Your search keyword '"CGG repeat"' showing total 299 results

1. A case report of oculopharyngodistal myopathy with 126 CGG repeat expansions in RILPL1

Author

Wenjing Wang, Tielun Yin, Xinyu Zhang, Zhaoxia Wang, Tianyun Wang, Shuo Zhang, Yingshuang Zhang, and Dongsheng Fan

Subjects

oculopharyngodistal myopathy, RILPL1, CGG repeat, OPDM4, myopathy, Genetics, QH426-470

Abstract

BackgroundOculopharyngodistal myopathy (OPDM) is a rare hereditary muscle disease characterized by progressive ptosis, ophthalmoplegia, dysphagia, dysarthria, and distal muscle weakness. The genetic basis was identified in 2019 with CGG repeat expansions in the noncoding region of LRP12. Similar expansions in GIPC1, NOTCH2NLC, and RILPL1 were later linked to OPDM, classifying the disease into OPDM1-4. OPDM4, associated with RILPL1, was discovered in 2022 with a few confirmed cases worldwide, leaving its clinical features and pathogenic mechanisms largely unexplored.Case presentationWe present a patient with OPDM4 who had suffered progressive ptosis, external ophthalmoplegia, pharyngeal weakness, facial muscle weakness, and distal limb weakness over the past 20 years. Electromyography (EMG) revealed myogenic damage and normal H-reflex latency. A biopsy of the left biceps brachii revealed myogenic changes with atypical rimmed vacuoles in some muscle fibers. Screening for extra-muscular system involvement revealed no obvious involvement of the heart or central nervous system. Genetic analysis confirmed 126 CGG repeat expansions in RILPL1 and excluded abnormal CGG repeat expansions in LRP12, GIPC1, and NOTCH2NLC.ConclusionThis case broadens the spectrum of CGG repeat numbers in the RILPL1 gene associated with OPDM4. In addition, systematic medical examinations revealed several new characteristics of OPDM4, which have not been reported previously, such as normal H reflex, potential mild cognitive impairment, etc. These findings expand our knowledge of the phenotypic spectrum of diseases caused by repeat CGG expansions in RILPL1.

Published

2025

2. Differential Progression of Motor Dysfunction Between Male and Female Fragile X Premutation Carriers Reveals Novel Aspects of Sex-Specific Neural Involvement

Author

Loesch, Danuta Z, Tassone, Flora, Atkinson, Anna, Stimpson, Paige, Trost, Nicholas, Pountney, Dean L, and Storey, Elsdon

Subjects

Medical Biochemistry and Metabolomics, Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Mental Health, Genetics, Pediatric, Rare Diseases, Fragile X Syndrome, Clinical Research, Behavioral and Social Science, Intellectual and Developmental Disabilities (IDD), Brain Disorders, Neurosciences, Neurodegenerative, Mental health, Neurological, FMR1 premutation, CGG repeat, female carriers, motor scores, progression rates, gender differences, Biochemistry and cell biology, Medical biochemistry and metabolomics

Abstract

Expansions of the CGG repeat in the non-coding segment of the FMR1 X-linked gene are associated with a variety of phenotypic changes. Large expansions (>200 repeats), which cause a severe neurodevelopmental disorder, the fragile x syndrome (FXS), are transmitted from the mothers carrying smaller, unstable expansions ranging from 55 to 200 repeats, termed the fragile X premutation. Female carriers of this premutation may themselves experience a wide range of clinical problems throughout their lifespan, the most severe being the late onset neurodegenerative condition called "Fragile X-Associated Tremor Ataxia Syndrome" (FXTAS), occurring between 8 and 16% of these carriers. Male premutation carriers, although they do not transmit expanded alleles to their daughters, have a much higher risk (40-50%) of developing FXTAS. Although this disorder is more prevalent and severe in male than female carriers, specific sex differences in clinical manifestations and progress of the FXTAS spectrum have been poorly documented. Here we compare the pattern and rate of progression (per year) in three motor scales including tremor/ataxia (ICARS), tremor (Clinical Tremor Rating scale, CRST), and parkinsonism (UPDRS), and in several cognitive and psychiatric tests scores, between 13 female and 9 male carriers initially having at least one of the motor scores ≥10. Moreover, we document the differences in each of the clinical and cognitive measures between the cross-sectional samples of 21 female and 24 male premutation carriers of comparable ages with FXTAS spectrum disorder (FSD), that is, who manifest one or more features of FXTAS. The results of progression assessment showed that it was more than twice the rate in male than in female carriers for the ICARS-both gait ataxia and kinetic tremor domains and twice as high in males on the CRST scale. In contrast, sex difference was negligible for the rate of progress in UPDRS, and all the cognitive measures. The overall psychiatric pathology score (SCL-90), as well as Anxiety and Obsessive/Compulsive domain scores, showed a significant increase only in the female sample. The pattern of sex differences for progression in motor scores was consistent with the results of comparison between larger, cross-sectional samples of male and female carriers affected with the FSD. These results were in concert with sex-specific distribution of MRI T2 white matter hyperintensities: all males, but no females, showed the middle cerebellar peduncle white matter hyperintensities (MCP sign), although the distribution and severity of these hyperintensities in the other brain regions were not dissimilar between the two sexes. In conclusion, the magnitude and specific pattern of sex differences in manifestations and progression of clinically recorded changes in motor performance and MRI lesion distribution support, on clinical grounds, the possibility of certain sex-limited factor(s) which, beyond the predictable effect of the second, normal FMR1 alleles in female premutation carriers, may have neuroprotective effects, specifically concerning the cerebellar circuitry.

Published

2021

3. Evaluation of the role of FMR1 CGG repeat allele in Parkinson's disease from the Chinese population.

Author

Juan Chen, Yuwen Zhao, Xun Zhou, Jin Xue, Qiao Xiao, Hongxu Pan, Xiaoxia Zhou, Yaqin Xiang, Jian Li, Liping Zhu, Zhou Zhou, Yang Yang, Qian Xu, Qiying Sun, Xinxiang Yan, Jieqiong Tan, Jinchen Li, Jifeng Guo, Ranhui Duan, and Beisha Tang

Subjects

PARKINSON'S disease & genetics, GENETIC mutation, ALLELES, GENETIC testing, RISK assessment, COMPARATIVE studies, PARKINSON'S disease, DESCRIPTIVE statistics, POLYMERASE chain reaction, LONGITUDINAL method, EPIGENOMICS, DISEASE risk factors

Abstract

Objective: There is controversial evidence that FMR1 premutation or "gray zone" (GZ) allele (small CGG expansion, 45-54 repeats) was associated with Parkinson's disease (PD). We aimed to explore further the association between FMR1 CGG repeat expansions and PD in a large sample of Chinese origin. Methods: We included a cohort of 2,362 PD patients and 1,072 controls from the Parkinson's Disease and Movement Disorders Multicenter Database and Collaborative Network in China (PD-MDCNC) in this study and conducted repeat-primed polymerase chain reaction (RP-PCR) for the size of FMR1 CGG repeat expansions. Results: Two PD patients were detected with FMR1 premutation (61 and 56 repeats), and the other eleven PD patients were detected with the GZ allele of FMR1 CGG repeat expansions. Those thirteen PD patients responded well to levodopa and were diagnosed with clinically established PD. Specifically, one female PD patient with GZ allele was also found with premature ovarian failure. However, compared to healthy controls, we found no significant enrichment of GZ allele carriers in PD patients or other subgroups of PD cases, including the subgroups of female, male, early-onset, and late-onset PD patients. Furthermore, we did not find any correlation between the FMR1 gene CGG repeat sizes and age at onset of PD. Conclusion: It suggested that FMR1 premutation was related to PD, but the GZ allele of FMR1 CGG repeat expansions was not significantly enriched in PD cases of Chinese origin. Further larger multiple ethnic studies are needed to determine further the role of the FMR1 GZ allele in PD. [ABSTRACT FROM AUTHOR]

Published

2023

4. Composition of the Intranuclear Inclusions of Fragile X-associated Tremor/Ataxia Syndrome

Author

Ma, Lisa, Herren, Anthony W, Espinal, Glenda, Randol, Jamie, McLaughlin, Bridget, Martinez-Cerdeño, Veronica, Pessah, Isaac N, Hagerman, Randi J, and Hagerman, Paul J

Subjects

Fragile X Syndrome, Brain Disorders, Genetics, Intellectual and Developmental Disabilities (IDD), Neurosciences, Rare Diseases, Neurodegenerative, 2.1 Biological and endogenous factors, Neurological, Amino Acid Sequence, Ataxia, Female, Flow Cytometry, Frontal Lobe, Humans, Intranuclear Inclusion Bodies, Male, Proteomics, Tremor, Fragile X, neurodegeneration, proteomics, CGG repeat, proteasome, inclusion, FXTAS, FMRpolyG, SUMO, ubiquitin, Biochemistry and Cell Biology, Clinical Sciences, Biochemistry and cell biology

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is a neurodegenerative disorder associated with a premutation repeat expansion (55-200 CGG repeats) in the 5' noncoding region of the FMR1 gene. Solitary intranuclear inclusions within FXTAS neurons and astrocytes constitute a hallmark of the disorder, yet our understanding of how and why these bodies form is limited. Here, we have discovered that FXTAS inclusions emit a distinct autofluorescence spectrum, which forms the basis of a novel, unbiased method for isolating FXTAS inclusions by preparative fluorescence-activated cell sorting (FACS). Using a combination of autofluorescence-based FACS and liquid chromatography/tandem mass spectrometry (LC-MS/MS)-based proteomics, we have identified more than two hundred proteins that are enriched within the inclusions relative to FXTAS whole nuclei. Whereas no single protein species dominates inclusion composition, highly enriched levels of conjugated small ubiquitin-related modifier 2 (SUMO 2) protein and p62/sequestosome-1 (p62/SQSTM1) protein were found within the inclusions. Many additional proteins involved with RNA binding, protein turnover, and DNA damage repair were enriched within inclusions relative to total nuclear protein. The current analysis has also allowed the first direct detection, through peptide sequencing, of endogenous FMRpolyG peptide, the product of repeat-associated non-ATG (RAN) translation of the FMR1 mRNA. However, this peptide was found only at extremely low levels and not within whole FXTAS nuclear preparations, raising the question whether endogenous RAN products exist at quantities sufficient to contribute to FXTAS pathogenesis. The abundance of the inclusion-associated ubiquitin- and SUMO-based modifiers supports a model for inclusion formation as the result of increased protein loads and elevated oxidative stress leading to maladaptive autophagy. These results highlight the need to further investigate FXTAS pathogenesis in the context of endogenous systems.

Published

2019

5. Recent progress in oculopharyngodistal myopathy research from clinical and genetic viewpoints.

Author

Ishiura H

Abstract

Oculopharyngodistal myopathy (OPDM) is a rare muscular disorder characterized by ocular symptoms, pharyngeal symptoms, facial weakness, and distal predominant limb muscle weakness. The cause of the disease was unknown for a long time. Recently, however, it has been reported that expansions of CGG or CCG repeats in LRP12 , LOC642361 / NUTM2B-AS1 , GIPC1 , NOTCH2NLC , RILPL1 , and ABCD3 are the causes of the disease. Cases sometimes present with neurological symptoms, and the clinical spectrum of diseases caused by expansions of CGG or CCG repeats has been proposed to be called FNOP-spectrum disorder after the names of fragile X-associated tremor/ataxia syndrome, neuronal intranuclear inclusion disease, oculopharyngeal myopathy with leukoencephalopathy, and OPDM. In this article, the recent progress in the field of OPDM is reviewed, and remaining issues in OPDM are discussed., Competing Interests: Declaration of conflicting interestsThe author declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published

2025

6. Mechanisms of the FMR1 Repeat Instability: How Does the CGG Sequence Expand?

Author

Tabolacci, Elisabetta, Nobile, Veronica, Pucci, Cecilia, and Chiurazzi, Pietro

Subjects

*FRAGILE X syndrome, *DNA structure, *HUNTINGTIN protein

Abstract

A dynamic mutation in exon 1 of the FMR1 gene causes Fragile X-related Disorders (FXDs), due to the expansion of an unstable CGG repeat sequence. Based on the CGG sequence size, two types of FMR1 alleles are possible: "premutation" (PM, with 56-200 CGGs) and "full mutation" (FM, with >200 triplets). Premutated females are at risk of transmitting a FM allele that, when methylated, epigenetically silences FMR1 and causes Fragile X syndrome (FXS), a very common form of inherited intellectual disability (ID). Expansions events of the CGG sequence are predominant over contractions and are responsible for meiotic and mitotic instability. The CGG repeat usually includes one or more AGG interspersed triplets that influence allele stability and the risk of transmitting FM to children through maternal meiosis. A unique mechanism responsible for repeat instability has not been identified, but several processes are under investigations using cellular and animal models. The formation of unusual secondary DNA structures at the expanded repeats are likely to occur and contribute to the CGG expansion. This review will focus on the current knowledge about CGG repeat instability addressing the CGG sequence expands. [ABSTRACT FROM AUTHOR]

Published

2022

7. Refining reproductive risk for FMR1 premutation carriers in the general obstetric population.

Author

Owens, Kailey M., Terhaar, Catherine, Zdrodowski, Jamie, Johnson, Lisa R., and Eveleigh, Deepa

Abstract

Female FMR1 premutation (FMR1 PM) carriers for fragile X syndrome (FXS) are at risk to have a child with FXS based on their CGG repeat size and AGG interruption number. Studies examining this risk in unselected populations of female PM carriers are lacking. This retrospective cohort study analyzed carrier status, CGG repeat length, AGG interruption result, and reproductive risk refinement in a population of female patients who underwent routine carrier screening for FXS. A total of 1536 PM carriers (0.43%) were identified, 95% of whom had between 55 and 90 CGG repeats. A number of 1334 carriers underwent AGG interruption testing. The majority had at least one AGG interruption and received a lower reproductive risk for FXS following AGG interruption testing (89% and 85%, respectively) as compared to their risk calculated based on CGG repeat size alone. The average change in risk across the population following AGG interruption testing was −3.4%, with a range from −50.8% to 48.9%. This article describes the range of CGG repeats and AGG interruptions in an unselected population of female PM carriers and suggests that most carriers would benefit from AGG interruption testing to refine their reproductive risk of having a child with FXS. [ABSTRACT FROM AUTHOR]

Published

2022

8. Evaluation of FMR4, FMR5 and FMR6 Expression Levels as Non-Invasive Biomarkers for the Diagnosis of Fragile X-Associated Primary Ovarian Insufficiency (FXPOI).

Author

Alvarez-Mora, Maria Isabel, Agusti, Ines, Wijngaard, Robin, Martinez-Barrios, Estefania, Barcos, Tamara, Borras, Aina, Peralta, Sara, Guimera, Marta, Goday, Ana, Manau, Dolors, and Rodriguez-Revenga, Laia

Subjects

*AMENORRHEA, *LINCRNA, *RECEIVER operating characteristic curves, *BIOMARKERS, *INTELLECTUAL disabilities, *DIAGNOSIS

Abstract

Female FMR1 (Fragile X mental retardation 1) premutation carriers are at risk for developing fragile X-associated primary ovarian insufficiency (FXPOI), a condition characterized by amenorrhea before age 40 years. Not all women with a FMR1 premutation suffer from primary ovarian insufficiency and nowadays there are no molecular or other biomarkers that can help predict the occurrence of FXPOI. Long non-coding RNAs (lncRNAs) comprise a group of regulatory transcripts which have versatile molecular functions, making them important regulators in all aspects of gene expression. In recent medical studies, lncRNAs have been described as potential diagnostic biomarkers in many diseases. The present study was designed to determine the expression profile of three lncRNAs derived from the FMR1 locus, FMR4, FMR5 and FMR6, in female FMR1 premutation carriers in order: (i) to determine a possible role in the pathogenesis of FXPOI and (ii) to investigate whether they could serve as a biomarker for the diagnosis of FXPOI. FMR4, FMR5 and FMR6 transcripts levels were evaluated in total RNA extracted from peripheral blood by digital droplet PCR and compared between FMR1 premutation carriers with FXPOI and without FXPOI. The diagnostic value of lncRNAs was evaluated by receiver operating characteristic (ROC) analysis. Results revealed a significant association between FXPOI and high expression levels of FMR4. No association was obtained for FMR5 or FMR6. ROC curve analysis revealed that FMR4 can distinguish FMR1 premutation carrier with FXPOI with a diagnostic power of 0.67. These findings suggest a potential role of FMR4 as a possible biomarker for FXPOI. [ABSTRACT FROM AUTHOR]

Published

2022

9. Enhancing Binding Affinity to CGG/CGG Triad: Optimizing Naphthyridine Carbamate Dimer Derivatives with Varied Linker Lengths.

Author

Shibata T, Nakamachi A, and Nakatani K

Subjects

Humans, Molecular Structure, DNA chemistry, DNA metabolism, Binding Sites, Trinucleotide Repeats, Ligands, Naphthyridines chemistry, Naphthyridines pharmacology, Naphthyridines chemical synthesis, Carbamates chemistry, Carbamates pharmacology, Dimerization

Abstract

This study examines the binding properties of six naphthyridine carbamate dimer (NCD) derivatives with varying linker lengths to the CGG/CGG triad, a non-canonical DNA structure linked to repeat expansion disorders. By altering the linker length from 2 to 4 methylene groups, we found changes in thermal stability of the ligand-bound complexes while maintaining a consistent 2 : 1 binding stoichiometry. Among the derivatives, CC23 showed superior binding affinity compared to the parent molecule CC33 (NCD). Spectroscopic analyses revealed that linker length influences the conformational equilibrium of NCD derivatives. Thermal melting temperature measurements demonstrated CC23's enhanced thermal stability over CC33. These findings underscore the potential of optimized NCD derivatives, like CC23, as tools to modulate CGG repeat structures, offering insights for therapeutic strategies targeting repeat expansion disorders., (© 2024 The Author(s). ChemMedChem published by Wiley-VCH GmbH.)

Published

2024

10. Fragile X Syndrome: Lessons Learned and What New Treatment Avenues Are on the Horizon.

Author

Hagerman, Randi J. and Hagerman, Paul J.

Subjects

*NERVE tissue proteins, *GENETIC mutation, *RNA-binding proteins, *NEUROTRANSMITTERS, *FRAGILE X syndrome, *DRUGS, *CHILD psychopathology, *MEDICAL research, *DISEASE complications

Abstract

Fragile X syndrome (FXS) is the most common form of inherited intellectual disability and the leading single-gene form of autism spectrum disorder, encompassing cognitive, behavioral, and physical forms of clinical involvement. FXS is caused by large expansions of a noncoding CGG repeat (>200 repeats) in the FMR1 gene, at which point the gene is generally silenced. Absence of FMR1 protein (FMRP), important for synaptic development and maintenance, gives rise to the neurodevelopmental disorder. There is, at present, no therapeutic approach that directly reverses the loss of FMRP; however, there is an increasing number of potential treatments that target the pathways dysregulated in FXS, including those that address the enhanced activity of the mGluR5 pathway and deficits in GABA pathways. Based on studies of targeted therapeutics to date, the prospects are good for one or more effective therapies for FXS in the near future. [ABSTRACT FROM AUTHOR]

Published

2022

11. Advanced technologies for the molecular diagnosis of fragile X syndrome

Author

Tassone, Flora

Subjects

Genetics, Brain Disorders, Behavioral and Social Science, Fragile X Syndrome, Intellectual and Developmental Disabilities (IDD), Rare Diseases, Genetic Testing, Pediatric, Alleles, DNA Methylation, Fragile X Mental Retardation Protein, Humans, Mass Screening, Molecular Diagnostic Techniques, Mutation, Prevalence, Trinucleotide Repeat Expansion, AGG interruption, CGG repeat, FXS, methylation, premutation, Southern Blot, triplet-primed PCR, Clinical Sciences

Abstract

Fragile X syndrome (FXS), a trinucleotide repeat disorder, is the most common heritable form of cognitive impairment. Since the discovery of the FMR1 gene in 1991, great strides have been made in the field of molecular diagnosis for FXS. Cytogenetic analysis, which was the method of diagnosis in the early 1990, was replaced by Southern blot and PCR analysis albeit with some limitations. In the past few years many PCR-based methodologies, able to amplify large full mutation expanded alleles, with or without methylation, have been proposed. Reviewed here are the advantages, disadvantages and limitations of the most recent developments in the field of FXS diagnosis.

Published

2015

12. Fragile X–associated tremor/ataxia syndrome

Author

Hagerman, Paul J and Hagerman, Randi J

Subjects

Biological Psychology, Biological Sciences, Psychology, Brain Disorders, Neurosciences, Genetics, Fragile X Syndrome, Neurodegenerative, Intellectual and Developmental Disabilities (IDD), Clinical Research, Rare Diseases, 2.1 Biological and endogenous factors, Aetiology, Mental health, Neurological, Animals, Ataxia, Diagnosis, Differential, Disease Models, Animal, Fragile X Mental Retardation Protein, Humans, Nematoda, Tremor, Trinucleotide Repeats, neurodegeneration, dementia, premutation, RNA toxicity, CGG repeat, FXTAS, General Science & Technology

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is a late-onset neurodegenerative disorder that affects some but not all carriers of small, noncoding CGG-repeat expansions (55-200 repeats; premutation) within the fragile X gene (FMR1). Principal features of FXTAS include intention tremor, cerebellar ataxia, Parkinsonism, memory and executive function deficits, autonomic dysfunction, brain atrophy with white matter disease, and cognitive decline. Although FXTAS was originally considered to be confined to the premutation range, rare individuals with a gray zone (45-54 repeats) or an unmethylated full mutation (>200 repeats) allele have now been described, the constant feature of the disorder remaining the requirement for FMR1 expression, in contradistinction to the gene silencing mechanism of fragile X syndrome. Although transcriptional activity is required for FXTAS pathogenesis, the specific trigger(s) for FXTAS pathogenesis remains elusive, highlighting the need for more research in this area. This need is underscored by recent neuroimaging findings of changes in the central nervous system that consistently appear well before the onset of clinical symptoms, thus creating an opportunity to delay or prevent the appearance of FXTAS.

Published

2015

13. Dysregulated iron metabolism in the choroid plexus in fragile X-associated tremor/ataxia syndrome

Author

Ariza, Jeanelle, Steward, Craig, Rueckert, Flora, Widdison, Matt, Coffman, Robert, Afjei, Atiyeh, Noctor, Stephen C, Hagerman, Randi, Hagerman, Paul, and Martínez-Cerdeño, Verónica

Subjects

Medical Physiology, Biomedical and Clinical Sciences, Fragile X Syndrome, Intellectual and Developmental Disabilities (IDD), Neurosciences, Brain Disorders, Genetics, Neurodegenerative, Rare Diseases, 2.1 Biological and endogenous factors, Neurological, Aged, Aged, 80 and over, Antigens, CD, Ataxia, Cation Transport Proteins, Ceruloplasmin, Choroid Plexus, Epithelium, Female, Humans, Intracellular Space, Iron, Male, Middle Aged, Receptors, Transferrin, Transferrin, Tremor, FXTAS, Fragile X, Neurodegeneration, FMR1, Autism, Premutation, CGG repeat, Choroid plexus, Ferroportin, Psychology, Cognitive Sciences, Neurology & Neurosurgery, Biological psychology

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is a late-onset neurodegenerative disorder associated with premutation alleles of the FMR1 gene that is characterized by progressive action tremor, gait ataxia, and cognitive decline. Recent studies of mitochondrial dysfunction in FXTAS have suggested that iron dysregulation may be one component of disease pathogenesis. We tested the hypothesis that iron dysregulation is part of the pathogenic process in FXTAS. We analyzed postmortem choroid plexus from FXTAS and control subjects, and found that in FXTAS iron accumulated in the stroma, transferrin levels were decreased in the epithelial cells, and transferrin receptor 1 distribution was shifted from the basolateral membrane (control) to a predominantly intracellular location (FXTAS). In addition, ferroportin and ceruloplasmin were markedly decreased within the epithelial cells. These alterations have implications not only for understanding the pathophysiology of FXTAS, but also for the development of new clinical treatments that may incorporate selective iron chelation.

Published

2015

14. Immune mediated disorders in women with a fragile X expansion and FXTAS

Author

Jalnapurkar, Isha, Rafika, Nuva, Tassone, Flora, and Hagerman, Randi

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Mental Illness, Mental Health, Brain Disorders, Intellectual and Developmental Disabilities (IDD), Fragile X Syndrome, Rare Diseases, Neurosciences, Neurodegenerative, Mental health, Neurological, Adult, Aged, Ataxia, Female, Fragile X Mental Retardation Protein, Humans, Immune System Diseases, Middle Aged, Time Factors, Tremor, Trinucleotide Repeat Expansion, CGG repeat, FMR1 gene, FXTAS, RNA toxicity, autoimmune disease, genetic counseling, premutation, Genetics, Clinical sciences

Abstract

Premutation alleles in fragile X mental retardation 1 (FMR1) can cause the late-onset neurodegenerative disorder, fragile X-associated tremor ataxia syndrome (FXTAS) and/or the fragile X-associated primary ovarian insufficiency in approximately 20% of heterozygotes. Heterozygotes of the FMR1 premutation have a higher incidence of immune mediated disorders such as autoimmune thyroid disorder, especially when accompanied by FXTAS motor signs. We describe the time course of symptoms of immune mediated disorders and the subsequent development of FXTAS in four women with an FMR1 CGG expansion, including three with the premutation and one with a gray zone expansion. These patients developed an immune mediated disorder followed by neurological symptoms that become consistent with FXTAS. In all patients we observed a pattern involving an initial appearance of disease symptoms-often after a period of heightened stress (depression, anxiety, divorce, general surgery) followed by the onset of tremor and/or ataxia. Immune mediated diseases are associated with the manifestations of FXTAS temporally, although further studies are needed to clarify this association. If a cause and effect relationship can be established, treatment of pre-existing immune mediated disorders may benefit patients with pathogenic FMR1 mutations.

Published

2015

15. FMRpolyG-positive inclusions in CNS and non-CNS organs of a fragile X premutation carrier with fragile X-associated tremor/ataxia syndrome

Author

Buijsen, Ronald AM, Sellier, Chantal, Severijnen, Lies-Anne WFM, Oulad-Abdelghani, Mustapha, Verhagen, Rob FM, Berman, Robert F, Charlet-Berguerand, Nicolas, Willemsen, Rob, and Hukema, Renate K

Subjects

Adrenal Glands, Ataxia, Brain, Female, Fragile X Mental Retardation Protein, Fragile X Syndrome, Heterozygote, Humans, Intranuclear Inclusion Bodies, Kidney, Male, Myocardium, Thyroid Gland, Tremor, Ubiquitin, FXTAS, CGG repeat, FMRpolyG, RAN translation, Gain-of-function, Inclusions, Biochemistry and Cell Biology, Clinical Sciences, Neurosciences

Abstract

UNLABELLED: para ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s40478-014-0162-2) contains supplementary material, which is available to authorized users.

Published

2014

16. Induced expression of expanded CGG RNA causes mitochondrial dysfunction in vivo

Author

Hukema, Renate K, Buijsen, Ronald Am, Raske, Chris, Severijnen, Lies Anne, Nieuwenhuizen-Bakker, Ingeborg, Minneboo, Michelle, Maas, Alex, de Crom, Rini, Kros, Johan M, Hagerman, Paul J, Berman, Robert F, and Willemsen, Rob

Subjects

Biochemistry and Cell Biology, Biological Sciences, Fragile X Syndrome, Intellectual and Developmental Disabilities (IDD), Rare Diseases, Brain Disorders, Neurosciences, Genetics, Neurodegenerative, Orphan Drug, 2.1 Biological and endogenous factors, Aetiology, Neurological, Animals, Anti-Bacterial Agents, Apoptosis, Ataxia, Disease Models, Animal, Doxycycline, Fatty Liver, Liver, Mice, Mice, Transgenic, Mitochondria, Promoter Regions, Genetic, RNA, Reactive Oxygen Species, Repetitive Sequences, Nucleic Acid, Tremor, apoptosis, caspase 3, CGG repeat, cytochrome C, FXTAS, gpx-1, inducible mouse model, mitochondria, RNA gain-of-function, Tet-On, dox, doxycycline, eGFP, enhanced green fluorescent protein, Fragile X-associated tremor, ataxia syndrome, gpx, gluthation peroxidase, rtTA, reverse tetracycline transactivator, TRE, Tet Responsive Element, FXTAS, Fragile X-associated tremor/ataxia syndrome, TRE, Tet Responsive Element, dox, doxycycline, eGFP, enhanced green fluorescent protein, gpx, gluthation peroxidase, rtTA, reverse tetracycline transactivator, Developmental Biology, Biochemistry and cell biology

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is a late-onset neurodegenerative disorder affecting carriers of premutation forms of the FMR1 gene, resulting in a progressive development of tremor, ataxia and neuropsychological problems. The disease is caused by an expanded CGG repeat in the FMR1 gene, leading to an RNA gain-of-function toxicity mechanism. In order to study the pathogenesis of FXTAS, new inducible transgenic mouse models have been developed that expresses either 11CGGs or 90CGGs at the RNA level under control of a Tet-On promoter. When bred to an hnRNP-rtTA driver line, doxycycline (dox) induced expression of the transgene could be found in almost all tissues. Dox exposure resulted in loss of weight and death within 5 d for the 90CGG RNA expressing mice. Immunohistochemical examination of tissues of these mice revealed steatosis and apoptosis in the liver. Decreased expression of GPX1 and increased expression of cytochrome C is found. These effects were not seen in mice expressing a normal sized 11CGG repeat. In conclusion, we were able to show in vivo that expression of an expanded CGG-repeat rather than overexpression of a normal CGG-repeat causes pathology. In addition, we have shown that expanded CGG RNA expression can cause mitochondrial dysfunction by regulating expression levels of several markers. Although FTXAS patients do not display liver abnormalities, our findings contribute to understanding of the molecular mechanisms underlying toxicity of CGG repeat RNA expression in an animal model. In addition, the dox inducible mouse lines offer new opportunities to study therapeutic interventions for FXTAS.

Published

2014

17. Composition of the Intranuclear Inclusions of Fragile X-associated Tremor/Ataxia Syndrome

Author

Lisa Ma, Anthony W. Herren, Glenda Espinal, Jamie Randol, Bridget McLaughlin, Veronica Martinez-Cerdeño, Isaac N. Pessah, Randi J. Hagerman, and Paul J. Hagerman

Subjects

Fragile X, neurodegeneration, proteomics, CGG repeat, proteasome, inclusion, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Fragile X-associated tremor/ataxia syndrome (FXTAS) is a neurodegenerative disorder associated with a premutation repeat expansion (55–200 CGG repeats) in the 5′ noncoding region of the FMR1 gene. Solitary intranuclear inclusions within FXTAS neurons and astrocytes constitute a hallmark of the disorder, yet our understanding of how and why these bodies form is limited. Here, we have discovered that FXTAS inclusions emit a distinct autofluorescence spectrum, which forms the basis of a novel, unbiased method for isolating FXTAS inclusions by preparative fluorescence-activated cell sorting (FACS). Using a combination of autofluorescence-based FACS and liquid chromatography/tandem mass spectrometry (LC-MS/MS)-based proteomics, we have identified more than two hundred proteins that are enriched within the inclusions relative to FXTAS whole nuclei. Whereas no single protein species dominates inclusion composition, highly enriched levels of conjugated small ubiquitin-related modifier 2 (SUMO 2) protein and p62/sequestosome-1 (p62/SQSTM1) protein were found within the inclusions. Many additional proteins involved with RNA binding, protein turnover, and DNA damage repair were enriched within inclusions relative to total nuclear protein. The current analysis has also allowed the first direct detection, through peptide sequencing, of endogenous FMRpolyG peptide, the product of repeat-associated non-ATG (RAN) translation of the FMR1 mRNA. However, this peptide was found only at extremely low levels and not within whole FXTAS nuclear preparations, raising the question whether endogenous RAN products exist at quantities sufficient to contribute to FXTAS pathogenesis. The abundance of the inclusion-associated ubiquitin- and SUMO-based modifiers supports a model for inclusion formation as the result of increased protein loads and elevated oxidative stress leading to maladaptive autophagy. These results highlight the need to further investigate FXTAS pathogenesis in the context of endogenous systems.

Published

2019

18. Distribution of AGG interruption patterns within nine world populations

Author

Yrigollen, Carolyn M, Sweha, Stefan, Durbin-Johnson, Blythe, Zhou, Lili, Berry-Kravis, Elizabeth, Fernandez-Carvajal, Isabel, Faradz, Sultana Mh, Amiri, Khaled, Shaheen, Huda, Polli, Roberta, Murillo-Bonilla, Luis, Silva Arevalo, Gabriel de Jesus, Cogram, Patricia, Murgia, Alessandra, and Tassone, Flora

Subjects

Pediatric, Brain Disorders, Genetics, Rare Diseases, Intellectual and Developmental Disabilities (IDD), Clinical Research, Fragile X Syndrome, AGG interruptions, FMR1 allele, CGG repeat, expansion, ethnicity, Clinical Sciences, Pharmacology and Pharmaceutical Sciences

Abstract

The CGG trinucleotide repeat within the FMR1 gene is associated with multiple clinical disorders, including fragile X-associated tremor/ataxia syndrome, fragile X-associated primary ovarian insufficiency, and fragile X syndrome. Differences in the distribution and prevalence of CGG repeat length and of AGG interruption patterns have been reported among different populations and ethnicities. In this study we characterized the AGG interruption patterns within 3,065 normal CGG repeat alleles from nine world populations including Australia, Chile, United Arab Emirates, Guatemala, Indonesia, Italy, Mexico, Spain, and United States. Additionally, we compared these populations with those previously reported, and summarized the similarities and differences. We observed significant differences in AGG interruption patterns. Frequencies of longer alleles, longer uninterrupted CGG repeat segments and alleles with greater than 2 AGG interruptions varied between cohorts. The prevalence of fragile X syndrome and FMR1 associated disorders in various populations is thought to be affected by the total length of the CGG repeat and may also be influenced by the AGG distribution pattern. Thus, the results of this study may be important in considering the risk of fragile X-related conditions in various populations.

Published

2014

19. Differential Progression of Motor Dysfunction Between Male and Female Fragile X Premutation Carriers Reveals Novel Aspects of Sex-Specific Neural Involvement

Author

Danuta Z. Loesch, Flora Tassone, Anna Atkinson, Paige Stimpson, Nicholas Trost, Dean L. Pountney, and Elsdon Storey

Subjects

FMR1 premutation, CGG repeat, female carriers, motor scores, progression rates, gender differences, Biology (General), QH301-705.5

Abstract

Expansions of the CGG repeat in the non-coding segment of the FMR1 X-linked gene are associated with a variety of phenotypic changes. Large expansions (>200 repeats), which cause a severe neurodevelopmental disorder, the fragile x syndrome (FXS), are transmitted from the mothers carrying smaller, unstable expansions ranging from 55 to 200 repeats, termed the fragile X premutation. Female carriers of this premutation may themselves experience a wide range of clinical problems throughout their lifespan, the most severe being the late onset neurodegenerative condition called “Fragile X-Associated Tremor Ataxia Syndrome” (FXTAS), occurring between 8 and 16% of these carriers. Male premutation carriers, although they do not transmit expanded alleles to their daughters, have a much higher risk (40–50%) of developing FXTAS. Although this disorder is more prevalent and severe in male than female carriers, specific sex differences in clinical manifestations and progress of the FXTAS spectrum have been poorly documented. Here we compare the pattern and rate of progression (per year) in three motor scales including tremor/ataxia (ICARS), tremor (Clinical Tremor Rating scale, CRST), and parkinsonism (UPDRS), and in several cognitive and psychiatric tests scores, between 13 female and 9 male carriers initially having at least one of the motor scores ≥10. Moreover, we document the differences in each of the clinical and cognitive measures between the cross-sectional samples of 21 female and 24 male premutation carriers of comparable ages with FXTAS spectrum disorder (FSD), that is, who manifest one or more features of FXTAS. The results of progression assessment showed that it was more than twice the rate in male than in female carriers for the ICARS-both gait ataxia and kinetic tremor domains and twice as high in males on the CRST scale. In contrast, sex difference was negligible for the rate of progress in UPDRS, and all the cognitive measures. The overall psychiatric pathology score (SCL-90), as well as Anxiety and Obsessive/Compulsive domain scores, showed a significant increase only in the female sample. The pattern of sex differences for progression in motor scores was consistent with the results of comparison between larger, cross-sectional samples of male and female carriers affected with the FSD. These results were in concert with sex-specific distribution of MRI T2 white matter hyperintensities: all males, but no females, showed the middle cerebellar peduncle white matter hyperintensities (MCP sign), although the distribution and severity of these hyperintensities in the other brain regions were not dissimilar between the two sexes. In conclusion, the magnitude and specific pattern of sex differences in manifestations and progression of clinically recorded changes in motor performance and MRI lesion distribution support, on clinical grounds, the possibility of certain sex-limited factor(s) which, beyond the predictable effect of the second, normal FMR1 alleles in female premutation carriers, may have neuroprotective effects, specifically concerning the cerebellar circuitry.

Published

2021

20. Development of Chinese genetic reference panel for Fragile X Syndrome and its application to the screen of 10,000 Chinese pregnant women and women planning pregnancy

Author

Fei Gao, Wen Huang, Yanjun You, Jie Huang, Juan Zhao, Jin Xue, Huaixing Kang, Yingbao Zhu, Zhengmao Hu, Emily G. Allen, Peng Jin, Kun Xia, and Ranhui Duan

Subjects

CGG repeat, FMR1, Fragile X Syndrome, Genetics, QH426-470

Abstract

Abstract Background Fragile X syndrome (FXS) is the most common inherited form of intellectual disability caused by a CGG repeat expansion in the 5′ untranslated region of the FMR1 gene. When the number of repeats exceeds 200, the gene becomes hypermethylated and is transcriptionally silenced, resulting in FXS. Other allelic forms of the gene that are studied because of their instability or phenotypic consequence include intermediate alleles (45–54 CGG repeats) and premutation alleles (55–200 repeats). Normal alleles are classified as having

Published

2020

21. Curcumin Regulates the r(CGG)exp RNA Hairpin Structure and Ameliorate Defects in Fragile X-Associated Tremor Ataxia Syndrome

Author

Arun Kumar Verma, Eshan Khan, Subodh Kumar Mishra, Amit Mishra, Nicolas Charlet-Berguerand, and Amit Kumar

Subjects

FXTAS, therapeutics, trinucleotide, CGG repeat, RAN translation, splicing defects, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Fragile X-associated tremor ataxia syndrome is an untreatable neurological and neuromuscular disorder caused by unstable expansion of 55–200 CGG nucleotide repeats in 5′ UTR of Fragile X intellectual disability 1 (FMR1) gene. The expansion of CGG repeats in the FMR1 mRNA elicits neuronal cell toxicity through two main pathogenic mechanisms. First, mRNA with CGG expanded repeats sequester specific RNA regulatory proteins resulting in splicing alterations and formation of ribonuclear inclusions. Second, repeat-associated non-canonical translation (RANT) of the CGG expansion produces a toxic homopolymeric protein, FMRpolyG. Very few small molecules are known to modulate these pathogenic events, limiting the therapeutic possibilities for FXTAS. Here, we found that a naturally available biologically active small molecule, Curcumin, selectively binds to CGG RNA repeats. Interestingly, Curcumin improves FXTAS associated alternative splicing defects and decreases the production and accumulation of FMRpolyG protein inclusion. Furthermore, Curcumin decreases cell cytotoxicity promptly by expression of CGG RNA in FXTAS cell models. In conclusion, our data suggest that small molecules like Curcumin and its derivatives may be explored as a potential therapeutic strategy against the debilitating repeats associated neurodegenerative disorders.

Published

2020

22. Diagnostic profile of the AmplideX Fragile X Dx and Carrier Screen Kit for diagnosis and screening of fragile X syndrome and other FMR1-related disorders.

Author

Berry-Kravis, Elizabeth, Zhou, Lili, Jackson, Jonathan, and Tassone, Flora

Abstract

Introduction: In 2009, a novel, CGG repeat primed FMR1 PCR assay was designed with primers flanking the triplet repeat region, as well as a third chimeric primer complementary to the (CGG)n repeat, that was capable of amplifying alleles throughout the repeat range. This assay for the first time allowed consistent detection of large full mutation alleles with PCR, resolution of heterozygosity in females and mapping of AGG interspersions. Areas Covered: The AmplideX Fragile X Dx and Carrier Screen Kit (Asuragen, Inc.) represents a refined assay that underwent validation with sensitivity analyses for FDA approval. Single-site precision, analytical sensitivity and specificity, limit of detection and diagnostic performance were assessed in comparison to reference methods at three independent sites. Single-site precision across all genotype categories showed 100% agreement at 20 ng input across multiple operators, days, instruments and kit lots. Compared to Southern Blot analysis, the overall percent agreement was over 98% for all expanded alleles. Expert Opinion: Limitations include no methylation assessment and hard to see full mutation peaks in some mosaic samples, but overall the assay is considered a highly accurate and time-efficient assay for FMR1 allele size determination. [ABSTRACT FROM AUTHOR]

Published

2021

23. Development of Chinese genetic reference panel for Fragile X Syndrome and its application to the screen of 10,000 Chinese pregnant women and women planning pregnancy.

Author

Gao, Fei, Huang, Wen, You, Yanjun, Huang, Jie, Zhao, Juan, Xue, Jin, Kang, Huaixing, Zhu, Yingbao, Hu, Zhengmao, Allen, Emily G., Jin, Peng, Xia, Kun, and Duan, Ranhui

Subjects

FRAGILE X syndrome, CHINESE people, PREGNANT women, AUSTRALIANS, MATERNAL age, X chromosome

Abstract

Background: Fragile X syndrome (FXS) is the most common inherited form of intellectual disability caused by a CGG repeat expansion in the 5′ untranslated region of the FMR1 gene. When the number of repeats exceeds 200, the gene becomes hypermethylated and is transcriptionally silenced, resulting in FXS. Other allelic forms of the gene that are studied because of their instability or phenotypic consequence include intermediate alleles (45–54 CGG repeats) and premutation alleles (55–200 repeats). Normal alleles are classified as having <45 CGG repeats. Population screening studies have been conducted among American and Australian populations; however, large population‐based studies have not been completed in China. Methods and Results: In this work we present FXS screening results from 10,145 women of childbearing age from China. We first created and tested a standard panel that was comprised of normal, intermediate, premutation, and full mutation samples, and we performed the screening after confirming the consistency of genotyping results among laboratories. Conclusion: Based on our findings, we have determined the intermediate and premutation carrier prevalence of 1/130 and 1/634, respectively, among Chinese women. [ABSTRACT FROM AUTHOR]

Published

2020

24. Curcumin Regulates the r(CGG)exp RNA Hairpin Structure and Ameliorate Defects in Fragile X-Associated Tremor Ataxia Syndrome.

Author

Verma, Arun Kumar, Khan, Eshan, Mishra, Subodh Kumar, Mishra, Amit, Charlet-Berguerand, Nicolas, and Kumar, Amit

Subjects

CURCUMIN, SMALL molecules, RNA, CEREBELLUM degeneration, NEUROMUSCULAR diseases, ATAXIA, SPINOCEREBELLAR ataxia

Abstract

Fragile X-associated tremor ataxia syndrome is an untreatable neurological and neuromuscular disorder caused by unstable expansion of 55–200 CGG nucleotide repeats in 5′ UTR of Fragile X intellectual disability 1 (FMR1) gene. The expansion of CGG repeats in the FMR1 mRNA elicits neuronal cell toxicity through two main pathogenic mechanisms. First, mRNA with CGG expanded repeats sequester specific RNA regulatory proteins resulting in splicing alterations and formation of ribonuclear inclusions. Second, repeat-associated non-canonical translation (RANT) of the CGG expansion produces a toxic homopolymeric protein, FMRpolyG. Very few small molecules are known to modulate these pathogenic events, limiting the therapeutic possibilities for FXTAS. Here, we found that a naturally available biologically active small molecule, Curcumin, selectively binds to CGG RNA repeats. Interestingly, Curcumin improves FXTAS associated alternative splicing defects and decreases the production and accumulation of FMRpolyG protein inclusion. Furthermore, Curcumin decreases cell cytotoxicity promptly by expression of CGG RNA in FXTAS cell models. In conclusion, our data suggest that small molecules like Curcumin and its derivatives may be explored as a potential therapeutic strategy against the debilitating repeats associated neurodegenerative disorders. Candidate small molecule Curcumin ameliorates expanded CGG RNA mediated disease pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2020

25. Neural progenitor cells from an adult patient with fragile X syndrome

Author

Schwartz, Philip H., Tassone, Flora, Greco, Claudia M., Nethercott, Hubert E., Ziaeian, Boback, Hagerman, Randi J., and Hagerman, Paul J.

Subjects

central-nervous-system, stem-cells, mental-retardation, human brain, cgg repeat, gene, model, establishment, instability, neurons

Abstract

Background: Currently, there is no adequate animal model to study the detailed molecular biochemistry of fragile X syndrome, the leading heritable form of mental impairment. In this study, we sought to establish the use of immature neural cells derived from adult tissues as a novel model of fragile X syndrome that could be used to more fully understand the pathology of this neurogenetic disease. Methods: By modifying published methods for the harvest of neural progenitor cells from the post-mortem human brain, neural cells were successfully harvested and grown from post-mortem brain tissue of a 25-year-old adult male with fragile X syndrome, and from brain tissue of a patient with no neurological disease. Results: The cultured fragile X cells displayed many of the characteristics of neural progenitor cells, including nestin and CD133 expression, as well as the biochemical hallmarks of fragile X syndrome, including CGG repeat expansion and a lack of FMRP expression. Conclusion: The successful production of neural cells from an individual with fragile X syndrome opens a new avenue for the scientific study of the molecular basis of this disorder, as well as an approach for studying the efficacy of new therapeutic agents.

Published

2005

26. Positive Emotional Support in Premutation Carrier Mothers of Adolescents and Adults With Fragile X Syndrome: Gene by Environment Interactions.

Author

Hartley, Sigan L., DaWalt, Leann S., Jinkuk Hong, Greenberg, Jan S., Mailick, Marsha R., and Hong, Jinkuk

Subjects

FRAGILE X syndrome, ADULTS, MULTILEVEL models, ECOLOGY

Abstract

Copyright of American Journal on Intellectual & Developmental Disabilities is the property of American Association on Intellectual & Developmental Disabilities and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2019

27. Molecular analysis of FMR1 alleles for fragile X syndrome diagnosis and patient stratification.

Author

Kumari, Daman and Usdin, Karen

Published

2020

28. Decreased functional brain response to emotional arousal and increased psychiatric symptomology in FMR1 premutation carriers.

Author

Brown, Stephanie S.G., Whalley, Heather C., Kind, Peter C., and Stanfield, Andrew C.

Subjects

*AROUSAL (Physiology), *MENTAL illness, *SYMPTOMS, *FUNCTIONAL magnetic resonance imaging, *FRAGILE X syndrome

Abstract

Highlights • BOLD response to emotional processing is reduced in male FMR1 premutation carriers. • No BOLD group x age interaction was found, suggesting stability of emotional changes. • Premutation carriers exhibited worse psychiatric symptomatology. • Carriers show increased autistic traits and impaired facial emotion recognition. • Clinical and neuropsychological measurements also showed no relationship with age. Abstract The FMR1 premutation is an expansion of the CGG repeat island in the FMR1 gene to between 55 and 200 repeats. Evidence suggests that as well as conferring risk for neurodegeneration, the premutation is also associated with increased risk for autistic traits and psychiatric symptoms. An emotional processing fMRI task was used to examine the response to a change in emotional arousal in 17 male carriers and 17 matched controls. A psychiatric symptom checklist (SCL-90-R), autism spectrum and empathy quotients (AQ and EQ), and the Ekman Faces Test were used to investigate clinical symptoms and emotional processing. Carriers exhibited significantly lower activation compared to controls at the bilateral superior parietal lobe, bilateral Brodmann Area (BA) 17 (V1), right intraparietal area and right BA18 (V2) when comparing high and low arousal conditions. Group by age analyses were not significant. Assessments revealed that carriers displayed significantly worse symptoms of psychiatric symptoms and higher levels of autistic traits, as well as impaired facial emotion recognition. No measurements revealed an association with age. Here, we show significantly altered emotional processing in carriers which display stability over age, suggesting that, unlike degenerative aspects, emotional symptoms may be consistent over the lifespan in carriers. [ABSTRACT FROM AUTHOR]

Published

2019

29. Premutations of FMR1 CGG repeats are not related to idiopathic premature ovarian failure in Iranian patients: A case control study.

Author

Asadi, Rezvaneh, Omrani, Mir Davood, Ghaedi, Hamid, Mirfakhraie, Reza, Azargashb, Eznollah, Habibi, Mohsen, and Pouresmaeili, Farkhondeh

Subjects

*PREMATURE ovarian failure, *POPULATION-based case control, *TRINUCLEOTIDE repeats, *ETIOLOGY of diseases, *CAPILLARY electrophoresis, *BIOLOGICAL tags

Abstract

Abstract Premature ovarian failure (POF) is a reproductive disease which affects 1 in 100 under 40 years women. FMR1 premutation carriers of CGG repeats are supposed to be at increased risk for POF. We have examined the 5′UTR region of the gene to find any association between the repeat size and the disease etiology in Iranian population. 30 women with early idiopathic POF and 30 fertile control women were selected. We used triplet repeat primed PCR (TP PCR) assay and gene-specific primers to amplify the CpG Island of FMR1 gene promoter region. The amplification results were analyzed by capillary electrophoresis and Gene Marker software. Among 30 patients, two had intermediate repeat size, one had premutation and the rest had CGG repeat of the normal range. Two of controls had intermediate repeats and none had a premutation. Two groups had significant differences in the repeat number average (p = 0.007) and in the average length of the smallest allele (p < 0.001), but had no promising difference in average length of the longest allele (p = 0.453). Although the two groups showed a significant difference in the length of alleles, their length was within normal range. Perhaps the polymorphism, in connection with the genome's entire network, has been involved in the development of the disease, or there has been a fundamentally different mechanism for the disease in Iranian population. A larger number of Iranian POF patients should be investigated for any probable relationship between the CGG triplet repeat length and the etiology of the disease. Highlights • Thirty women of early idiopathic POF and 30 fertile controls screened for CpG Island of FMR1 promoter region. • While two groups had a significant difference in the length of repeats, the observed longitudinal polymorphism was within the normal range. • No significant association was between longitudinal changes of CGG repeats of the FMR1 gene and POF. [ABSTRACT FROM AUTHOR]

Published

2018

30. Use of human-derived stem cells to create a novel, in vitro model designed to explore FMR1 CGG repeat instability amongst female premutation carriers.

Author

Gustin, Stephanie L. F., Wang, Guangwen, Baker, Valerie M., Latham, Gary, and Sebastiano, Vittorio

Subjects

*STEM cells, *GENETIC transcription, *FRAGILE X syndrome, *SPECTROPHOTOMETERS, *TRINUCLEOTIDE repeats

Abstract

Objective: Create a model, using reprogrammed cells, to provide a platform to identify the mechanisms of CGG repeat instability amongst female fragile X mental retardation 1 gene (FMR1) premutation (PM) carriers.Methods: Female PM carriers (with and without POI) and healthy controls were enrolled from June 2013 to April 2014. Patient-derived fibroblasts (FB) were reprogrammed to induced pluripotent stem cells (iPSC) using viral vectors, encoding KLF4, OCT4, SOX2, and MYC. FMR1 CGG repeat-primed PCR was used to assess the triplet repeat structure of the FMR1 gene. FMR1 promoter methylation (%) was determined using FMR1 methylation PCR (mPCR). Quantification of FMR1 transcripts by RT-qPCR was used to evaluate the effect of reprogramming on gene transcription, as well as to correlate patient phenotype with FMR1 expression. Production of FMR1 protein (FMRP) was determined using a liquid bead array-based immunoassay.Results: Upon induction to pluripotency, all control clones exhibited maintenance of progenitor cell CGG repeat number, whereas 10 of 12 clones derived from PM carriers maintained their input CGG repeat number, one of which expanded and one contracted. As compared to parent FB, iPSC clones exhibited a skewed methylation pattern; however, downstream transcription and translation appeared unaffected. Further, the PM carriers, regardless of phenotype, exhibited similar FMR1 transcription and translation to the controls.Conclusions: This is the first study to establish a stem cell model aimed to understand FMR1 CGG repeat instability amongst female PM carriers. Our preliminary data indicate that CGG repeat number, transcription, and translation are conserved upon induction to pluripotency. [ABSTRACT FROM AUTHOR]

Published

2018

31. Assessment of efficacy of prenatal genetic diagnosis for fragile X syndrome using nested PCR.

Author

Miao, Zhengyou, Liu, Xiaodan, Li, Weiwei, He, Qunyan, and Liu, Xia

Subjects

*FRAGILE X syndrome, *HUMAN chromosome abnormalities, *POLYMERASE chain reaction, *PRENATAL diagnosis, *AUTISM spectrum disorders

Abstract

Fragile X syndrome (FXS) is the most common inherited cause of intellectual disability and the leading monogenic cause of autism spectrum disorder. It has previously been demonstrated that prenatal genetic diagnosis is efficient for the diagnosis of FXS. The present study investigated the diagnostic effects of nested polymerase chain reaction (PCR) for fragile X mental retardation 1 (FMR1) and expanded CGG repeats. It was demonstrated that the nested PCR assay rapidly measured the multi-copies of the FMR1 gene in individual samples. The nested PCR assay detected normal CGG repeat lengths and expanded CGG repeat lengths with a low occurrence of false positives. In addition, the nested PCR assay resulted in increased sensitivity and specificity for patients with FXS. Furthermore, the nested PCR assay identified the mutation and generated conclusive cases for FXS, indicating that this assay is beneficial for the diagnosis of FXS patients. In conclusion, these outcomes indicate that nested PCR assay is a reliable and easier method for diagnosis of FXS, which may be used for the diagnosis of FXS patients. [ABSTRACT FROM AUTHOR]

Published

2018

32. Evaluation of simultaneous binding of Chromomycin A3 to the multiple sites of DNA by the new restriction enzyme assay.

Author

Murase, Hirotaka, Noguchi, Tomoharu, and Sasaki, Shigeki

Subjects

*ANTINEOPLASTIC agents, *ANTINEOPLASTIC agent synthesis, *BINDING site assay, *DNA replication, *NUCLEOTIDE sequence

Abstract

Chromomycin A3 (CMA3) is an aureolic acid-type antitumor antibiotic. CMA3 forms dimeric complexes with divalent cations, such as Mg 2+ , which strongly binds to the GC rich sequence of DNA to inhibit DNA replication and transcription. In this study, the binding property of CMA3 to the DNA sequence containing multiple GC-rich binding sites was investigated by measuring the protection from hydrolysis by the restriction enzymes, Acc II and Fnu 4HI, for the center of the CGCG site and the 5′-GC↓GGC site, respectively. In contrast to the standard DNase I footprinting method, the DNA substrates are fully hydrolyzed by the restriction enzymes, therefore, the full protection of DNA at all the cleavable sites indicates that CMA3 simultaneously binds to all the binding sites. The restriction enzyme assay has suggested that CMA3 has a high tendency to bind the successive CGCG sites and the CGG repeat. [ABSTRACT FROM AUTHOR]

Published

2018

33. Detecting AGG Interruptions in Females With a FMR1 Premutation by Long-Read Single-Molecule Sequencing: A 1 Year Clinical Experience.

Author

Ardui, Simon, Race, Valerie, de Ravel, Thomy, Van Esch, Hilde, Devriendt, Koenraad, Matthijs, Gert, and Vermeesch, Joris R.

Subjects

FRAGILE X syndrome, GENETIC mutation, PREIMPLANTATION genetic diagnosis

Abstract

The fragile X syndrome arises from the FMR1 CGG expansion of a premutation (55-200 repeats) to a fullmutation allele (>200 repeats) and is themost frequent cause of inherited X-linked intellectual disability. The risk for a premutation to expand to a full mutation allele depends on the repeat length and AGG triplets interrupting this repeat. In genetic counseling it is important to have information on both these parameters to provide an accurate risk estimate to women carrying a premutation allele and weighing up having children. For example, in case of a small risk a woman might opt for a natural pregnancy followed up by prenatal diagnosis while she might choose for preimplantation genetic diagnosis (PGD) if the risk is high. Unfortunately, the detection of AGG interruptions was previously hampered by technical difficulties complicating their use in diagnostics. Therefore we recently developed, validated and implemented a new methodology which uses long-read single-molecule sequencing to identify AGG interruptions in females with a FMR1 premutation. Here we report on the assets of AGG interruption detection by sequencing and the impact of implementing the assay on genetic counseling. [ABSTRACT FROM AUTHOR]

Published

2018

34. Evaluating the clinical utility of a long-read sequencing-based approach in genetic testing of fragile-X syndrome.

Author

Hou, Fei, Mao, Aiping, Shan, Shan, Li, Yan, Meng, Wanli, Zhan, Jiahan, Nie, Wenying, and Jin, Hua

Subjects

*GENETIC testing, *FRAGILE X syndrome, *GENETIC counseling, *GENETIC variation, *NUCLEOTIDE sequencing

Abstract

• Long-read sequencing-based methods were developed to analyze FMR1 genetic variations. • CAFXS successfully called all the FMR1 CGG expansion. • CAFXS identified 24-bp microdeletions, which was miscalled by conventional methods. • CAFXS allowed for precise constructing FMR1 CGG repeat and AGG interruption pattern. • CAFXS represents a more comprehensive and accurate approach for FXS genetic testing. Fragile X syndrome (FXS) arises from the FMR1 CGG expansion. Comprehensive genetic testing for FMR1 CGG expansions, AGG interruptions, and microdeletions is essential to provide genetic counseling for females carrying premutation alleles. However, conventional PCR-based FMR1 assays mainly focus on CGG repeats, and could detect AGG interruption only in males. The clinical utility of a long-read sequencing-based assay termed comprehensive analysis of FXS (CAFXS) was evaluated in 238 high-risk samples by comparing to conventional PCR assays. PCR assays identified five premuation and three full mutation categories alleles in all the samples, and CAFXS successfully called all the FMR1 CGG expansion. CAFXS identified 24-bp microdeletions upstream to the trinucleotide region with 30 CGG repeats, which was miscalled by the length-based PCR methods. CAFXS also identified a 187-bp deletion in about 1/7 of the sequencing reads in a male patient with mosaic full mutation alleles. CAFXS allowed for precise constructing the FMR1 CGG repeat and AGG interruption pattern in all the samples, and identified a novel and alternative CGA interruption in one normal female sample. CAFXS represents a more comprehensive and accurate approach for FXS genetic testing that potentially enables more informed genetic counseling compared to PCR-based methods. [ABSTRACT FROM AUTHOR]

Published

2023

35. Fragile X-Associated Tremor/Ataxia Syndrome: From Molecular Pathogenesis to Development of Therapeutics

Author

Ha Eun Kong, Juan Zhao, Shunliang Xu, Peng Jin, and Yan Jin

Subjects

FXTAS pathogenesis, CGG repeat, RNA toxicity, RAN translation, FXTAS therapeutics, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Fragile X-associated tremor/ataxia syndrome (FXTAS) is a neurodegenerative disorder caused by a premutation CGG repeat expansion (55–200 repeats) within the 5′ UTR of the fragile X gene (FMR1). FXTAS is characterized by intension tremor, cerebellar ataxia, progressive neurodegeneration, parkinsonism and cognitive decline. The development of transgenic mouse and Drosophila melanogaster models carrying an expanded CGG repeat has yielded valuable insight into the pathophysiology of FXTAS. To date, we know of two main molecular mechanisms of this disorder: (1) a toxic gain of function of the expanded CGG-repeat FMR1 mRNA, which results in the binding/sequestration of the CGG-binding proteins; and (2) CGG repeat-associated non-AUG-initiated (RAN) translation, which generates a polyglycine peptide toxic to cells. Besides these CGG-mediated mechanisms, recent studies have shed light on additional mechanisms of pathogenesis, such as the antisense transcript ASFMR1, mitochondrial dysfunction, DNA damage from R-loop formation and 5-hydroxymethylcytosine (5hmC)-mediated epigenetic modulation. Here we summarize the recent progress towards understanding the etiology of FXTAS and provide an overview of potential treatment strategies.

Published

2017

36. Refining the risk for fragile X–associated primary ovarian insufficiency (FXPOI) by FMR1 CGG repeat size

Author

Weiya He, Sarah L. Nolin, Krista Charen, Katharine E. Shelly, Nicole Tortora, Lisa Shubeck, Stephanie L. Sherman, Heather S. Hipp, Bonnie McKinnon, Emily G. Allen, Anne Glicksman, and Ashima Amin

Subjects

medicine.medical_specialty, Fragile x, Obstetrics, business.industry, Age at menopause, Primary ovarian insufficiency, Menopause, Premature, Primary Ovarian Insufficiency, FMR1, Article, Fragile X Mental Retardation Protein, Increased risk, Family planning, Cgg repeat, Fragile X Syndrome, medicine, Humans, Female, business, Risk assessment, Genetics (clinical)

Abstract

Purpose Approximately 20–30% of women with an FMR1 premutation experience fragile X–associated primary ovarian insufficiency (FXPOI); however, current risk estimates based on repeat size only identify women with the midrange of repeats to be at the highest risk. Methods To better understand the risk by repeat size, we collected self-reported reproductive histories on 1,668 women and divided them into high-resolution repeat size bins of ~5 CGG repeats to determine a more accurate risk for FXPOI in relation to CGG repeat length. Results As previously reported, women with 70–100 CGG repeats were at the highest risk for FXPOI using various statistical models to compare average age at menopause and risk of FXPOI, with women with 85–89 repeats being at the highest risk. Importantly, women with 120 repeats did not have a significantly increased risk for FXPOI compared to women with

Published

2021

37. Molecular analysis of fragile X syndrome (FXS) among Malaysian patients with developmental disability.

Author

ALI, Ernie Zuraida, YAKOB, Yusnita, MD DESA, Norsiah, ISHAK, Taufik, ZAKARIA, Zubaidah, Lock-Hock NGU, and Wee-Teik KENG

Abstract

Fragile X syndrome (FXS) is a neurodevelopmental disorder commonly found worldwide, caused by the silencing of fragile X mental retardation 1 (FMR1) gene on the X-chromosome. Most of the patients lost FMR1 function due to an expansion of cytosine-guanine-guanine (CGG) repeat at the 5' untranslated region (5'UTR) of the gene. The purpose of this study is to identify the prevalence of FXS and characterize the FMR1 gene CGG repeats distribution among children with developmental disability in Malaysia. Genomic DNA of 2201 samples from different ethnicities (Malays, Chinese, Indian and others) of both genders were PCR-amplified from peripheral blood leukocytes based on specific primers at 5'UTR of FMR1 gene. Full mutations and mosaics were successfully identified by triple methylation specific PCR (ms-PCR) and subsequently verified with FragilEase kit. The findings revealed for the first time the prevalence of FXS full mutation in children with developmental disability in Malaysia was 3.5%, a slightly higher figure as compared to other countries. Molecular investigation also identified 0.2% and 0.4% probands have permutation and intermediate alleles, respectively. The CGG repeats length observation showed 95% of patients had normal alleles within 11 to 44 CGG repeats; with 29 repeats found most common among Malays and Indians while 28 repeats were most common among Chinese. In conclusion, this is the first report of prevalence and characterisation of CGG repeats that reflects genetic variability among Malaysian ethnic grouping. [ABSTRACT FROM AUTHOR]

Published

2017

38. Oculopharyngodistal myopathy with coexisting histology of systemic neuronal intranuclear inclusion disease: Clinicopathologic features of an autopsied patient harboring CGG repeat expansions in LRP12

Author

Hiroshi Shimizu, Yoshiaki Honma, Takeshi Ikeuchi, Yo Higuchi, Norikazu Hara, Naomi Mezaki, Akinori Miyashita, Osamu Onodera, Akiyoshi Kakita, Izumi Kawachi, Kazuhiro Sanpei, Miura Takeshi, and Rie Saito

Subjects

Male, Pathology, medicine.medical_specialty, Neurology, Intranuclear Inclusion Bodies, Oculopharyngodistal Myopathy, Neuropathology, Neuronal intranuclear inclusion disease, Muscular Dystrophies, lcsh:RC346-429, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, NEURONAL INTRANUCLEAR INCLUSION DISEASE, medicine, Humans, Muscle, Skeletal, Letter to the Editor, lcsh:Neurology. Diseases of the nervous system, business.industry, Histology, Neurodegenerative Diseases, Oculopharyngodistal myopathy, Noncoding CGG expansions, Pedigree, Oculopharyngeal myopathy with leukoencephalopathy, Cgg repeat, Neurology (clinical), business, Trinucleotide Repeat Expansion, Low Density Lipoprotein Receptor-Related Protein-1

Published

2020

39. Site-specific R-loops induce CGG repeat contraction and fragile X gene reactivation.

Author

Lee, Hun-Goo, Imaichi, Sachiko, Kraeutler, Elizabeth, Aguilar, Rodrigo, Lee, Yong-Woo, Sheridan, Steven D., and Lee, Jeannie T.

Subjects

*FRAGILE X syndrome, *DNA demethylation, *GENE expression, *AUTISM spectrum disorders, *GENES

Abstract

Here, we describe an approach to correct the genetic defect in fragile X syndrome (FXS) via recruitment of endogenous repair mechanisms. A leading cause of autism spectrum disorders, FXS results from epigenetic silencing of FMR1 due to a congenital trinucleotide (CGG) repeat expansion. By investigating conditions favorable to FMR1 reactivation, we find MEK and BRAF inhibitors that induce a strong repeat contraction and full FMR1 reactivation in cellular models. We trace the mechanism to DNA demethylation and site-specific R-loops, which are necessary and sufficient for repeat contraction. A positive feedback cycle comprising demethylation, de novo FMR1 transcription, and R-loop formation results in the recruitment of endogenous DNA repair mechanisms that then drive excision of the long CGG repeat. Repeat contraction is specific to FMR1 and restores the production of FMRP protein. Our study therefore identifies a potential method of treating FXS in the future. [Display omitted] • We identify an approach to excise long CGG repeats in fragile X syndrome • CGG contraction involves recruitment of endogenous DNA repair machinery • Site-specific R-loop formation is necessary and sufficient for the repeat contraction • CGG repeat contraction reactivates the silenced FMR1 gene and restores FMRP protein Site-specific R-loop formation leads to the contraction of expanded CGG repeats associated with fragile X syndrome and restores expression of the silenced FMRP protein. [ABSTRACT FROM AUTHOR]

Published

2023

40. Detecting AGG Interruptions in Male and Female FMR1 Premutation Carriers by Single-Molecule Sequencing.

Author

Ardui, Simon, Race, Valerie, Zablotskaya, Alena, Hestand, Matthew S., Esch, Hilde, Devriendt, Koenraad, Matthijs, Gert, and Vermeesch, Joris R.

Abstract

ABSTRACT The FMR1 gene contains an unstable CGG repeat in its 5′ untranslated region. Premutation alleles range between 55 and 200 repeat units and confer a risk for developing fragile X-associated tremor/ataxia syndrome or fragile X-associated primary ovarian insufficiency. Furthermore, the premutation allele often expands to a full mutation during female germline transmission giving rise to the fragile X syndrome. The risk for a premutation to expand depends mainly on the number of CGG units and the presence of AGG interruptions in the CGG repeat. Unfortunately, the detection of AGG interruptions is hampered by technical difficulties. Here, we demonstrate that single-molecule sequencing enables the determination of not only the repeat size, but also the complete repeat sequence including AGG interruptions in male and female alleles with repeats ranging from 45 to 100 CGG units. We envision this method will facilitate research and diagnostic analysis of the FMR1 repeat expansion. [ABSTRACT FROM AUTHOR]

Published

2017

41. Molecular Correlates and Recent Advancements in the Diagnosis and Screening of FMR1-Related Disorders.

Author

Rajan-Babu, Indhu-Shree and Chong, Samuel S.

Subjects

*GENE mapping, *MOSAICISM, *DNA methylation, *DIAGNOSIS of fragile X syndrome, *INTELLECTUAL disabilities, *POLYMERASE chain reaction

Abstract

Fragile X syndrome (FXS) is the most common monogenic cause of intellectual disability and autism. Molecular diagnostic testing of FXS and related disorders (fragile X-associated primary ovarian insufficiency (FXPOI) and fragile X-associated tremor/ataxia syndrome (FXTAS)) relies on a combination of polymerase chain reaction (PCR) and Southern blot (SB) for the fragile X mental retardation 1 (FMR1) CGG-repeat expansion and methylation analyses. Recent advancements in PCR-based technologies have enabled the characterization of the complete spectrum of CGG-repeat mutation, with or without methylation assessment, and, as a result, have reduced our reliance on the labor- and time-intensive SB, which is the gold standard FXS diagnostic test. The newer and more robust triplet-primed PCR or TP-PCR assays allow the mapping of AGG interruptions and enable the predictive analysis of the risks of unstable CGG expansion during mother-to-child transmission. In this review, we have summarized the correlation between several molecular elements, including CGG-repeat size, methylation, mosaicism and skewed X-chromosome inactivation, and the extent of clinical involvement in patients with FMR1-related disorders, and reviewed key developments in PCR-based methodologies for the molecular diagnosis of FXS, FXTAS and FXPOI, and large-scale (CGG)n expansion screening in newborns, women of reproductive age and high-risk populations. [ABSTRACT FROM AUTHOR]

Published

2016

42. Structure and stability upon maternal transmission of common and intermediate FMR1 (Fragile X Mental Retardation 1) alleles in a sample of the Brazilian population

Author

Leonardo P. Capelli, Regina C. Mingroni-Netto, and Angela M. Vianna-Morgante

Subjects

FMR1 gene, CGG repeat, fragile X, Genetics, QH426-470

Abstract

In order to investigate the stability of the FMR1 (Fragile X Mental Retardation 1) alleles from the normal population, when maternally inherited, we analyzed 75 mother-to-son transmissions. Sixty-eight alleles fell within the common range with 20-40 CGG repeats, and seven alleles were intermediate, with 41-48 repeats. No change was observed either in the length or in the structure of these repeats upon transmission. Fifty-three alleles were ascertained in different families, and their size distribution was similar to those described for European and European-derived populations, with three peaks of frequency: 66% of the alleles with (CGG)29, (CGG)30 or (CGG)31, 7.5% with (CGG)20, and 5.7% with (CGG)23. Regarding the AGG interspersion pattern, 69.8% had two AGG repeats, 20.8% had one, 5.7% had three and 3.8% had none. The most common patterns were 10+9+9 (30.2%), 9+9+9 (18.9%), 10+9 (7.5%), and 10+9+10 (7.5%). About 70% of the alleles with up to 40 repeats were linked to the DXS548/FRAXAC1 haplotype 7-3, the most commonly reported in normal populations. Four out of five intermediate alleles were in linkage with the two haplotypes most frequently associated to the FMR1 full mutation, 2-1 and 6-4. These four alleles showed long uninterrupted CGG repeats at the 3' end. The 9+9+22, 9+9+23 and 9+9+28 alleles were linked to the haplotype 2-1, and the 9+37 allele, to the haplotype 6-4. The pattern of AGG interspersion of these alleles and the associated haplotypes were in accordance with the two main pathways toward mutation previously proposed.

Published

2005

43. Neuroimaging Insight Into Fragile X-Associated Neuropsychiatric Disorders: Literature Review

Author

Andrea Elias-Mas, Maria Isabel Alvarez-Mora, Conxita Caro-Benito, and Laia Rodriguez-Revenga

Subjects

Psychiatry, Fragile x, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, neuropathology, Ataxia, neuroimaging, business.industry, Primary ovarian insufficiency, RC435-571, Disease, Neuropathology, FMR1, FXAND, nervous system diseases, Psychiatry and Mental health, Neuroimaging, Cgg repeat, medicine, functional studies, Systematic Review, medicine.symptom, business, FMR1 premutation

Abstract

FMR1 premutation is defined by 55–200 CGG repeats in the Fragile X Mental Retardation 1 (FMR1) gene. FMR1 premutation carriers are at risk of developing a neurodegenerative disease called fragile X-associated tremor/ataxia syndrome (FXTAS) and Fragile X-associated primary ovarian insufficiency (FXPOI) in adulthood. In the last years an increasingly board spectrum of clinical manifestations including psychiatric disorders have been described as occurring at a greater frequency among FMR1 premutation carriers. Herein, we reviewed the neuroimaging findings reported in relation with psychiatric symptomatology in adult FMR1 premutation carriers. A structured electronic literature search was conducted on FMR1 premutation and neuroimaging yielding a total of 3,229 articles examined. Of these, 7 articles were analyzed and are included in this review. The results showed that the main radiological findings among adult FMR1 premutation carriers presenting neuropsychiatric disorders were found on the amygdala and hippocampus, being the functional abnormalities more consistent and the volumetric changes more inconsistent among studies. From a molecular perspective, CGG repeat size, FMR1 mRNA and FMRP levels have been investigated in relation with the neuroimaging findings. Based on the published results, FMRP might play a key role in the pathophysiology of the psychiatric symptoms described among FMR1 premutation carriers. However, additional studies including further probes of brain function and a broader scope of psychiatric symptom measurement are required in order to obtain a comprehensive landscape of the neuropsychiatric phenotype associated with the FMR1 premutation.

Published

2021

44. Human-specific tandem repeat expansion and differential gene expression during primate evolution

Author

Mark Chaisson, Alex A. Pollen, Ruiyang Li, Arvis Sulovari, Glennis A. Logsdon, Mitchell R. Vollger, Peter A. Audano, Evan E. Eichler, David Porubsky, Wesley C. Warren, and Damage and Repair in Cancer Development and Cancer Treatment (DARE)

Subjects

Primates, SUSCEPTIBILITY LOCI, INSULIN GENE, RNA Splicing, VNTR, INSTABILITY, Genomics, Retrotransposon, CGG REPEAT, Biology, STR, Genome, Evolution, Molecular, Tandem repeat, Animals, Humans, Disease, GENOME-WIDE ASSOCIATION, Gene, Multidisciplinary, HEXANUCLEOTIDE REPEAT, Genome, Human, MUTATIONS, Biological Sciences, Subtelomere, REGIONS, genome instability, Variable number tandem repeat, tandem repeat, Evolutionary biology, Tandem Repeat Sequences, Genomic Structural Variation, Microsatellite, tandem repeat expansion, GENERATION

Abstract

Short tandem repeats (STRs) and variable number tandem repeats (VNTRs) are important sources of natural and disease-causing variation, yet they have been problematic to resolve in reference genomes and genotype with short-read technology. We created a framework to model the evolution and instability of STRs and VNTRs in apes. We phased and assembled 3 ape genomes (chimpanzee, gorilla, and orangutan) using long-read and 10x Genomics linked-read sequence data for 21,442 human tandem repeats discovered in 6 haplotype-resolved assemblies of Yoruban, Chinese, and Puerto Rican origin. We define a set of 1,584 STRs/VNTRs expanded specifically in humans, including large tandem repeats affecting coding and noncoding portions of genes (e.g., MUC3A , CACNA1C ). We show that short interspersed nuclear element–VNTR– Alu (SVA) retrotransposition is the main mechanism for distributing GC-rich human-specific tandem repeat expansions throughout the genome but with a bias against genes. In contrast, we observe that VNTRs not originating from retrotransposons have a propensity to cluster near genes, especially in the subtelomere. Using tissue-specific expression from human and chimpanzee brains, we identify genes where transcript isoform usage differs significantly, likely caused by cryptic splicing variation within VNTRs. Using single-cell expression from cerebral organoids, we observe a strong effect for genes associated with transcription profiles analogous to intermediate progenitor cells. Finally, we compare the sequence composition of some of the largest human-specific repeat expansions and identify 52 STRs/VNTRs with at least 40 uninterrupted pure tracts as candidates for genetically unstable regions associated with disease.

Published

2019

45. Positive Emotional Support in Premutation Carrier Mothers of Adolescents and Adults With Fragile X Syndrome: Gene by Environment Interactions

Author

Leann Smith DaWalt, Sigan L. Hartley, Jinkuk Hong, Jan S. Greenberg, and Marsha R. Mailick

Subjects

Adult, Male, Heterozygote, Cortisol awakening response, Emotional support, Adolescent, Health Status, Population, Mothers, Article, 050105 experimental psychology, Fragile X Mental Retardation Protein, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Trinucleotide Repeats, Arts and Humanities (miscellaneous), Developmental and Educational Psychology, medicine, Humans, 0501 psychology and cognitive sciences, education, Aged, education.field_of_study, Gene by environment, 05 social sciences, Social Support, General Medicine, Genetic Status, Middle Aged, medicine.disease, FMR1, Fragile X syndrome, Psychiatry and Mental health, Neuropsychology and Physiological Psychology, Cgg repeat, Fragile X Syndrome, Pediatrics, Perinatology and Child Health, Female, Gene-Environment Interaction, Self Report, Neurology (clinical), Psychology, 030217 neurology & neurosurgery, Clinical psychology

Abstract

We examined the benefit of emotional support on daily health in premutation carrier mothers of adolescents and adults with fragile X syndrome (n = 114), and whether this benefit was moderated by the mother's genetic status (FMR1 CGG repeat length). In an 8-day daily diary, maternal daily health was assessed subjectively through self-reported number of physical health symptoms and physiologically via cortisol awakening response. Multilevel lagged-day models indicated that premutation carrier mothers with midrange CGG repeats derived less health benefit from a day with high positive emotional support than those with lower or higher numbers of repeats within the premutation range. The data support the influence of both genetic and environmental influences on the health of this population.

Published

2019

46. Association between the FMR1 CGG repeat lengths and the severity of idiopathic primary ovarian insufficiency: a meta analysis

Author

Ying Liu, Wenxiang Zhang, Jing Huang, Yingchun Liu, Jing Wang, and Hong Jiang

Subjects

Oncology, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Primary ovarian insufficiency, Biomedical Engineering, Pharmaceutical Science, Medicine (miscellaneous), Diminished ovarian reserve, macromolecular substances, 02 engineering and technology, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, business.industry, General Medicine, 021001 nanoscience & nanotechnology, FMR1, nervous system diseases, Fmr1 gene, Cgg repeat, 030220 oncology & carcinogenesis, Meta-analysis, 0210 nano-technology, business, Biotechnology

Abstract

Aim: Reports on the association of the CGG repeat length in the FMR1 gene with the severity of idiopathic POI are inconclusive. Therefore, a meta analysis was performed to investigate the r...

Published

2019

47. Expansions and contractions of the FMR1 CGG repeat in 5,508 transmissions of normal, intermediate, and premutation alleles

Author

Emily G. Allen, Stephanie L. Sherman, Gary J. Latham, James N. Macpherson, Andrew Hadd, Nicole Tortora, Carl Dobkin, Anne Glicksman, Angela Maria Vianna-Morgante, Sarah L. Nolin, and Montserrat Milà

Subjects

Male, 0301 basic medicine, Fragile x, Inheritance Patterns, fragile X, Gene Expression, 030105 genetics & heredity, Biology, Fragile X Mental Retardation Protein, 03 medical and health sciences, Gene Frequency, trinucleotide repeat instability, Genetics, Humans, Allele, FMR1, Alleles, Genetics (clinical), MUTAÇÃO GENÉTICA, Original Articles, Pedigree, 030104 developmental biology, Cgg repeat, Fragile X Syndrome, Original Article, Female, Trinucleotide Repeat Expansion, Premutation allele

Abstract

Instability of the FMR1 repeat, commonly observed in transmissions of premutation alleles (55–200 repeats), is influenced by the size of the repeat, its internal structure and the sex of the transmitting parent. We assessed these three factors in unstable transmissions of 14/3,335 normal (~5 to 44 repeats), 54/293 intermediate (45–54 repeats), and 1561/1,880 premutation alleles. While most unstable transmissions led to expansions, contractions to smaller repeats were observed in all size classes. For normal alleles, instability was more frequent in paternal transmissions and in alleles with long 3′ uninterrupted repeat lengths. For premutation alleles, contractions also occurred more often in paternal than maternal transmissions and the frequency of paternal contractions increased linearly with repeat size. All paternal premutation allele contractions were transmitted as premutation alleles, but maternal premutation allele contractions were transmitted as premutation, intermediate, or normal alleles. The eight losses of AGG interruptions in the FMR1 repeat occurred exclusively in contractions of maternal premutation alleles. We propose a refined model of FMR1 repeat progression from normal to premutation size and suggest that most normal alleles without AGG interruptions are derived from contractions of maternal premutation alleles.

Published

2019

48. The prevalence of CGG repeat expansion mutation in FMR1 gene in the northern Chinese women of reproductive age

Author

Guifeng Ding, Xiuli Yang, Xiaomei Wang, Liying Zou, Songtao Wang, Yinan Ma, Junqi Ma, Fengying Wang, Hong Pan, Xiaowei Liu, Hua Yang, Kefang Wang, Xiaolin Qiao, Sai-Nan Zhu, Chenghong Yin, Xiuhua Ma, Yu Qi, Xiaorong Wang, Yue Yang, Xin Wang, Lifang Sun, Xing Wei, and Dandan Liu

Subjects

0301 basic medicine, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, China, lcsh:Internal medicine, Adolescent, lcsh:QH426-470, Genetic counseling, Prenatal diagnosis, 030105 genetics & heredity, Abortion, Cohort Studies, Fragile X Mental Retardation Protein, Young Adult, 03 medical and health sciences, FMR1 gene, Trinucleotide Repeats, Pregnancy, Genetics, medicine, Humans, Allele, lcsh:RC31-1245, reproductive and urinary physiology, Genetics (clinical), Obstetrics, business.industry, Reproduction, Pregnancy Outcome, FMR1, abortion, nervous system diseases, Fmr1 gene, lcsh:Genetics, 030104 developmental biology, Cgg repeat, Mutation, embryonic structures, Mutation (genetic algorithm), Female, Pre-mutation, business, Research Article, Fragile X syndrome

Abstract

Background The prevalence of CGG repeat expansion mutation in FMR1 gene varies among different populations. In this study, we investigated the prevalence of this mutation in women of reproductive age from northern China. Methods A total of 11,891 pre-conceptional or pregnant women, including 5037 pregnant women and 7357 women with the history of spontaneous abortion or induced abortion due to delayed growth of the embryos, were recruited. The number of CGG repeats in FMR1 was measured by the TRP-PCR method. We also offered genetic counseling and prenatal diagnosis to the women carrying pre-mutation or full mutation alleles. Results The prevalence of pre-mutation in reproductive women in northern China was 1/410, higher than that in southern China and Korea but lower than that in western countries. We also found that the prevalence of pre-mutation was relatively high (1/320) in women with abortion history. Conclusion Screening for CGG repeat expansion mutation in FMR1 should be recommended to the women with the history of spontaneous abortion or induced abortion due to delayed growth of the embryos.

Published

2019

49. Expansion of 5’ UTR CGG repeat in RILPL1 is associated with oculopharyngodistal myopathy

Author

Xinzhuang Yang, Yang Wang, Yi-Cheng Zhu, Chao Ling, Haitao Ren, Liying Cui, Ding-Ding Zhang, Jianxiong Shen, Jing-Wen Niu, Pidong Li, Dan Xu, Yanhuan Zhao, Xueyu Guo, Zhen Wang, Lin Chen, Yi Dai, and Depeng Wang

Subjects

Weakness, Five prime untranslated region, Ptosis, Cgg repeat, business.industry, medicine, Etiology, Methylation, medicine.symptom, Bioinformatics, Trinucleotide repeat expansion, business, Gene

Abstract

Oculopharyngodistal myopathy is an adult-onset degenerative muscle disorder characterized by ptosis, ophthalmoplegia and weakness of the facial, pharyngeal and limb muscles. Trinucleotide repeat expansions in non-coding regions of LRP12, G1PC1and NOTCH2NLC were recently reported to be the etiologies for OPDM. However, a significant portion of OPDM patients still have unknown genetic causes. In this study, we performed long-read whole-genome sequencing in a large five-generation family of 156 individuals, including 22 patients diagnosed with typical OPDM and identified CGG repeat expansions in RILPL1 gene in all patients we tested while not in unaffected family members. Methylation analysis indicated that methylation levels of the RILPL1 gene were unaltered in OPDM patients, which was in consistent with previous reports. Our findings first provided evidences that RILPL1 were associated OPDM which we suggested as OPDM type 4.

Published

2021

50. Relationships between Mitochondrial Function, AMPK, and TORC1 Signaling in Lymphoblasts with Premutation Alleles of the FMR1 Gene

Author

Paul R. Fisher, Kevin Ngoie, Bruce E. Kemp, Anna Atkinson, Elsdon Storey, Danuta Z. Loesch, Oana Sanislav, Claire Y. Allan, and Sarah J. Annesley

Subjects

Male, AMPK, Mitochondrion, AMP-Activated Protein Kinases, Fragile X Mental Retardation Protein, TOR complex I, Lymphocytes, Biology (General), FMR1, Spectroscopy, Lymphoblast, General Medicine, Cell biology, Computer Science Applications, Mitochondria, Fragile X syndrome, Chemistry, Signalling, Female, medicine.symptom, Signal Transduction, medicine.medical_specialty, Ataxia, QH301-705.5, Biology, Mechanistic Target of Rapamycin Complex 1, Catalysis, Article, Inorganic Chemistry, Mitochondrial Proteins, Internal medicine, medicine, Humans, Physical and Theoretical Chemistry, Allele, Protein kinase A, QD1-999, Molecular Biology, Alleles, molecular_biology, Organic Chemistry, medicine.disease, Fmr1 gene, Endocrinology, CGG repeat, Fragile X Syndrome, fragile X-associated tremor/ataxia syndrome (FXTAS), Trinucleotide repeat expansion, Trinucleotide Repeat Expansion, Function (biology)

Abstract

The X-linked FMR1 gene contains a non-coding trinucleotide repeat in its 5’ region that, in normal, healthy individuals contains 20–44 copies. Large expansions of this region (&gt, 200 copies) cause fragile X syndrome (FXS), but expansions of 55–199 copies (referred to as premutation alleles) predispose carriers to a neurodegenerative disease called fragile X-associated tremor/ataxia syndrome (FXTAS). The cytopathological mechanisms underlying FXTAS are poorly understood, but abnormalities in mitochondrial function are believed to play a role. We previously reported that lymphoblastoid cell lines (LCLs, or lymphoblasts) of premutation carriers have elevated mitochondrial respiratory activities. In the carriers, especially those not clinically affected with FXTAS, AMP-activated protein kinase (AMPK) activity was shown to be elevated. In the FXTAS patients, however, it was negatively correlated with brain white matter lesions, suggesting a protective role in the molecular mechanisms. Here, we report an enlarged and extended study of mitochondrial function and associated cellular stress-signaling pathways in lymphoblasts isolated from male and female premutation carriers, regardless of their clinical status, and healthy controls. The results confirmed the elevation of AMPK and mitochondrial respiratory activities and reduction in reactive O2 species (ROS) levels in premutation cells and revealed for the first time that target of rapamycin complex I (TORC1) activities are reduced. Extensive correlation, multiple regression, and principal components analysis revealed the best fitting statistical explanations of these changes in terms of the other variables measured. These suggested which variables might be the most “proximal” regulators of the others in the extensive network of known causal interactions amongst the measured parameters of mitochondrial function and cellular stress signaling. In the resulting model, the premutation alleles activate AMPK and inhibit both TORC1 and ROS production, the reduced TORC1 activity contributes to activation of AMPK and of nonmitochondrial metabolism, and the higher AMPK activity results in elevated catabolic metabolism, mitochondrial respiration, and ATP steady state levels. In addition, the results suggest a separate CGG repeat number-dependent elevation of TORC1 activity that is insufficient to overcome the inhibition of TORC1 in premutation cells but may presage the previously reported activation of TORC1 in FXS cells.

Published

2021