Your search keyword '"Martinez-Cerdeno V"' showing total 25 results

1. Fragile X associated tremor/ataxia syndrome: its clinical presentation, pathology, and treatment.

Author

Salcedo-Arellano, MJ, Hagerman, RJ, and Martinez-Cerdeno, V

Subjects

Biological Psychology, Psychology, Rare Diseases, Intellectual and Developmental Disabilities (IDD), Clinical Research, Aging, Brain Disorders, Neurodegenerative, Neurosciences, Genetics, Fragile X Syndrome, Aetiology, 2.1 Biological and endogenous factors, Neurological, Antidepressive Agents, Ataxia, Brain, Deep Brain Stimulation, Female, Fragile X Mental Retardation Protein, Humans, Male, Memantine, Neurologic Examination, Pregnanolone, Symptom Assessment, Tremor, Degeneration, FMR1, FMRP, Fragile X, Inclusion, Motor alteration, Neurology & Neurosurgery

Abstract

The fragile X associated tremor/ataxia syndrome (FXTAS) is a neurodegenerative disease associated with the repetition of CGG triplets (55-200 CGG repetitions) in the FMR1 gene. The premutation of the FMR1 gene, contrasting with the full mutation (more than 200 CGG repetitions), presents an increased production of messenger and a similar or slightly decreased production of FMRP protein. FXTAS affects 40% of men and 16% of women carriers of the premutation. It presents with a wide constellation of neurological signs such as intention tremor, cerebellar ataxia, parkinsonism, executive function deficits, peripheral neuropathy and cognitive decline leading to dementia among others. In this review, we present what is currently known about the molecular mechanism, the radiological findings and the pathology, as well as the complexity of the diagnosis and management of FXTAS.

Published

2019

2. Clinical and Neuropathological Features Associated With Loss of RAB39B

Author

Gao, Y, Martinez-Cerdeno, V, Hogan, KJ, McLean, CA, Lockhart, PJ, Gao, Y, Martinez-Cerdeno, V, Hogan, KJ, McLean, CA, and Lockhart, PJ

Published

2020

3. Patterns of neurogenesis and migration in late rodent cortical development

Author

Kriegstein, A. R., Noctor, S. C., Martinez-Cerdeno, V., and Ivic, L.

Published

2004

4. Pathology and Astrocytes in Autism

Author

Vakilzadeh G and Martinez-Cerdeño V

Subjects

autism, astrocyte, postmortem, gfap, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Gelareh Vakilzadeh,1,2 Veronica Martinez-Cerdeño1– 3 1Department of Pathology and Laboratory Medicine, UC Davis School of Medicine, Sacramento, CA, USA; 2Institute for Pediatric Regenerative Medicine, and Shriners Hospitals for Children, Sacramento, CA, USA; 3MIND Institute, UC Davis School of Medicine, Sacramento, CA, USACorrespondence: Veronica Martinez-Cerdeño, 2425 Stockton Boulevard, Sacramento, CA, 95817, USA, Tel +916 453-2163, Email vmartinezcerdeno@ucdavis.eduAbstract: A distinct pathology for autism spectrum disorder (ASD) remains elusive. Human and animal studies have focused on investigating the role of neurons in ASD. However, recent studies have hinted that glial cell pathology could be a characteristic of ASD. Astrocytes are the most abundant glial cell in the brain and play an important role in neuronal function, both during development and in adult. They regulate neuronal migration, dendritic and spine development, and control the concentration of neurotransmitters at the synaptic cleft. They are also responsible for synaptogenesis, synaptic development, and synaptic function. Therefore, any change in astrocyte number and/or function could contribute to the impairment of connectivity that has been reported in ASD. Data available to date is scarce but indicates that while the number of astrocytes is reduced, their state of activation and their GFAP expression is increased in ASD. Disruption of astrocyte function in ASD may affect proper neurotransmitter metabolism, synaptogenesis, and the state of brain inflammation. Astrocytes alterations are common to ASD and other neurodevelopmental disorders. Future studies about the role of astrocytes in ASD are required to better understand this disorder.Keywords: autism, astrocyte, postmortem, GFAP

Published

2023

5. Translation of Expanded CGG Repeats into FMRpolyG Is Pathogenic and May Contribute to Fragile X Tremor Ataxia Syndrome

Author

Sellier, C, Buijsen, Ronald, He, F, Natla, S, Jung, L, Tropel, P, Gaucherot, A, Jacobs, H, Meziane, H, Vincent, A, Champy, MF, Sorg, T, Pavlovic, G, Wattenhofer-Donze, M, Birling, MC, Oulad-Abdelghani, M, Eberling, P, Ruffenach, F, Joint, M, Anheim, M, Martinez-Cerdeno, V, Tassone, F, Willemsen, Rob, Hukema, Renate, Viville, S, Martinat, C, Todd, PK, Charlet-Berguerand, N, Sellier, C, Buijsen, Ronald, He, F, Natla, S, Jung, L, Tropel, P, Gaucherot, A, Jacobs, H, Meziane, H, Vincent, A, Champy, MF, Sorg, T, Pavlovic, G, Wattenhofer-Donze, M, Birling, MC, Oulad-Abdelghani, M, Eberling, P, Ruffenach, F, Joint, M, Anheim, M, Martinez-Cerdeno, V, Tassone, F, Willemsen, Rob, Hukema, Renate, Viville, S, Martinat, C, Todd, PK, and Charlet-Berguerand, N

Published

2017

6. Rapidly Progressing Neurocognitive Disorder in a Male with FXTAS and Alzheimer’s Disease

Author

Aydin EY, Schneider A, Protic D, Wang JY, Martínez-Cerdeño V, Tassone F, Tang HT, Perlman S, and Hagerman RJ

Subjects

fxtas, alzheimer’s disease, cognitive decline, neurocognitive disorder, premutation, neurogenetics, Geriatrics, RC952-954.6

Abstract

Elber Yuksel Aydin, 1, 2 Andrea Schneider, 1, 3 Dragana Protic, 1, 4 Jun Yi Wang, 1, 5 Veronica Martínez-Cerdeño, 1, 6 Flora Tassone, 1, 7 Hiu-Tung Tang, 7 Susan Perlman, 8 Randi J Hagerman 1, 3 1Medical Investigation of Neurodevelopmental Disorders (MIND) Institute, University of California Davis, Sacramento, CA, USA; 2Istanbul Faculty of Medicine, Istanbul University, Istanbul, Turkey; 3Department of Pediatrics, University of California Davis School of Medicine, Sacramento, CA, USA; 4Department of Pharmacology, Clinical Pharmacology and Toxicology, School of Medicine, University of Belgrade, Belgrade, Serbia; 5Center for Mind and Brain, University of California Davis School of Medicine, Sacramento, CA, USA; 6Department of Pathology and Laboratory Medicine, Institute for Pediatric Regenerative Medicine, University of California Davis School of Medicine and Shriners Hospital, Sacramento, CA, USA; 7Department of Biochemistry and Molecular Medicine, University of California Davis School of Medicine, Sacramento, CA, USA; 8Department of Neurology, University of California Los Angeles School of Medicine, Los Angeles, CA, USACorrespondence: Randi J HagermanMIND Institute UCDMC, 2825 50th Street, Sacramento, CA 95817, USAEmail rjhagerman@ucdavis.eduAbstract: Fragile X–associated tremor/ataxia syndrome (FXTAS) is a neurodegenerative disorder that usually begins in the early 60s and affects carriers of premutation expansion (55– 200 CGG repeats) of the fragile X mental retardation 1 (FMR1) gene. Additional disorders can co-occur with FXTAS including Alzheimer’s disease (AD). Here we discuss a case report of a male with 67 CGG repeats in FMR1 who had mild late-onset FXTAS symptoms followed by neurocognitive disorder symptoms consistent with AD. The patient has developed tremor and ataxia that are the two characteristic symptoms of FXTAS. In addition, he shows rapid cognitive decline, brain atrophy most substantial in the medial temporal lobe, and decreased metabolism in the brain regions that are the characteristic findings of AD. The purpose of this study is to describe a patient profile with both diseases and review the details of an overlap between these two diseases.Keywords: FXTAS, Alzheimer’s disease, cognitive decline, neurocognitive disorder, premutation, neurogenetics

Published

2020

7. Microglia Regulate the Number of Neural Precursor Cells in the Developing Cerebral Cortex

Author

Cunningham, C. L., primary, Martinez-Cerdeno, V., additional, and Noctor, S. C., additional

Published

2013

8. Reelin Immunoreactivity in the Adult Primate Brain: Intracellular Localization in Projecting and Local Circuit Neurons of the Cerebral Cortex, Hippocampus and Subcortical Regions

Author

Martinez-Cerdeno, V., primary

Published

2002

9. Mitochondrial dysfunction in brain tissues and Extracellular Vesicles Fragile X-associated tremor/ataxia syndrome.

Author

Yao PJ, Manolopoulos A, Eren E, Rivera SM, Hessl DR, Hagerman R, Martinez-Cerdeno V, Tassone F, and Kapogiannis D

Subjects

Humans, Male, Aged, Female, Middle Aged, Cerebellum metabolism, Cerebellum pathology, Aged, 80 and over, Brain metabolism, Brain pathology, Frontal Lobe metabolism, Frontal Lobe pathology, Fragile X Syndrome genetics, Fragile X Syndrome metabolism, Fragile X Syndrome pathology, Fragile X Syndrome physiopathology, Tremor genetics, Tremor metabolism, Tremor physiopathology, Tremor pathology, Extracellular Vesicles metabolism, Ataxia genetics, Ataxia metabolism, Ataxia pathology, Ataxia physiopathology, Fragile X Mental Retardation Protein genetics, Fragile X Mental Retardation Protein metabolism, Mitochondria metabolism, Mitochondria pathology

Abstract

Objective: Mitochondrial impairments have been implicated in the pathogenesis of Fragile X-associated tremor/ataxia syndrome (FXTAS) based on analysis of mitochondria in peripheral tissues and cultured cells. We sought to assess whether mitochondrial abnormalities present in postmortem brain tissues of patients with FXTAS are also present in plasma neuron-derived extracellular vesicles (NDEVs) from living carriers of fragile X messenger ribonucleoprotein1 (FMR1) gene premutations at an early asymptomatic stage of the disease continuum., Methods: We utilized postmortem frozen cerebellar and frontal cortex samples from a cohort of eight patients with FXTAS and nine controls and measured the quantity and activity of the mitochondrial proteins complex IV and complex V. In addition, we evaluated the same measures in isolated plasma NDEVs by selective immunoaffinity capture targeting L1CAM from a separate cohort of eight FMR1 premutation carriers and four age-matched controls., Results: Lower complex IV and V quantity and activity were observed in the cerebellum of FXTAS patients compared to controls, without any differences in total mitochondrial content. No patient-control differences were observed in the frontal cortex. In NDEVs, FMR1 premutation carriers compared to controls had lower activity of Complex IV and Complex V, but higher Complex V quantity., Interpretation: Quantitative and functional abnormalities in mitochondrial electron transport chain complexes IV and V seen in the cerebellum of patients with FXTAS are also manifest in plasma NDEVs of FMR1 premutation carriers. Plasma NDEVs may provide further insights into mitochondrial pathologies in this syndrome and could potentially lead to the development of biomarkers for predicting symptomatic FXTAS among premutation carriers and disease monitoring., (© 2024 The Authors. Annals of Clinical and Translational Neurology published by Wiley Periodicals LLC on behalf of American Neurological Association. This article has been contributed to by U.S. Government employees and their work is in the public domain in the USA.)

Published

2024

10. Randomized clinical trial of low dose suramin intravenous infusions for treatment of autism spectrum disorder.

Author

Hough D, Mao AR, Aman M, Lozano R, Smith-Hicks C, Martinez-Cerdeno V, Derby M, Rome Z, Malan N, and Findling RL

Abstract

Background: There is a critical need for effective treatment of the core symptoms of autism spectrum disorder (ASD). The purinergic antagonist suramin may improve core symptoms through restoration of normal mitochondrial function and reduction of neuro-inflammation via its known antagonism of P2X and P2Y receptors. Nonclinical studies in fragile X knockout mice and the maternal immune activation model support these hypotheses., Methods: We conducted a 14 week, randomized, double-blind, placebo-controlled proof -of-concept study (N = 52) to test the efficacy and safety of suramin intravenous infusions in boys aged 4-15 years with moderate to severe ASD. The study had 3 treatment arms: 10 mg/kg suramin, 20 mg/kg suramin, and placebo given at baseline, week 4, and week 8. The Aberrant Behavior Checklist of Core Symptoms (ABC-Core) (subscales 2, 3, and 5) was the primary endpoint and the Clinical Global Impressions-Improvement (CGI-I) was a secondary endpoint., Results: Forty-four subjects completed the study. The 10 mg/kg suramin group showed a greater, but statistically non-significant, numeric improvement (- 12.5 ± 3.18 [mean ± SE]) vs. placebo (- 8.9 ± 2.86) in ABC-Core at Week 14. The 20 mg/kg suramin group did not show improvement over placebo. In exploratory analyses, the 10 mg/kg arm showed greater ABC Core differences from placebo in younger subjects and among those with less severe symptoms. In CGI-I, the 10 mg/kg arm showed a statistically significant improvement from baseline (2.8 ± 0.30 [mean ± SE]) compared to placebo (1.7 ± 0.27) (p = 0.016). The 20 mg/kg arm had a 2.0 ± 0.28 improvement in CGI-I, which was not statistically significant compared to placebo (p = 0.65)., Conclusion: Suramin was generally safe and well tolerated over 14 weeks; most adverse events were mild to moderate in severity. Trial Registration Registered with the South African Health Authority, registration number DOH-27-0419-6116., Clinicaltrials: Gov registration ID is NCT06058962, last update posted 2023-09-28., (© 2023. The Author(s).)

Published

2023

11. Excitatory neuron-specific suppression of the integrated stress response contributes to autism-related phenotypes in fragile X syndrome.

Author

Hooshmandi M, Sharma V, Thörn Perez C, Sood R, Krimbacher K, Wong C, Lister KC, Ureña Guzmán A, Bartley TD, Rocha C, Maussion G, Nadler E, Roque PM, Gantois I, Popic J, Lévesque M, Kaufman RJ, Avoli M, Sanz E, Nader K, Hagerman RJ, Durcan TM, Costa-Mattioli M, Prager-Khoutorsky M, Lacaille JC, Martinez-Cerdeno V, Gibson JR, Huber KM, Sonenberg N, Gkogkas CG, and Khoutorsky A

Subjects

Animals, Mice, Fragile X Mental Retardation Protein genetics, Neurons metabolism, Phenotype, Mice, Knockout, Disease Models, Animal, Fragile X Syndrome genetics, Fragile X Syndrome metabolism, Autistic Disorder, Autism Spectrum Disorder

Abstract

Dysregulation of protein synthesis is one of the key mechanisms underlying autism spectrum disorder (ASD). However, the role of a major pathway controlling protein synthesis, the integrated stress response (ISR), in ASD remains poorly understood. Here, we demonstrate that the main arm of the ISR, eIF2α phosphorylation (p-eIF2α), is suppressed in excitatory, but not inhibitory, neurons in a mouse model of fragile X syndrome (FXS; Fmr1 -/y ). We further show that the decrease in p-eIF2α is mediated via activation of mTORC1. Genetic reduction of p-eIF2α only in excitatory neurons is sufficient to increase general protein synthesis and cause autism-like behavior. In Fmr1 -/y mice, restoration of p-eIF2α solely in excitatory neurons reverses elevated protein synthesis and rescues autism-related phenotypes. Thus, we reveal a previously unknown causal relationship between excitatory neuron-specific translational control via the ISR pathway, general protein synthesis, and core phenotypes reminiscent of autism in a mouse model of FXS., Competing Interests: Declaration of interests M.C.-M. is a member of Neuron’s advisory board and a shareholder of Altos Labs and Mikrovia., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

12. Insight and Recommendations for Fragile X-Premutation-Associated Conditions from the Fifth International Conference on FMR1 Premutation.

Author

Tassone F, Protic D, Allen EG, Archibald AD, Baud A, Brown TW, Budimirovic DB, Cohen J, Dufour B, Eiges R, Elvassore N, Gabis LV, Grudzien SJ, Hall DA, Hessl D, Hogan A, Hunter JE, Jin P, Jiraanont P, Klusek J, Kooy RF, Kraan CM, Laterza C, Lee A, Lipworth K, Losh M, Loesch D, Lozano R, Mailick MR, Manolopoulos A, Martinez-Cerdeno V, McLennan Y, Miller RM, Montanaro FAM, Mosconi MW, Potter SN, Raspa M, Rivera SM, Shelly K, Todd PK, Tutak K, Wang JY, Wheeler A, Winarni TI, Zafarullah M, and Hagerman RJ

Subjects

Humans, Mutation genetics, RNA, Messenger metabolism, Trinucleotide Repeat Expansion genetics, Fragile X Mental Retardation Protein genetics, Fragile X Mental Retardation Protein metabolism, Fragile X Syndrome diagnosis, Fragile X Syndrome genetics, Fragile X Syndrome therapy

Abstract

The premutation of the fragile X messenger ribonucleoprotein 1 ( FMR1 ) gene is characterized by an expansion of the CGG trinucleotide repeats (55 to 200 CGGs) in the 5' untranslated region and increased levels of FMR1 mRNA. Molecular mechanisms leading to fragile X-premutation-associated conditions (FXPAC) include cotranscriptional R-loop formations, FMR1 mRNA toxicity through both RNA gelation into nuclear foci and sequestration of various CGG-repeat-binding proteins, and the repeat-associated non-AUG (RAN)-initiated translation of potentially toxic proteins. Such molecular mechanisms contribute to subsequent consequences, including mitochondrial dysfunction and neuronal death. Clinically, premutation carriers may exhibit a wide range of symptoms and phenotypes. Any of the problems associated with the premutation can appropriately be called FXPAC. Fragile X-associated tremor/ataxia syndrome (FXTAS), fragile X-associated primary ovarian insufficiency (FXPOI), and fragile X-associated neuropsychiatric disorders (FXAND) can fall under FXPAC. Understanding the molecular and clinical aspects of the premutation of the FMR1 gene is crucial for the accurate diagnosis, genetic counseling, and appropriate management of affected individuals and families. This paper summarizes all the known problems associated with the premutation and documents the presentations and discussions that occurred at the International Premutation Conference, which took place in New Zealand in 2023.

Published

2023

13. A Postmortem MRI Study of Cerebrovascular Disease and Iron Content at End-Stage of Fragile X-Associated Tremor/Ataxia Syndrome.

Author

Wang JY, Sonico GJ, Salcedo-Arellano MJ, Hagerman RJ, and Martinez-Cerdeno V

Subjects

Humans, Tremor diagnostic imaging, Tremor pathology, Iron, Ataxia diagnostic imaging, Ataxia pathology, Magnetic Resonance Imaging, Atrophy, Fragile X Syndrome diagnostic imaging, Fragile X Syndrome pathology, Cerebrovascular Disorders

Abstract

Brain changes at the end-stage of fragile X-associated tremor/ataxia syndrome (FXTAS) are largely unknown due to mobility impairment. We conducted a postmortem MRI study of FXTAS to quantify cerebrovascular disease, brain atrophy and iron content, and examined their relationships using principal component analysis (PCA). Intracranial hemorrhage (ICH) was observed in 4/17 FXTAS cases, among which one was confirmed by histologic staining. Compared with seven control brains, FXTAS cases showed higher ratings of T2-hyperintensities (indicating cerebral small vessel disease) in the cerebellum, globus pallidus and frontoparietal white matter, and significant atrophy in the cerebellar white matter, red nucleus and dentate nucleus. PCA of FXTAS cases revealed negative associations of T2-hyperintensity ratings with anatomic volumes and iron content in the white matter, hippocampus and amygdala, that were independent from a highly correlated number of regions with ICH and iron content in subcortical nuclei. Post-hoc analysis confirmed PCA findings and further revealed increased iron content in the white matter, hippocampus and amygdala in FXTAS cases compared to controls, after adjusting for T2-hyperintensity ratings. These findings indicate that both ischemic and hemorrhagic brain damage may occur in FXTAS, with the former being marked by demyelination/iron depletion and atrophy, and the latter by ICH and iron accumulation in basal ganglia.

Published

2023

14. Dysregulated cholesterol metabolism, aberrant excitability and altered cell cycle of astrocytes in fragile X syndrome.

Author

Ren B, Burkovetskaya M, Jung Y, Bergdolt L, Totusek S, Martinez-Cerdeno V, Stauch K, Korade Z, and Dunaevsky A

Subjects

Animals, Humans, Astrocytes metabolism, Proteomics, Fragile X Mental Retardation Protein genetics, Fragile X Mental Retardation Protein metabolism, Cell Cycle, Cholesterol metabolism, Fragile X Syndrome genetics, Fragile X Syndrome metabolism

Abstract

Fragile X syndrome (FXS), the most prevalent heritable form of intellectual disability, is caused by the transcriptional silencing of the FMR1 gene. While neuronal contribution to FXS has been extensively studied in both animal and human-based models of FXS, the roles of astrocytes, a type of glial cells in the brain, are largely unknown. Here, we generated a human-based FXS model via differentiation of astrocytes from human-induced pluripotent stem cells (hiPSCs) and human embryonic stem cells (hESCs) and characterized their development, function, and proteomic profiles. We identified shortened cell cycle, enhanced Ca 2+ signaling, impaired sterol biosynthesis, and pervasive alterations in the proteome of FXS astrocytes. Our work identified astrocytic impairments that could contribute to the pathogenesis of FXS and highlight astrocytes as a novel therapeutic target for FXS treatment., (© 2023 The Authors. GLIA published by Wiley Periodicals LLC.)

Published

2023

15. PARP1-mediated PARylation activity is essential for oligodendroglial differentiation and CNS myelination.

Author

Wang Y, Zhang Y, Zhang S, Kim B, Hull VL, Xu J, Prabhu P, Gregory M, Martinez-Cerdeno V, Zhan X, Deng W, and Guo F

Subjects

Animals, Cell Survival drug effects, Central Nervous System growth & development, Cuprizone pharmacology, Female, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Multiple Sclerosis chemically induced, Multiple Sclerosis metabolism, Multiple Sclerosis pathology, Myelin Sheath genetics, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Oligodendrocyte Precursor Cells cytology, Oligodendrocyte Precursor Cells metabolism, Oligodendrocyte Transcription Factor 2 deficiency, Oligodendrocyte Transcription Factor 2 genetics, Oligodendrocyte Transcription Factor 2 metabolism, Oligodendroglia cytology, Oligodendroglia metabolism, Oligodendroglia physiology, Poly (ADP-Ribose) Polymerase-1 deficiency, Poly (ADP-Ribose) Polymerase-1 genetics, RNA metabolism, Remyelination drug effects, Repressor Proteins genetics, Repressor Proteins metabolism, Cell Differentiation, Central Nervous System metabolism, Myelin Sheath metabolism, Poly (ADP-Ribose) Polymerase-1 metabolism, Poly ADP Ribosylation physiology

Abstract

The function of poly(ADP-ribosyl) polymerase 1 (PARP1) in myelination and remyelination of the central nervous system (CNS) remains enigmatic. Here, we report that PARP1 is an intrinsic driver for oligodendroglial development and myelination. Genetic PARP1 depletion impairs the differentiation of oligodendrocyte progenitor cells (OPCs) into oligodendrocytes and impedes CNS myelination. Mechanistically, PARP1-mediated PARylation activity is not only necessary but also sufficient for OPC differentiation. At the molecular level, we identify the RNA-binding protein Myef2 as a PARylated target, which controls OPC differentiation through the PARylation-modulated derepression of myelin protein expression. Furthermore, PARP1's enzymatic activity is necessary for oligodendrocyte and myelin regeneration after demyelination. Together, our findings suggest that PARP1-mediated PARylation activity may be a potential therapeutic target for promoting OPC differentiation and remyelination in neurological disorders characterized by arrested OPC differentiation and remyelination failure such as multiple sclerosis., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

16. FXTAS presents with upregulation of the cytokines IL12 and TNFα.

Author

Dufour BD, Amina S, and Martinez-Cerdeno V

Subjects

Aged, Aged, 80 and over, Autopsy, Female, Humans, Male, Middle Aged, Up-Regulation, Arachnoiditis metabolism, Ataxia metabolism, Cerebellum metabolism, Fragile X Syndrome metabolism, Interleukin-12 Subunit p35 metabolism, Tremor metabolism, Tumor Necrosis Factor-alpha metabolism

Abstract

Introduction: Fragile X Tremor and Ataxia Syndrome is a progressive neurodegenerative disorder that develops in some FMR1 premutation carriers. The objective of this study is to characterize how cytokine levels are altered in the FXTAS brain., Methods: Fresh frozen cerebellar tissue from FXTAS cases and controls was homogenized and analyzed for 12 different cytokines using a commercially available ELISA panel., Results: Relative to controls, FXTAS cases showed large and significant increases in the cytokines IL-12 and TNFα. There were large but non-significant increases in the levels of IL-2, IL-8, and IL-10 in FXTAS cases. The cytokines IL-1A, IL-1B, IL-4 IL-6, IL-17A, IFNγ, and GM-CSF were not different between FXTAS and control subjects., Conclusions: For the first time, we demonstrate an increase in the pro-inflammatory cytokines TNFα and IL-12 in the FXTAS brain, both of which are implicated in the pathogenesis of Multiple Sclerosis, another neurodegenerative disorder that predominantly consists of white matter disease., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2021

17. Fragile X syndrome and associated disorders: Clinical aspects and pathology.

Author

Salcedo-Arellano MJ, Dufour B, McLennan Y, Martinez-Cerdeno V, and Hagerman R

Subjects

Animals, Ataxia genetics, Ataxia metabolism, Ataxia pathology, Fragile X Mental Retardation Protein metabolism, Fragile X Syndrome metabolism, Humans, Neurodegenerative Diseases genetics, Neurodegenerative Diseases metabolism, Neurodegenerative Diseases pathology, Tremor genetics, Tremor metabolism, Tremor pathology, Fragile X Mental Retardation Protein genetics, Fragile X Syndrome genetics, Fragile X Syndrome pathology

Abstract

This review aims to assemble many years of research and clinical experience in the fields of neurodevelopment and neuroscience to present an up-to-date understanding of the clinical presentation, molecular and brain pathology associated with Fragile X syndrome, a neurodevelopmental condition that develops with the full mutation of the FMR1 gene, located in the q27.3 loci of the X chromosome, and Fragile X-associated tremor/ataxia syndrome a neurodegenerative disease experienced by aging premutation carriers of the FMR1 gene. It is important to understand that these two syndromes have a very distinct clinical and pathological presentation while sharing the same origin: the mutation of the FMR1 gene; revealing the complexity of expansion genetics., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

18. Deficit of corpus callosum axons, reduced axon diameter and decreased area are markers of abnormal development of interhemispheric connections in autistic subjects.

Author

Wegiel J, Kaczmarski W, Flory M, Martinez-Cerdeno V, Wisniewski T, Nowicki K, Kuchna I, and Wegiel J

Subjects

Adolescent, Adult, Axons ultrastructure, Child, Child, Preschool, Cohort Studies, Corpus Callosum ultrastructure, Female, Humans, Male, Microscopy, Electron, Middle Aged, Myelin Sheath metabolism, Myelin Sheath pathology, Myelin Sheath ultrastructure, Young Adult, Autistic Disorder complications, Autistic Disorder pathology, Axons pathology, Corpus Callosum pathology, Developmental Disabilities etiology, Functional Laterality physiology

Abstract

Introduction: In autism spectrum disorder, lack of coherence and of complex information processing, and narrowly focused interests and repetitive behaviors are considered a sign of long-range underconnectivity and short-range overconnectivity. The goal of this morphometric study of five anatomically and functionally different segments of the corpus callosum (CC) was to establish patterns of differences between long-range interhemispheric connections in nine neurotypical and nine autistic subjects., Results: Electron microscopy revealed a significant reduction in average axon diameter and axon cross-sectional area in autistic subjects, and reduction in CC segment-specific diversification of connections of functionally different cortical regions. The study shows an increase in the percentage of small diameter axons (< 0.651 μm) and a decrease in the percentage of axons with large diameter (> 1.051 μm). The total number of small-diameter axons is reduced in segment I and III by 43% on average. The number of medium- and large-diameter axons is reduced in all five CC segments by an average of 49 and 72%, respectively., Conclusions: The detected pattern of pathology suggests a failure of mechanisms controlling guidance of axons during development leading to axonal deficit, and failure of mechanisms controlling axon structure. A reduction in axon diameter may affect the velocity and volume of signal transmission, and distort functional specialization of CC segments. Significant deficits in axon number and reduction in axon size in all five CC segments appear to be substantial components of brain connectome integrity distortion which may contribute to the autism phenotype.

Published

2018

19. The role of reduced expression of fragile X mental retardation protein in neurons and increased expression in astrocytes in idiopathic and syndromic autism (duplications 15q11.2-q13).

Author

Wegiel J, Brown WT, La Fauci G, Adayev T, Kascsak R, Kascsak R, Flory M, Kaczmarski W, Kuchna I, Nowicki K, Martinez-Cerdeno V, Wisniewski T, and Wegiel J

Subjects

Adolescent, Adult, Animals, Brain metabolism, Cerebral Cortex pathology, Child, Child, Preschool, Female, Humans, Immunohistochemistry, Male, Middle Aged, Young Adult, Astrocytes metabolism, Autistic Disorder genetics, Autistic Disorder metabolism, Fragile X Mental Retardation Protein genetics, Fragile X Mental Retardation Protein metabolism, Neurons metabolism

Abstract

Fragile X syndrome (FXS), caused by lack of fragile X mental retardation protein (FMRP), is associated with a high prevalence of autism. The deficit of FMRP reported in idiopathic autism suggests a mechanistic overlap between FXS and autism. The overall goal of this study is to detect neuropathological commonalities of FMRP deficits in the brains of people with idiopathic autism and with syndromic autism caused by dup15q11.2-q13 (dup15). This study tests the hypothesis based on our preliminary data that both idiopathic and syndromic autism are associated with brain region-specific deficits of neuronal FMRP and structural changes of the affected neurons. This immunocytochemical study revealed neuronal FMRP deficits and shrinkage of deficient neurons in the cerebral cortex, subcortical structures, and cerebellum in subjects with idiopathic and dup(15)/autism. Neuronal FMRP deficit coexists with surprising infiltration of the brains of autistic children and adults with FMRP-positive astrocytes known to be typical only for the fetal and short postnatal periods. In the examined autistic subjects, these astrocytes selectively infiltrate the border between white and gray matter in the cerebral and cerebellar cortex, the molecular layer of the cortex, part of the amygdala and thalamus, central cerebellar white matter, and dentate nucleus. Astrocyte pathology results in an additional local loss of FMRP in neurons and their shrinkage. Neuronal deficit of FMRP and shrinkage of affected neurons in structures free of FMRP-positive astrocytes and regions infiltrated with FMRP-expressing astrocytes appear to reflect mechanistic, neuropathological, and functional commonalities of FMRP abnormalities in FXS and autism spectrum disorder. Autism Res 2018, 11: 1316-1331. © 2018 International Society for Autism Research, Wiley Periodicals, Inc. LAY SUMMARY: Immunocytochemistry reveals a deficit of fragile X mental retardation protein (FMRP) in neurons of cortical and subcortical brain structures but increased FMRP expression in astrocytes infiltrating gray and white matter. The detected shrinkage of FMRP-deficient neurons may provide a mechanistic explanation of reported neuronal structural and functional changes in autism. This study contributes to growing evidence of mechanistic commonalities between fragile X syndrome and autism spectrum disorder., (© 2018 International Society for Autism Research, Wiley Periodicals, Inc.)

Published

2018

20. Presence of Middle Cerebellar Peduncle Sign in FMR1 Premutation Carriers Without Tremor and Ataxia.

Author

Famula JL, McKenzie F, McLennan YA, Grigsby J, Tassone F, Hessl D, Rivera SM, Martinez-Cerdeno V, and Hagerman RJ

Abstract

Here we report five cases of male FMR1 premutation carriers who present without clinical symptoms of the fragile X-associated tremor/ataxia syndrome (FXTAS), but who on MRI demonstrate white matter hyperintensities in the middle cerebellar peduncles (MCP sign) and other brain regions, a rare finding. MCP sign is the major radiological feature of FXTAS; it is therefore remarkable to identify five cases in which this MRI finding is present in the absence of tremor and ataxia, the major clinical features of FXTAS. Subjects underwent a detailed neurological evaluation, neuropsychological testing, molecular testing, and MRI evaluation utilizing T2 imaging described here. Additional white matter disease was present in the corpus callosum in four of the five cases. However, all cases were asymptomatic for motor signs of FXTAS.

Published

2018

21. Translation of Expanded CGG Repeats into FMRpolyG Is Pathogenic and May Contribute to Fragile X Tremor Ataxia Syndrome.

Author

Sellier C, Buijsen RAM, He F, Natla S, Jung L, Tropel P, Gaucherot A, Jacobs H, Meziane H, Vincent A, Champy MF, Sorg T, Pavlovic G, Wattenhofer-Donze M, Birling MC, Oulad-Abdelghani M, Eberling P, Ruffenach F, Joint M, Anheim M, Martinez-Cerdeno V, Tassone F, Willemsen R, Hukema RK, Viville S, Martinat C, Todd PK, and Charlet-Berguerand N

Subjects

Animals, Ataxia metabolism, Brain metabolism, Brain pathology, Fragile X Mental Retardation Protein metabolism, Fragile X Syndrome metabolism, Humans, Male, Mice, Mice, Transgenic, Nuclear Lamina pathology, Peptides metabolism, Real-Time Polymerase Chain Reaction, Tremor metabolism, Ataxia genetics, DNA-Binding Proteins metabolism, Fragile X Mental Retardation Protein genetics, Fragile X Syndrome genetics, Membrane Proteins metabolism, Nuclear Lamina metabolism, Peptides genetics, Protein Biosynthesis, RNA, Messenger metabolism, Tremor genetics, Trinucleotide Repeat Expansion genetics

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is a neurodegenerative disorder caused by a limited expansion of CGG repeats in the 5' UTR of FMR1. Two mechanisms are proposed to cause FXTAS: RNA gain-of-function, where CGG RNA sequesters specific proteins, and translation of CGG repeats into a polyglycine-containing protein, FMRpolyG. Here we developed transgenic mice expressing CGG repeat RNA with or without FMRpolyG. Expression of FMRpolyG is pathogenic, while the sole expression of CGG RNA is not. FMRpolyG interacts with the nuclear lamina protein LAP2β and disorganizes the nuclear lamina architecture in neurons differentiated from FXTAS iPS cells. Finally, expression of LAP2β rescues neuronal death induced by FMRpolyG. Overall, these results suggest that translation of expanded CGG repeats into FMRpolyG alters nuclear lamina architecture and drives pathogenesis in FXTAS., (Copyright © 2017 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2017

22. Augmented noncanonical BMP type II receptor signaling mediates the synaptic abnormality of fragile X syndrome.

Author

Kashima R, Roy S, Ascano M, Martinez-Cerdeno V, Ariza-Torres J, Kim S, Louie J, Lu Y, Leyton P, Bloch KD, Kornberg TB, Hagerman PJ, Hagerman R, Lagna G, and Hata A

Subjects

Animals, Autistic Disorder genetics, Brain metabolism, Cofilin 1 metabolism, Crosses, Genetic, Drosophila melanogaster, Fragile X Syndrome metabolism, Gene Expression Regulation, HEK293 Cells, Heterozygote, Humans, Lim Kinases metabolism, Mice, Mice, Knockout, Neurites metabolism, Neurons metabolism, Phosphorylation, Plasmids metabolism, Prefrontal Cortex metabolism, Protein Domains, RNA, Small Interfering metabolism, Signal Transduction, Bone Morphogenetic Protein Receptors, Type II metabolism, Fragile X Syndrome genetics

Abstract

Epigenetic silencing of fragile X mental retardation 1 (FMR1) causes fragile X syndrome (FXS), a common inherited form of intellectual disability and autism. FXS correlates with abnormal synapse and dendritic spine development, but the molecular link between the absence of the FMR1 product FMRP, an RNA binding protein, and the neuropathology is unclear. We found that the messenger RNA encoding bone morphogenetic protein type II receptor (BMPR2) is a target of FMRP. Depletion of FMRP increased BMPR2 abundance, especially that of the full-length isoform that bound and activated LIM domain kinase 1 (LIMK1), a component of the noncanonical BMP signal transduction pathway that stimulates actin reorganization to promote neurite outgrowth and synapse formation. Heterozygosity for BMPR2 rescued the morphological abnormalities in neurons both in Drosophila and in mouse models of FXS, as did the postnatal pharmacological inhibition of LIMK1 activity. Compared with postmortem prefrontal cortex tissue from healthy subjects, the amount of full-length BMPR2 and of a marker of LIMK1 activity was increased in this brain region from FXS patients. These findings suggest that increased BMPR2 signal transduction is linked to FXS and that the BMPR2-LIMK1 pathway is a putative therapeutic target in patients with FXS and possibly other forms of autism., (Copyright © 2016, American Association for the Advancement of Science.)

Published

2016

23. Advances in the Understanding of the Gabaergic Neurobiology of FMR1 Expanded Alleles Leading to Targeted Treatments for Fragile X Spectrum Disorder.

Author

Lozano R, Martinez-Cerdeno V, and Hagerman RJ

Subjects

Alleles, Animals, Clinical Trials as Topic methods, Drug Design, Fragile X Mental Retardation Protein genetics, Fragile X Syndrome genetics, Fragile X Syndrome physiopathology, GABA Agonists pharmacology, Humans, Molecular Targeted Therapy, Fragile X Syndrome drug therapy, GABA Agonists therapeutic use, gamma-Aminobutyric Acid metabolism

Abstract

Fragile X spectrum disorder (FXSD) includes: fragile X syndrome (FXS), fragile X-associated tremor ataxia syndrome (FXTAS) and fragile X-associated primary ovarian insufficiency (FXPOI), as well as other medical, psychiatric and neurobehavioral problems associated with the premutation and gray zone alleles. FXS is the most common monogenetic cause of autism (ASD) and intellectual disability (ID). The understanding of the neurobiology of FXS has led to many targeted treatment trials in FXS. The first wave of phase II clinical trials in FXS were designed to target the mGluR5 pathway; however the results did not show significant efficacy and the trials were terminated. The advances in the understanding of the GABA system in FXS have shifted the focus of treatment trials to GABA agonists, and a new wave of promising clinical trials is under way. Ganaxolone and allopregnanolone (GABA agonists) have been studied in individuals with FXSD and are currently in phase II trials. Both allopregnanolone and ganaxolone may be efficacious in treatment of FXS and FXTAS, respectively. Allopregnanolone, ganaxolone, riluzole, gaboxadol, tiagabine, and vigabatrin are potential GABAergic treatments. The lessons learned from the initial trials have not only shifted the targeted system, but also have refined the design of clinical trials. The results of these new trials will likely impact further clinical trials for FXS and other genetic disorders associated with ASD.

Published

2015

24. c- and N-myc regulate neural precursor cell fate, cell cycle, and metabolism to direct cerebellar development.

Author

Wey A, Martinez Cerdeno V, Pleasure D, and Knoepfler PS

Subjects

2',3'-Cyclic-Nucleotide Phosphodiesterases metabolism, Age Factors, Animals, Animals, Newborn, Basic Helix-Loop-Helix Transcription Factors metabolism, Brain cytology, Brain growth & development, Brain metabolism, Bromodeoxyuridine metabolism, Embryo, Mammalian, Glutamate Decarboxylase metabolism, Intermediate Filament Proteins genetics, Mice, Mice, Knockout, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Nestin, Proto-Oncogene Proteins c-myc deficiency, Tubulin metabolism, Cell Cycle physiology, Cerebellum cytology, Cerebellum growth & development, Cerebellum metabolism, Gene Expression Regulation, Developmental genetics, Neural Stem Cells physiology, Proto-Oncogene Proteins c-myc metabolism

Abstract

Separate murine knockout (KO) of either c- or N-myc genes in neural stem and precursor cells (NSC) driven by nestin-cre causes microcephaly. The cerebellum is particularly affected in the N-myc KO, leading to a strong reduction in cerebellar granule neural progenitors (CGNP) and mature granule neurons. In humans, mutation of N-myc also causes microcephaly in Feingold Syndrome. We created a double KO (DKO) of c- and N-myc using nestin-cre, which strongly impairs brain growth, particularly that of the cerebellum. Granule neurons were almost absent from the Myc DKO cerebellum, and other cell types were relatively overrepresented, including astroglia, oligodendrocytes, and Purkinje neurons. These findings are indicative of a profound disruption of cell fate of cerebellar stem and precursors. DKO Purkinje neurons were strikingly lacking in normal arborization. Inhibitory neurons were ectopic and exhibited very abnormal GAD67 staining patterns. Also consistent with altered cell fate, the adult DKO cerebellum still retained a residual external germinal layer (EGL). CGNP in the DKO EGL were almost uniformly NeuN and p27KIP1 positive as well as negative for Math1 and BrdU at the peak of normal cerebellar proliferation at P6. The presence of some mitotic CGNP in the absence of S phase cells suggests a possible arrest in M phase. CGNP and NSC metabolism also was affected by loss of Myc as DKO cells exhibited weak nucleolin staining. Together these findings indicate that c- and N-Myc direct cerebellar development by maintaining CGNP and NSC populations through inhibiting differentiation as well as directing rapid cell cycling and active cellular metabolism.

Published

2010

25. Progenitors from the postnatal forebrain subventricular zone differentiate into cerebellar-like interneurons and cerebellar-specific astrocytes upon transplantation.

Author

Milosevic A, Noctor SC, Martinez-Cerdeno V, Kriegstein AR, and Goldman JE

Subjects

Animals, Astrocytes cytology, Biomarkers metabolism, Cell Membrane metabolism, Cerebellum metabolism, Electrophysiology, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, Interneurons cytology, Patch-Clamp Techniques, Rats, Rats, Sprague-Dawley, Stem Cells cytology, Astrocytes metabolism, Brain Tissue Transplantation, Cell Differentiation physiology, Cerebellum cytology, Interneurons metabolism, Prosencephalon cytology, Prosencephalon growth & development, Stem Cell Transplantation, Stem Cells physiology

Abstract

Forebrain subventricular zone (SVZ) progenitor cells give rise to glia and olfactory bulb interneurons during early postnatal life in rats. We investigated the potential of SVZ cells to alter their fate by transplanting them into a heterotypic neurogenic and gliogenic environment-the cerebellum. Transplanted cells were examined 1 to 7 weeks and 6 months post transplantation. Forebrain progenitors populated the cerebellum and differentiated into oligodendrocytes, cerebellar-specific Bergmann glia and velate astrocytes, and neurons. The transplanted cells that differentiated into neurons maintained an interneuronal fate: they were GABA-positive, expressed interneuronal markers, such as calretinin, and exhibited membrane properties that are characteristic of interneurons. However, the transplanted interneurons lost the expression of the olfactory bulb transcription factors Tbr2 and Dlx1, and acquired a cerebellar-like morphology. Forebrain SVZ progenitors thus have the potential to adapt to a new environment and integrate into diverse regions, and may be a useful tool in transplantation strategies.

Published

2008