithyroid treatment instead., Conclusion: This syndrome uncovers the role of selenoproteins in humans. The severe neurodevelopmental disabilities manifested in 4 patients with SECISBP2 deficiency highlight an additional phenotype in this multisystem disorder. Early diagnosis and treatment are required, and long-term evaluation will determine the full spectrum of manifestations and the impact of therapy., Competing Interests: Conflict of Interest The authors declare no conflicts of interest, (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

2. Development of the APBD-SQ, a novel patient-reported outcome for health-related quality of life in adult polyglucosan body disease.

Author

Wilson GE, Goldman DS, Saxe H, Li X, Goldberg JD, Lau HA, and Abreu NJ

Subjects

Humans, Male, Female, Middle Aged, Adult, Aged, Severity of Illness Index, Surveys and Questionnaires, Self Report, Nervous System Diseases, Quality of Life psychology, Glycogen Storage Disease psychology, Patient Reported Outcome Measures

Abstract

Adult polyglucosan body disease (APBD) is a rare autosomal recessive glycogen storage disorder that leads to slowly progressive multi-organ dysfunction in adulthood. A novel disease-specific patient-reported outcome measure was created and administered to assess symptom burden and health-related quality of life (HR-QOL) in APBD. Thirty-six participants between 30 and 79 years of age (83% ≥60 years, 56% male) completed the anonymous questionnaire independently or with a caregiver proxy (75% self-report). Unemployment predicted an 18.3 (95% CI: 2.8, 33.8; p = 0.028) higher composite disease severity score and a 28.8 (95% CI: 8.2, 49.4; p = 0.010) higher composite HR-QOL score. Use of one or more assistive devices also predicted a 29.3 (95% CI: 8.3, 50.4; p = 0.011) higher composite disease severity score and a 41.8 (95% CI: 10.9, 72.8; p = 0.013) higher composite HR-QOL score. Proxy survey completion predicted a 19.4 (95% CI: 4.1, 34.7; p = 0.020) higher composite disease severity score compared to self-report. Older age at survey completion predicted a 27.4 higher composite HR-QOL score (95% CI: 2.5, 52.4; p = 0.039) for participants in their sixties compared to those between 30 and 59 years old. The development of the Adult Polyglucosan Body Disease questionnaire on Symptom burden and health-related Quality of life (APBD-SQ) marks an important stride forward in capturing the patient experience as a tool for disease monitoring and future research., Competing Interests: Declaration of competing interest D.S.G. and H.S. serve on the Executive Board of the APBDRF. H.A.L. has received personal compensation for consulting, serving on a scientific advisory board, speaking, or other activities with Actelion, Amicus, Biomarin, Chiesi, Indorsia, Pfizer, Prevail Therapeutics, Sanofi Genzyme, Ultragenyx, Shire. H.A.L. has also received research support from Amicus, Biomarin, Sanofi Genzyme, GlaxoSmithKline, Mallinckrodt, Protalix, Pfizer, Sangamo, Shire, Ultragenyx and is currently employed by Ultragenyx. N.J.A. has received research support from Amicus Therapeutics, BioMarin, Sangamo Therapeutics, Sanofi, and Takeda Pharmaceuticals. G.E.W., X.L., and J.D.G. have nothing to disclose., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

3. Neuro-Ophthalmic Manifestations of Adult Polyglucosan Body Disease.

Author

Dugue AG, Abreu NJ, Pillai C, Galetta SL, and Grossman SN

Abstract

Background: Adult polyglucosan body disease (APBD) is caused by a deficiency in glycogen branching enzyme that leads to polyglucosan accumulation in multiple organs. It has a progressive clinical course with prominent neurologic manifestations. We aim to describe the neuro-ophthalmic manifestations of APBD., Methods: This is a case series of 3 individuals with genetically proven APBD. Written informed consent was provided by the brothers. We also performed a literature review on the current state of knowledge on APBD through PubMed., Results: Brother 1 developed gait imbalance and length-dependent polyneuropathy in his 40s followed by progressive urinary symptoms in his 50s. He reported diplopia and blurry vision in his 60s. Neuro-ophthalmic assessment revealed bilateral optic neuropathy, convergence insufficiency, and a right fourth nerve palsy. Genetic testing showed a homozygous pathogenic variant in GBE1 c.986A>C p.Tyr329Ser. Brother 2 developed progressive urinary symptoms in his 40s that were followed by cognitive deficits, length-dependent polyneuropathy, and lower extremity weakness in his 50s and 60s. He reported blurred vision, and neuro-ophthalmic evaluation revealed bilateral optic neuropathy. Genetic testing revealed the same variant as Brother 1, GBE1 c.986A>C p.Tyr329Ser. Brother 3 developed progressive urinary urgency and lower extremity weakness in his 50s followed by a length-dependent polyneuropathy in his 60s. He reported diplopia and blurry vision in his 70s. Neuro-ophthalmic assessment revealed bilateral optic neuropathy and convergence insufficiency. Genetic testing revealed the same variant as Brothers 1 and 2, GBE1 c.986A>C p.Tyr329Ser., Conclusions: There is an array of afferent and efferent neuro-ophthalmic manifestations in APBD. Neuro-ophthalmic evaluation is crucial in evaluating and treating patients with APBD, particularly in those with visual dysfunction., Competing Interests: The authors report no conflicts of interest., (Copyright © 2024 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the North American Neuro-Opthalmology Society.)

Published

2024

4. Rare predicted deleterious FEZF2 variants are associated with a neurodevelopmental phenotype.

Author

Garber A, Weingarten LS, Abreu NJ, Elloumi HZ, Haack T, Hildebrant C, Martínez-Gil N, Mathews J, Müller AJ, Valenzuela Palafoll I, Steigerwald C, and Chung WK

Subjects

Adolescent, Child, Child, Preschool, Female, Humans, Male, Developmental Disabilities genetics, Developmental Disabilities pathology, Genetic Association Studies, Genetic Predisposition to Disease, Nerve Tissue Proteins genetics, Transcription Factors genetics, Intellectual Disability genetics, Intellectual Disability pathology, Neurodevelopmental Disorders genetics, Neurodevelopmental Disorders pathology, Phenotype

Abstract

FEZF2 encodes a transcription factor critical to neurodevelopment that regulates other neurodevelopment genes. Rare variants in FEZF2 have previously been suggested to play a role in autism, and cases of 3p14 microdeletions that include FEZF2 share a neurodevelopmental phenotype including mild dysmorphic features and intellectual disability. We identified seven heterozygous predicted deleterious variants in FEZF2 (three frameshifts, one recurrent missense in two independent cases, one nonsense, and one complete gene deletion) in unrelated individuals with neurodevelopmental disorders including developmental delay/intellectual disability, autism, and/or attention-deficit/hyperactivity. Variants were confirmed to be de novo in five of seven cases and paternally inherited from an affected father in one. Predicted deleterious variants in FEZF2 may affect the expression of genes that are involved in fate choice pathways in developing neurons, and thus contribute to the neurodevelopmental phenotype. Future studies are needed to clarify the mechanism by which FEZF2 leads to this neurodevelopmental disorder., (© 2024 Wiley Periodicals LLC.)

Published

2024

5. Relapsing White Matter Disease and Subclinical Optic Neuropathy: From the National Multiple Sclerosis Society Case Conference Proceedings

Author

O'Neill KA, Dugue A, Abreu NJ, Balcer LJ, Branche M, Galetta S, Graves J, Kister I, Magro C, Miller C, Newsome SD, Pappas J, Rucker J, Steigerwald C, William CM, Zamvil SS, Grossman SN, and Krupp LB

Subjects

Adolescent, Male, Humans, Contrast Media, Hypesthesia, Gadolinium, Optic Nerve Diseases diagnosis, Optic Nerve Diseases etiology, Leukoencephalopathies

Abstract

A 16-year-old adolescent boy presented with recurrent episodes of weakness and numbness. Brain MRI demonstrated subcortical, juxtacortical, and periventricular white matter T2 hyperintensities with gadolinium enhancement. CSF was positive for oligoclonal bands that were not present in serum. Despite treatment with steroids, IV immunoglobulins, plasmapheresis, and rituximab, he continued to have episodes of weakness and numbness and new areas of T2 hyperintensity on imaging. Neuro-ophthalmologic examination revealed a subclinical optic neuropathy with predominant involvement of the papillomacular bundle. Genetic evaluation and brain biopsy led to an unexpected diagnosis.

Published

2024

6. Factors Associated With Underutilization of Genetic Testing in Autism Spectrum Disorders.

Author

Abreu NJ, Chiujdea M, Liu S, Zhang B, and Spence SJ

Subjects

Child, Humans, Microarray Analysis, Genetic Testing, Family, Autism Spectrum Disorder diagnosis, Autism Spectrum Disorder genetics, Intellectual Disability genetics

Abstract

Background: We sought to identify patient and provider factors associated with low completion of genetic testing, specifically chromosomal microarray (CMA), for autism spectrum disorder (ASD)., Methods: Medical record review was conducted of children newly diagnosed with ASD without prior genetic testing at a single academic medical center from February 2015 through January 2016., Results: Only 41.9% of individuals with ASD completed CMA testing over at least 18 months from diagnosis (n = 140 of 334). Time to CMA completion varied, with a median of 86.5 days (interquartile range 2 to 214.5 days). Provider recommendation of genetic testing at the diagnostic visit and greater number of follow-up visits were associated with CMA completion. On multivariate regression, CMA completion was inversely associated with age (odds ratio [OR] = 0.8 for each year older, 95% confidence interval [CI] 0.7, 0.9; P = 0.001) and directly associated with intellectual disability or global developmental delay (OR = 2.2, 95% CI 1.3, 3.8; P = 0.004), first-degree relative with ASD (OR = 2.5, 95% CI 1.0, 6.0; P = 0.044), and public insurance (OR = 1.7, 95% CI 1.0, 2.9; P = 0.037). Parental concern and cost/insurance coverage were the most frequently documented barriers., Conclusions: Workflows to support early genetic testing recommendation and ordering soon after diagnosis may increase utilization, incorporating both family and provider perspectives. Genetic counseling highlighting the utility of genetic testing across the life span, phenotypic variability of genetic disorders, and possibility of de novo variants in ASD may also improve utilization., Competing Interests: Declaration of competing interest None., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2024

7. CLN2 disease resulting from a novel homozygous deep intronic splice variant in TPP1 discovered using long-read sequencing.

Author

Steigerwald C, Borsuk J, Pappas J, Galey M, Scott A, Devaney JM, Miller DE, and Abreu NJ

Subjects

Humans, Serine Proteases genetics, Aminopeptidases genetics, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases genetics, Tripeptidyl-Peptidase 1, Neuronal Ceroid-Lipofuscinoses genetics

Abstract

Neuronal ceroid lipofuscinosis type 2 (CLN2) is an autosomal recessive neurodegenerative disorder with enzyme replacement therapy available. We present two siblings with a clinical diagnosis of CLN2 disease, but no identifiable TPP1 variants after standard clinical testing. Long-read sequencing identified a homozygous deep intronic variant predicted to affect splicing, confirmed by clinical DNA and RNA sequencing. This case demonstrates how traditional laboratory assays can complement emerging molecular technologies to provide a precise molecular diagnosis., Competing Interests: Declaration of Competing Interest DEM holds stock options in MyOme and is on a scientific advisory board at Oxford Nanopore Technologies (ONT), is engaged in a research agreement with ONT, and they have paid for his travel to speak on their behalf. NJA has received research support from Amicus Therapeutics, Sangamo Therapeutics, Sanofi, and Takeda Pharmaceuticals. CGS receives consulting fees from Vigil Neuroscience. AIS is a consultant for Circumvent Pharmaceuticals. JMD is an employee of GeneDx, LLC. The other authors declare no conflicts., (Copyright © 2023. Published by Elsevier Inc.)

Published

2023

8. Pearls & Oy-sters: CSF1R -Related Leukoencephalopathy With Spinal Cord Lesions Mimicking Multiple Sclerosis.

Author

Jain A, Arena VP, Steigerwald C, Borja MJ, Kister I, and Abreu NJ

Subjects

Adult, Humans, Magnetic Resonance Imaging, Mutation, Receptor Protein-Tyrosine Kinases, Spinal Cord pathology, Multiple Sclerosis diagnosis, Multiple Sclerosis diagnostic imaging, Leukoencephalopathies diagnostic imaging, Leukoencephalopathies genetics

Abstract

CSF1R -related leukoencephalopathy is an autosomal dominant neurologic disorder causing microglial dysfunction with a wide range of neurologic complications, including motor dysfunction, dementia, and seizures. This case report highlights an unusual presentation of CSF1R -related leukoencephalopathy with radiographic spinal cord involvement initially diagnosed as multiple sclerosis. This case highlights the importance of considering adult-onset neurogenetic disorders in the setting of white matter disease. Genetic testing provides a confirmatory diagnosis for an expanding number of adult-onset leukoencephalopathies and informs therapeutic decision-making., (© 2023 American Academy of Neurology.)

Published

2023

9. Neuro-Ophthalmologic Variability in Presentation of Genetically Confirmed Wolfram Syndrome: A Case Series and Review.

Author

Jauregui R, Abreu NJ, Golan S, Panarelli JF, Sigireddi M, Nayak GK, Gold DM, Rucker JC, Galetta SL, and Grossman SN

Abstract

Wolfram syndrome is a neurodegenerative disorder caused by pathogenic variants in the genes WFS1 or CISD2 . Clinically, the classic phenotype is composed of optic atrophy, diabetes mellitus type 1, diabetes insipidus, and deafness. Wolfram syndrome, however, is phenotypically heterogenous with variable clinical manifestations and age of onset. We describe four cases of genetically confirmed Wolfram syndrome with variable presentations, including acute-on-chronic vision loss, dyschromatopsia, and tonic pupils. All patients had optic atrophy, only three had diabetes, and none exhibited the classic Wolfram phenotype. MRI revealed a varying degree of the classical features associated with the syndrome, including optic nerve, cerebellar, and brainstem atrophy. The cohort's genotype and presentation supported the reported phenotype-genotype correlations for Wolfram, where missense variants lead to milder, later-onset presentation of the Wolfram syndrome spectrum. When early onset optic atrophy and/or diabetes mellitus are present in a patient, a diagnosis of Wolfram syndrome should be considered, as early diagnosis is crucial for the appropriate referrals and management of the associated conditions. Nevertheless, the condition should also be considered in otherwise unexplained, later-onset optic atrophy, given the phenotypic spectrum.

Published

2023

10. Two cases of MT-ND5 -related mitochondrial disorder misdiagnosed as seronegative neuromyelitis optica spectrum disorder.

Author

Wilkins SR, Yu AW, Steigerwald C, Tanji K, Iglesias AD, Hirano M, Kister I, Riley CS, and Abreu NJ

Subjects

Humans, Aquaporin 4, Autoantibodies, Magnetic Resonance Imaging, Diagnostic Errors, Neuromyelitis Optica, Mitochondrial Diseases diagnosis, Mitochondrial Diseases genetics

Abstract

Neuromyelitis optica spectrum disorder (NMOSD) is an autoimmune disease primarily affecting the optic nerves and spinal cord, which is usually associated with anti-aquaporin-4 antibodies. Here, we present two individuals who were negative for anti-aquaporin-4 antibodies and were initially diagnosed with seronegative NMOSD. Each patient's clinical course and radiographic features raised suspicion for an alternative disease process. Both individuals were found to have pathogenic variants of MT-ND5 , encoding subunit 5 of mitochondrial complex I, ultimately leading to a revised diagnosis of a primary mitochondrial disorder. These cases illustrate the importance of biochemical and genetic testing in atypical cases of NMOSD.

Published

2023

11. Deep Brain Stimulation for the Management of AIFM1-Related Disabling Tremor: A Case Series.

Author

Tunyi J, Abreu NJ, Tripathi R, Mathew MT, Mears A, Agrawal P, Thakur V, Rezai AR, and Reyes EL

Subjects

Humans, Male, Apoptosis Inducing Factor genetics, Apoptosis Inducing Factor metabolism, Quality of Life, Tremor genetics, Tremor therapy, Charcot-Marie-Tooth Disease, Deep Brain Stimulation

Abstract

The AIFM1 gene encodes a mitochondrial protein that acts as a flavin adenine dinucleotide-dependent nicotinamide adenine dinucleotide oxidase and apoptosis regulator. Monoallelic pathogenic AIFM1 variants result in a spectrum of X-linked neurological disorders, including Cowchock syndrome. Common features in Cowchock syndrome include a slowly progressive movement disorder, cerebellar ataxia, progressive sensorineural hearing loss, and sensory neuropathy. We identified a novel maternally inherited hemizygous missense AIFM1 variant, c.1369C>T p.(His457Tyr), in two brothers with clinical features consistent with Cowchock syndrome using next-generation sequencing. Both individuals had a progressive complex movement disorder phenotype, including disabling tremor poorly responsive to medications. Deep brain stimulation (DBS) of the ventral intermediate thalamic nucleus ameliorated contralateral tremor and improved their quality of life; this suggests the beneficial role for DBS in treatment-resistant tremor within AIFM1-related disorders., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

12. Pathogenic missense variants altering codon 336 of GARS1 lead to divergent dominant phenotypes.

Author

Meyer AP, Forrest ME, Nicolau S, Wiszniewski W, Bland MP, Tsao CY, Antonellis A, and Abreu NJ

Subjects

Humans, Codon, Mutation, Phenotype, Charcot-Marie-Tooth Disease genetics, Glycine-tRNA Ligase genetics

Abstract

Heterozygosity for missense variants and small in-frame deletions in GARS1 has been reported in patients with a range of genetic neuropathies including Charcot-Marie-Tooth disease type 2D (CMT2D), distal hereditary motor neuropathy type V (dHMN-V), and infantile spinal muscular atrophy (iSMA). We identified two unrelated patients who are each heterozygous for a previously unreported missense variant modifying amino-acid position 336 in the catalytic domain of GARS1. One patient was a 20-year-old woman with iSMA, and the second was a 41-year-old man with CMT2D. Functional studies using yeast complementation assays support a loss-of-function effect for both variants; however, this did not reveal variable effects that might explain the phenotypic differences. These cases expand the mutational spectrum of GARS1-related disorders and demonstrate phenotypic variability based on the specific substitution at a single residue., (© 2022 Wiley Periodicals LLC.)

Published

2022

13. Novel truncating variant in KMT2E associated with cerebellar hypoplasia and velopharyngeal dysfunction.

Author

Abreu NJ, Siemon AE, Baylis AL, Kirschner RE, Pfau RB, Ho ML, Hickey SE, and Truxal KV

Abstract

KMT2E -related neurodevelopmental disorder is a recently described intellectual disability syndrome often with speech difficulties. Here, we describe an individual with a heterozygous frameshift variant in KMT2E (NM_182931.2:c.2334_2337delTTAC, p.[Tyr779AlafsTer41]), intellectual disability, cerebellar hypoplasia, and velopharyngeal dysfunction. This case suggests potential mechanisms of speech disturbance in the disorder, requiring further investigation., Competing Interests: None of the authors has a relevant conflict of interest., (© 2022 The Authors. Clinical Case Reports published by John Wiley & Sons Ltd.)

Published

2022

14. Editorial commentary on "Gait phenotype in Batten disease: A marker of disease progression".

Author

Abreu NJ and de Los Reyes EC

Subjects

Disease Progression, Gait, Humans, Lysosomes, Phenotype, Neuronal Ceroid-Lipofuscinoses genetics

Abstract

Batten disease, also known as neuronal ceroid lipofuscinosis, refers to a diverse group of 13 hereditary inborn errors of metabolism resulting in the abnormal accumulation of autofluorescent storage material in lysosomes leading to neurodegeneration, typically with associated intractable epilepsy, behavioral dysregulation, cognitive, motor, language and visual decline, as well as a shortened life expectancy [1]. Assessment of disease progression within this population is fraught with difficulty because individuals may have limited attention or cooperation affecting compliance with requested tasks, or have visual impairment reducing options for methods of assessment. Further, language and cognitive assessments have been designed to assess typically developing individuals based on specific age limits, which then fail to capture low developmental functioning once the mental age of the individual drops below the basal age of the assessment tool. Yet, metrics to measure disease progression are essential to inform therapeutic decision-making, prognostication, and clinical trial outcomes., (Copyright © 2021. Published by Elsevier Ltd.)

Published

2021

15. Longitudinal MRI brain volume changes over one year in children with mucopolysaccharidosis types IIIA and IIIB.

Author

Abreu NJ, Selvaraj B, Truxal KV, Moore-Clingenpeel M, Zumberge NA, McNally KA, McBride KL, Ho ML, and Flanigan KM

Subjects

Adolescent, Brain metabolism, Child, Child, Preschool, Corpus Callosum diagnostic imaging, Corpus Callosum metabolism, Corpus Callosum pathology, Female, Humans, Longitudinal Studies, Magnetic Resonance Imaging, Male, Mucopolysaccharidosis III metabolism, Mucopolysaccharidosis III pathology, White Matter diagnostic imaging, White Matter metabolism, White Matter pathology, Brain diagnostic imaging, Learning physiology, Mucopolysaccharidosis III diagnostic imaging

Abstract

Objective: To quantify changes in segmented brain volumes over 12 months in children with mucopolysaccharidosis types IIIA and IIIB (MPS IIIA and IIIB)., Methods: In order to establish suitable outcome measures for clinical trials, twenty-five children greater than 2 years of age were enrolled in a prospective natural history study of MPS IIIA and IIIB at Nationwide Children's Hospital. Data from sedated non-contrast brain 3 T MRIs and neuropsychological measures were reviewed from the baseline visit and at 12-month follow-up. No intervention beyond standard clinical care was provided. Age- and sex-matched controls were gathered from the National Institute of Mental Health Data Archive. Automated brain volume segmentation with longitudinal processing was performed using FreeSurfer., Results: Of the 25 subjects enrolled with MPS III, 17 children (4 females, 13 males) completed at least one MRI with interpretable volumetric data. The ages ranged from 2.8 to 13.7 years old (average 7.2 years old) at enrollment, including 8 with MPS IIIA and 9 with MPS IIIB. At baseline, individuals with MPS III demonstrated reduced cerebral white matter and corpus callosum volumes, but greater volumes of the lateral ventricles, cerebellar cortex, and cerebellar white matter compared to controls. Among the 13 individuals with MPS III with two interpretable MRIs, there were annualized losses or plateaus in supratentorial brain tissue volumes (cerebral cortex -42.10 ± 18.52 cm 3 /year [mean ± SD], cerebral white matter -4.37 ± 11.82 cm 3 /year, subcortical gray matter -6.54 ± 3.63 cm 3 /year, corpus callosum -0.18 ± 0.62 cm 3 /yr) and in cerebellar cortex (-0.49 ± 12.57 cm 3 /year), with a compensatory increase in lateral ventricular volume (7.17 ± 6.79 cm 3 /year). Reductions in the cerebral cortex and subcortical gray matter were more striking in individuals younger than 8 years of age. Greater cerebral cortex volume was associated with higher fine and gross motor functioning on the Mullen Scales of Early Learning, while greater subcortical gray matter volume was associated with higher nonverbal functioning on the Leiter International Performance Scale. Larger cerebellar cortex was associated with higher receptive language performance on the Mullen, but greater cerebellar white matter correlated with worse adaptive functioning on the Vineland Adaptive Behavioral Scales and visual problem-solving on the Mullen., Conclusions: Loss or plateauing of supratentorial brain tissue volumes may serve as longitudinal biomarkers of MPS III age-related disease progression compared to age-related growth in typically developing controls. Abnormally increased cerebellar white matter in MPS III, and its association with worse performance on neuropsychological measures, suggest the possibility of pathophysiological mechanisms distinct from neurodegeneration-associated atrophy that warrant further investigation., (Copyright © 2021. Published by Elsevier Inc.)

Published

2021

16. Overview of gene therapy in spinal muscular atrophy and Duchenne muscular dystrophy.

Author

Abreu NJ and Waldrop MA

Subjects

Biological Products, Humans, Oligonucleotides, Antisense therapeutic use, Recombinant Fusion Proteins, United States, Genetic Therapy, Muscular Atrophy, Spinal genetics, Muscular Atrophy, Spinal therapy, Muscular Dystrophy, Duchenne genetics, Muscular Dystrophy, Duchenne therapy

Abstract

Both 5q-linked spinal muscular atrophy (SMA) and Duchenne muscular dystrophy (DMD) are fatal monogenic neuromuscular disorders caused by loss-of-function mutations. SMA is an autosomal recessive disorder affecting motor neurons that is typically caused by homozygous whole-gene deletions of SMN1. DMD is an X-linked recessive muscle disease most often due to exon deletions, but also duplications and smaller sized variants within the DMD gene. Gene replacement therapy offers the opportunity to correct the underlying genetic defect by the introduction of a functional gene. We review the transformative work from clinical trials to United States Food and Drug Administration approval of onasemnogene abeparvovec-xioi in SMA and its application in clinical practice and the early results of microdystrophin delivery in DMD. We also review the introduction of antisense oligonucleotides to alter pre-messenger RNA splicing to promote exon inclusion (as in nusinersen in SMA) or exclusion (as in eteplirsen in DMD) into neuromuscular therapeutics. There are multiple promising novel genetically mediated therapies on the horizon, which in aggregate point towards a hopeful future for individuals with SMA and DMD., (© 2020 Wiley Periodicals LLC.)

Published

2021

17. Emerging Subspecialties in Neurology: Neurodevelopmental disabilities.

Author

Abreu NJ, Urion DK, and Asato MR

Subjects

Humans, Curriculum, Internship and Residency, Neurodevelopmental Disorders, Neurology education, Pediatrics education

Published

2020

18. Homozygous variants in AMPD2 and COL11A1 lead to a complex phenotype of pontocerebellar hypoplasia type 9 and Stickler syndrome type 2.

Author

Abreu NJ, Koboldt DC, Gastier-Foster JM, Dave-Wala A, Flanigan KM, and Waldrop MA

Subjects

Cerebellar Diseases diagnosis, Cerebellar Diseases diagnostic imaging, Cerebellar Diseases pathology, Child, Preschool, Collagen Type XI genetics, Connective Tissue Diseases diagnosis, Connective Tissue Diseases diagnostic imaging, Connective Tissue Diseases pathology, Exome genetics, Female, Homozygote, Humans, Infant, Magnetic Resonance Imaging, Male, Mutation genetics, Pedigree, Phenotype, Vitreous Detachment diagnosis, Vitreous Detachment diagnostic imaging, Vitreous Detachment pathology, AMP Deaminase genetics, Cerebellar Diseases genetics, Collagen Type XI deficiency, Connective Tissue Diseases genetics, Vitreous Detachment genetics

Abstract

Pontocerebellar hypoplasia type 9 (PCH9) is an autosomal recessive neurodevelopmental disorder caused by pathogenic variants in the AMPD2 gene. We evaluated the son of a consanguineous couple who presented with profound hypotonia and global developmental delay. Other features included sensorineural hearing loss, asymmetric astigmatism, and high myopia. Clinical whole-exome sequence analysis identified a homozygous missense variant in AMPD2 (NM_001257360.1:c.2201C > T, p.[Pro734Leu]) that has not been previously reported. Given the strong phenotypic overlap with PCH9, including the identification of the typical "Figure 8" appearance of the brainstem on neuroimaging, we suspect this variant was causative of the neurodevelopmental disability in this individual. An additional homozygous nonsense variant in COL11A1 (NM_001854.4:c.1168G > T, p.[Glu390Ter]) was identified. Variants in this alternatively spliced region of COL11A1 have been identified to cause an autosomal recessive form of Stickler syndrome type 2 characterized by sensorineural hearing loss and eye abnormalities, but without musculoskeletal abnormalities. The COL11A1 variant likely also contributed to the individual's phenotype, suggesting two potentially relevant genetic findings. This challenging case highlights the importance of detailed phenotypic characterization when interpreting whole exome data., (© 2019 Wiley Periodicals, Inc.)

Published

2020