Your search keyword '"NEUROLOGICAL disorders -- Genetic aspects"' showing total 356 results

1. Lessons and pitfalls of whole genome sequencing.

Author

Record, Christopher J. and Reilly, Mary M.

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *INTRAVENOUS immunoglobulins, *ATAXIA, *NEUROLOGICAL disorders, *GENETIC variation, *GENES, *BIOINFORMATICS, *MUSCULAR atrophy, *DEMYELINATION, *GENETIC testing, *SEQUENCE analysis, *SINGLE nucleotide polymorphisms, *CHARCOT-Marie-Tooth disease

Abstract

Whole-genome sequencing (WGS) has recently become the first-line genetic investigation for many suspected genetic neurological disorders. While its diagnostic capabilities are innumerable, as with any test, it has its limitations. Clinicians should be aware of where WGS is extremely reliable (detecting singlenucleotide variants), where its reliability is much improved (detecting copy number variants and small repeat expansions) and where it may miss/misinterpret a variant (large repeat expansions, balanced structural variants or low heteroplasmy mitochondrial DNA variants). Bioinformatic technology and virtual gene panels are constantly evolving, and it is important to know what genes and what types of variant are being tested; the current National Health Service Genomic Medicine Service WGS offers more than early iterations of the 100 000 Genomes Project analysis. Close communication between clinician and laboratory, ideally through a multidisciplinary team meeting, is encouraged where there is diagnostic uncertainty. [ABSTRACT FROM AUTHOR]

Published

2024

2. Generalized Stiffness in Hereditary Hyperekplexia Responsive to Trihexyphenidyl: A Novel Finding.

Author

Rudrabhatla, Pavan Kumar, Divya, K. P., Fasaludeen, Alfiya, Menon, Ramshekhar N., Cherian, Ajith, Urulangodi, Madhusoodanan, and Sundaram, Soumya

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *CRYING, *PHYSICAL diagnosis, *NEUROLOGIC examination, *PIPERIDINE, *RARE diseases, *APNEA, *ELECTROENCEPHALOGRAPHY, *NEUROLOGICAL disorders, *GENETIC variation, *STARTLE reaction, *GENETIC mutation, *MUSCARINIC antagonists, *CLONAZEPAM, *CYANOSIS, *SEQUENCE analysis

Abstract

The article focuses on hereditary hyperekplexia (HPX), a rare disorder characterized by exaggerated startle response and generalized muscle stiffness, often presenting in infancy. It discusses the standard treatment with clonazepam and explores the novel use of trihexyphenidyl to alleviate persistent generalized stiffness episodes in patients unresponsive to clonazepam.

Published

2024

3. Hospitalisation and mortality among privately insured individuals with COVID-19 in the United States: The role of intellectual disabilities and Neurogenetic disorders.

Author

Davis, A., Copeland-Linder, N., Phuong, K., Belcher, H., and Eck, K. van

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *CROSS-sectional method, *HEALTH services accessibility, *RESEARCH funding, *HOSPITAL care, *HEALTH insurance, *PRIVATE sector, *RETROSPECTIVE studies, *DESCRIPTIVE statistics, *INTELLECTUAL disabilities, *ODDS ratio, *MEDICAL records, *ACQUISITION of data, *SOCIODEMOGRAPHIC factors, *CONFIDENCE intervals, *COVID-19, *COMORBIDITY, *MEDICAL care costs, *DISEASE complications, MORTALITY risk factors

Abstract

Background Individuals with intellectual disabilities (IDs) and neurogenetic conditions (IDNDs) are at greater risk for comorbidities that may increase adverse outcomes for this population when they have coronavirus disease 2019 (COVID-19). The study aims are to examine the population-level odds of hospitalisation and mortality of privately insured individuals with COVID-19 with and without IDNDs IDs, controlling for sociodemographics and comorbid health conditions. Methods This is a retrospective, cross-sectional study of 1174 individuals with IDs and neurogenetic conditions within a population of 752 237 de-identified, privately insured, US patients diagnosed with COVID-19 between February 2020 and September 2020. Odds of hospitalisation and mortality among COVID-19 patients with IDNDs adjusted for demographic characteristics, Health Resources and Services Administration region, states with Affordable Care Act and number of comorbid health conditions were analysed. Results Patients with IDNDs overall had higher rates of COVID-19 hospitalisation than those without IDNDs (35.01% vs. 12.65%, P< .0001) and had higher rates of COVID-19 mortality than those without IDNDs (4.94% vs. .88%, P < .0001). Adjusting for sociodemographic factors only, the odds of being hospitalised for COVID-19 associated with IDNDs was 4.05 [95% confidence interval (CI) 3.56–4.61]. Adjusting for sociodemographic factors and comorbidity count, the odds of hospitalisation for COVID-19 associated with IDNDs was 1.42 (95% CI 1.25–1.61). The odds of mortality from COVID-19 for individuals with IDNDs adjusted for sociodemographic factors only was 4.65 (95% CI 3.47–6.24). The odds of mortality from COVID-19 for patients with IDNDs adjusted for sociodemographic factors and comorbidity count was 2.70 (95% CI 2.03–3.60). A major finding of the study was that even when considering the different demographic structure and generally higher disease burden of patients with IDNDs, having a IDND was an independent risk factor for increased hospitalisation and mortality compared with patients without IDNDs. Conclusions Individuals with IDNDs had significantly higher odds of hospitalisation and mortality after adjusting for sociodemographics. Results remained significant with a slight attenuation after adjusting for sociodemographics and comorbidities. Adjustments for comorbidity count demonstrated a dose–response increase in odds of both hospitalisation and mortality, illustrating the cumulative effect of health concerns on COVID-19 outcomes. Together, findings highlight that individuals with IDNDs experience vulnerability for negative COVID-19 health outcomes with implications for access to comprehensive healthcare. [ABSTRACT FROM AUTHOR]

Published

2024

4. Data-Driven Characterization of Genetic Variability in Disease Pathways and Pesticide-Induced Nervous System Disease in the United States Population.

Author

Kosnik, Marissa B., Antczak, Philipp, and Fantke, Peter

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *PEARSON correlation (Statistics), *ENVIRONMENTAL health, *DATA analysis, *ALZHEIMER'S disease, *MULTIPLE sclerosis, *RESEARCH funding, *POPULATION health, *FISHER exact test, *DESCRIPTIVE statistics, *PARKINSON'S disease, *DISEASE prevalence, *PESTICIDES, *NEUROLOGICAL disorders, *GENE expression profiling, *DISEASE susceptibility, *SINGLE nucleotide polymorphisms, *REGRESSION analysis, *DISEASE incidence

Abstract

BACKGROUND: Genetic susceptibility to chemicals is incompletely characterized. However, nervous system disease development following pesticide exposure can vary in a population, implying some individuals may have higher genetic susceptibility to pesticide-induced nervous system disease. OBJECTIVES: We aimed to build a computational approach to characterize single-nucleotide polymorphisms (SNPs) implicated in chemically induced adverse outcomes and used this framework to assess the link between differential population susceptibility to pesticides and human nervous system disease. METHODS: We integrated publicly available datasets of Chemical–Gene, Gene–Pathway, and SNP–Disease associations to build Chemical–Pathway– Gene–SNP–Disease linkages for humans. As a case study, we integrated these linkages with spatialized pesticide application data for the US from 1992 to 2018 and spatialized nervous system disease rates for 2018. Through this, we characterized SNPs that may be important in states with high disease occurrence based on the pesticides used there. RESULTS: We found that the number of SNP hits per pesticide in US states positively correlated with disease incidence and prevalence for Alzheimer’s disease, Parkinson disease, and multiple sclerosis. We performed frequent itemset mining to differentiate pesticides used over time in states with high and low disease occurrence and found that only 19% of pesticide sets overlapped between 10 states with high disease occurrence and 10 states with low disease occurrence rates, and more SNPs were implicated in pathways in high disease occurrence states. Through a crossvalidation of subsets of five high and low disease occurrence states, we characterized SNPs, genes, pathways, and pesticides more frequently implicated in high disease occurrence states. DISCUSSION: Our findings support that pesticides contribute to nervous system disease, and we developed priority lists of SNPs, pesticides, and pathways for further study. This data-driven approach can be adapted to other chemicals, diseases, and locations to characterize differential population susceptibility to chemical exposures. [ABSTRACT FROM AUTHOR]

Published

2024

5. Expanding the Phenotype of the CACNA1C-Associated Neurological Disorders in Children: Systematic Literature Review and Description of a Novel Mutation.

Author

Cipriano, Lorenzo, Piscopo, Raffaele, Aiello, Chiara, Novelli, Antonio, Iolascon, Achille, and Piscopo, Carmelo

Subjects

NEUROLOGICAL disorders -- Genetic aspects, CARDIOVASCULAR system abnormalities, TEETH abnormalities, MUSCULOSKELETAL system diseases, DESCRIPTIVE statistics, INTELLECTUAL disabilities, CALCIUM, GENETIC variation, SYSTEMATIC reviews, GENETIC mutation, GINGIVAL hyperplasia, PHENOTYPES, CHILDREN

Abstract

Background: CACNA1C gene encodes the alpha 1 subunit of the CaV1.2 L-type Ca2+ channel. Pathogenic variants in this gene have been associated with cardiac rhythm disorders such as long QT syndrome, Brugada syndrome and Timothy syndrome. Recent evidence has suggested the possible association between CACNA1C mutations and neurologically-isolated (in absence of cardiac involvement) phenotypes in children, giving birth to a wider spectrum of CACNA1C-related clinical presentations. However, to date, little is known about the variety of both neurological and non-neurological signs/symptoms in the neurologically-predominant phenotypes. Methods and Results: We conducted a systematic review of neurologically-predominant presentations without cardiac conduction defects, associated with CACNA1C mutations. We also reported a novel de novo missense pathogenic variant in the CACNA1C gene of a children patient presenting with constructional, dressing and oro-buccal apraxia associated with behavioral abnormalities, mild intellectual disability, dental anomalies, gingival hyperplasia and mild musculoskeletal defects, without cardiac conduction defects. Conclusions: The present study highlights the importance of considering the investigation of the CACNA1C gene in children's neurological isolated syndromes, and expands the phenotype of the CACNA1C related conditions. In addition, the present study highlights that, even in absence of cardiac conduction defects, nuanced clinical manifestations of the Timothy syndrome (e.g., dental and gingival defects) could be found. These findings suggest the high variable expressivity of the CACNA1C gene and remark that the absence of cardiac involvement should not mislead the diagnosis of a CACNA1C related disorder. [ABSTRACT FROM AUTHOR]

Published

2024

6. The Base Hit: Neurological Diseases and Genetic Susceptibilities to Pesticide Exposures.

Author

Arnold, Carrie

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *ENVIRONMENTAL health, *SYNDROMES, *NEUROTOXICOLOGY, *TOXICOLOGY, *GENETIC markers, *NEURODEGENERATION, *NEUROLOGICAL disorders, *PESTICIDES, *ENVIRONMENTAL exposure, *DISEASE susceptibility

Abstract

The article discusses a study published in the issue which explored a computational approach to connect pesticide exposures with generic variants associated with Alzheimer's disease (AD), Parkinson's disease (PD), and multiple sclerosis (MS). Topics include importance of understanding genetic susceptibility to pesticides, the reliance of traditional methods of assessing gene-environment interactions on large longitudinal studies, and strength of the study.

Published

2024

7. Noncanonical splice‐site variant in peripheral myelin protein 22 gene (PMP22) in a patient with hereditary neuropathy with liability to pressure palsies.

Author

Kawamoto, Norifumi, Hamada, Yuichi, Kobayashi, Shunsuke, Naruse, Hiroya, Ishiura, Hiroyuki, Matsukawa, Takashi, Mitsui, Jun, Tsuji, Shoji, Sonoo, Masahiro, and Toda, Tatsushi

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *PROTEIN metabolism, *IN vitro studies, *CHROMOSOMES, *PERIPHERAL neuropathy, *ENTRAPMENT neuropathies, *NERVE conduction studies, *SEQUENCE analysis, *GENETIC variation, *FAMILIAL spastic paraplegia, *MUSCLE weakness, *T-test (Statistics), *GENETIC carriers, *CHARCOT-Marie-Tooth disease, *FOOT, *NUMBNESS, *GENETIC markers, *TIBIA, *POLYMERASE chain reaction

Abstract

Aim: Hereditary neuropathy with liability to pressure palsies (HNPP) is a peripheral neuropathy with autosomal dominant inheritance. Diagnosis can be made from the characteristic abnormalities determined by nerve conduction studies (NCS), including subclinical deficits at physiological compression sites. Heterozygous deletion of the chromosome 17p11.2–p12 region including the peripheral myelin protein 22 gene (PMP22) is the cause in the majority of cases. However, the loss of function of PMP22 due to frameshift‐causing insertion/deletion, missense, nonsense, or splice‐site disrupting variants cause HNPP in some patients. We report a case of a patient diagnosed with HNPP on the basis of clinical features and the results of NCS. No deletions of PMP22 were detected by fluorescence in situ hybridization. Methods: We performed direct nucleotide sequence analysis and identified a heterozygous variant, c.78 + 3G > T, in PMP22. Since this variant is located outside the canonical splice site at the exon 2–intron 2 junction, we investigated whether the variant causes aberrant splicing and leads to the skipping of exon 2 of PMP22 by in vitro minigene splicing assay. Results: We demonstrated that the c.78 + 3G > T variant causes the skipping of exon 2 and leads to loss of function of the mutant allele. Conclusion: Searching for sequence variants located outside the canonical splice sites should also be considered even when deletion of PMP22 is not found in a patient with a clinical diagnosis suggesting HNPP. [ABSTRACT FROM AUTHOR]

Published

2023

8. Common and disorder-specific cortical thickness alterations in internalizing, externalizing and thought disorders during early adolescence: an Adolescent Brain and Cognitive Development study.

Author

Yu, Gechang, Liu, Zhaowen, Wu, Xinran, Becker, Benjamin, Zhang, Kai, Fan, Huaxin, Peng, Songjun, Kuang, Nanyu, Kang, Jujiao, Dong, Guiying, Zhao, Xing-Ming, Schumann, Gunter, Feng, Jianfeng, Sahakian, Barbara J., Robbins, Trevor W., Palaniyappan, Lena, and Zhang, Jie

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *COGNITION, *CEREBRAL cortical thinning, *GENETIC variation, *BRAIN cortical thickness, *GENOME-wide association studies, *NEUROGLIA, *MENTAL illness, *NEURORADIOLOGY, *SOMATOSENSORY disorders, *AUDITORY cortex, *CHILDREN, *ADOLESCENCE

Abstract

Background: A growing body of neuroimaging studies has reported common neural abnormalities among mental disorders in adults. However, it is unclear whether the distinct disorder-specific mechanisms operate during adolescence despite the overlap among disorders. Methods: We studied a large cohort of more than 11 000 preadolescent (age 9–10 yr) children from the Adolescent Brain and Cognitive Development cohort. We adopted a regrouping approach to compare cortical thickness (CT) alterations and longitudinal changes between healthy controls (n = 4041) and externalizing (n = 1182), internalizing (n = 1959) and thought disorder (n = 347) groups. Genome-wide association study (GWAS) was performed on regional CT across 4468 unrelated European youth. Results: Youth with externalizing or internalizing disorders exhibited increased regional CT compared with controls. Externalizing (p = 8 × 10−4, Cohen d = 0.10) and internalizing disorders (p = 2 × 10−3, Cohen d = 0.08) shared thicker CT in the left pars opercularis. The somatosensory and the primary auditory cortex were uniquely affected in externalizing disorders, whereas the primary motor cortex and higher-order visual association areas were uniquely affected in internalizing disorders. Only youth with externalizing disorders showed decelerated cortical thinning from age 10–12 years. The GWAS found 59 genome-wide significant associated genetic variants across these regions. Cortical thickness in common regions was associated with glutamatergic neurons, while internalizing-specific regional CT was associated with astrocytes, oligodendrocyte progenitor cells and GABAergic neurons. Limitations: The sample size of the GWAS was relatively small. Conclusion: Our study provides strong evidence for the presence of specificity in CT, developmental trajectories and underlying genetic underpinnings among externalizing and internalizing disorders during early adolescence. Our results support the neurobiological validity of the regrouping approach that could supplement the use of a dimensional approach in future clinical practice. [ABSTRACT FROM AUTHOR]

Published

2023

9. Functional Gait Disorders: Clinical presentations, Phenotypes and Implications for treatment.

Author

Issak, Sara, Kanaan, Richard, Nielsen, Glenn, Fini, Natalie A., and Williams, Gavin

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *DIAGNOSIS of neurological disorders, *NEUROLOGICAL disorders, *MOVEMENT disorders, *GAIT disorders, *HEALTH care teams, *PHENOTYPES, *SYMPTOMS

Abstract

Functional Gait Disorders (FGD) are a common presentation of motor-Functional Neurological Disorders (motor-FND) that affect walking ability. To provide a narrative review of the current literature on FGD. A narrative overview of published literature was undertaken, based on a systematic search of relevant databases, authoritative texts and citation tracking. FGD is multidimensional and disabling, with numerous phenotypes described in the literature, including 'knee buckling,' 'astasia-abasia' and 'excessive slowness.' Motor symptoms such as weakness or tremor, and non-motor symptoms, such as pain and fatigue may contribute to the disability and distress in FGD. Phenotypic features and clinical signs are seen in FGD that demonstrate inconsistency and incongruity with structural disease. A limited number of treatment studies have specifically focussed on FGD, however, reporting of outcomes from motor-FND cohorts has demonstrated short and long-term improvements in walking ability through multidisciplinary rehabilitation. The relative contribution of motor and non-motor symptoms in FGD remains unknown, but it is likely that non-motor symptoms increase the illness burden and should be considered during assessment and treatment. Recommended treatment for FGD involves multidisciplinary rehabilitation, but optimum treatment elements are yet to be determined. [ABSTRACT FROM AUTHOR]

Published

2023

10. Genomic Medicine in Neurology.

Author

Menon, Kriti, Agarwal, Divya, Chaudhari, Dinesh, and Renjen, Pushpendra Nath

Subjects

NEUROLOGICAL disorders -- Genetic aspects, NEUROLOGICAL disorder prevention, NEUROLOGY, NEUROLOGICAL disorders, SEQUENCE analysis, TERTIARY care, GENETIC testing, RETROSPECTIVE studies, GENOMICS, SYMPTOMS, DESCRIPTIVE statistics, DISEASE management, FAMILY history (Medicine)

Abstract

Introduction: Approximately 80% of genes actively expresses in the brain cells and about 40% of known genetic disorders affect the central nervous system. The advances in the field of genetics and genomics have solved the problem of the diagnostic odyssey in neurological genetic diseases to great extent. The molecular genetic technology has helped in understanding the association of various genetic factors with neurological disorders, filling the gaps in genomic medicine and has led to discovery of novel diseases and their causative genes and helps in providing a multidisciplinary care to the patient and the family. Methods: We have retrospectively evaluated the utility of genetic testing, acceptance of presymptomatic testing, and scope of prevention and management of adult-onset neurological condition in 15 patients from unrelated families, who underwent a minimum of one genetic test to evaluate the genetic basis of their clinical manifestation and/or a positive family history. Results: All of the 15 patients underwent atleast one genetic test. Exome sequencing was the most commonly used molecular test. Definitive diagnoses were obtained for 9/15 families which indicated the diagnostic yield of genetic testing to be around 60% in this patient cohort. A negative or inclusive result was obtained for 6/15 patients with no further genetic testing done. Presymptomatic genetic testing was offered to the extended family members of four families, but none of the family members opted for the same. Prenatal/preimplantation genetic testing options were provided to three families based on the definitive diagnosis obtained from the genetic testing result. [ABSTRACT FROM AUTHOR]

Published

2023

11. Sulfonylurea for improving neurological features in neonatal diabetes: A systematic review and meta‐analyses.

Author

de Gouveia Buff Passone, Caroline, Giani, Elisa, Vaivre‐Douret, Laurence, Kariyawasam, Dulanjalee, Berdugo, Marianne, Garcin, Laure, Beltrand, Jacques, Bernardo, Wanderley Marques, and Polak, Michel

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *NEUROLOGICAL disorder prevention, *NEUROPHYSIOLOGY, *META-analysis, *NEUROLOGICAL disorders, *GENETIC mutation, *INFANT development, *SYSTEMATIC reviews, *EPILEPSY, *MUSCLE tone, *DIABETES, *SULFONYLUREAS, *COGNITION, *PSYCHOLOGY of movement, *ATTENTION-deficit hyperactivity disorder, *ATTENTION, *DESCRIPTIVE statistics, *DATA analysis software, *MOTOR ability, *DISEASE risk factors, *SYMPTOMS, *CHILDREN

Abstract

Objective: In monogenic diabetes due to KCNJ11 and ABCC8 mutations that impair KATP‐ channel function, sulfonylureas improve long‐term glycemic control. Although KATP channels are extensively expressed in the brain, the effect of sulfonylureas on neurological function has varied widely. We evaluated published evidence about potential effects of sulfonylureas on neurological features, especially epilepsy, cognition, motor function and muscular tone, visuo‐motor integration, and attention deficits in children and adults with KCNJ11 and ABCC8‐related neonatal‐onset diabetes mellitus. Research Design and Methods: We conducted a systematic review and meta‐analyses of the literature (PROSPERO, CRD42021254782), including individual‐patient data, according to PRISMA, using RevMan software. We also graded the level of evidence. Results: We selected 34 of 776 publications. The evaluation of global neurological function before and after sulfonylurea (glibenclamide) treatment in 114 patients yielded a risk difference (RD) of 58% (95%CI, 43%–74%; I2 = 54%) overall and 73% (95%CI, 32%–113%; I2 = 0%) in the subgroup younger than 4 years; the level of evidence was moderate and high, respectively. EEG studies of epilepsy showed a RD of 56% (95%CI, 23%–89%; I2 = 34%) in patients with KCNJ11 mutations, with a high quality of evidence. For hypotonia and motor function, the RDs were 90% (95%CI, 69%–111%; I2 = 0%) and 73% (95%CI, 35%–111%; I2 = 0%), respectively, with a high level of evidence. Conclusions: Glibenclamide significantly improved neurological abnormalities in patients with neonatal‐onset diabetes due to KCNJ11 or ABCC8 mutations. Hypotonia was the symptom that responded best. Earlier treatment initiation was associated with greater benefits. [ABSTRACT FROM AUTHOR]

Published

2022

12. Editors' commentary.

Author

Smith, Phil E. M. and Fuller, Geraint N.

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *SERIAL publications, *GENOME-wide association studies, *MAGNETIC resonance imaging, *REFLECTION (Philosophy), *NEUROLOGICAL disorders, *SEQUENCE analysis

Published

2024

13. Hereditary neuropathy with liability to pressure palsies (HNPP): Intrafamilial phenotypic variability and early childhood refusal to walk as the presenting symptom.

Author

Karklinsky, Shani, Kugler, Shir, Bar-Yosef, Omer, Nissenkorn, Andreea, Grossman-Jonish, Anat, Tirosh, Irit, Vivante, Asaf, and Pode-Shakked, Ben

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *DEMYELINATION, *GENETIC disorders, *PARESTHESIA, *DIFFERENTIAL diagnosis, *MICROARRAY technology, *COMORBIDITY, *PHENOTYPES

Abstract

Background: Limping and/or refusal to walk is a common complaint in the setting of the pediatric department, with a widely diverse differential diagnosis. An unusual etiology, is that of a hereditary neuropathy. Hereditary neuropathy with liability to pressure palsies (HNPP) is a recurrent, episodic demyelinating neuropathy, most commonly caused by a 17p11.2 chromosomal deletion encompassing the PMP22 gene. Methods: We pursued chromosomal microarray analysis (CMA) in multiple affected individuals of a single extended family, manifesting a range of phenotypic features consistent with HNPP. Results: A 4.5 years-old boy presented for in-patient evaluation due to refusal to walk. Initial investigations including spine MRI and bone scan failed to yield a conclusive diagnosis. Following family history, which implied an autosomal dominant mode of inheritance, CMA was pursued and confirmed a 17p11.2 deletion in the proband consistent with HNPP. Importantly, following this diagnosis, four additional affected family members were demonstrated to harbor the deletion. Their variable phenotypic features, ranging from a prenatal diagnosis of a 6 months-old sibling, to recurrent paresthesias manifesting in the fourth decade of life, are discussed. Conclusions: Our experience with the family reported herein demonstrates how a thorough anamnesis can lead to a rare genetic etiology with a favorable prognosis and prevent unnecessary investigations, and underscores HNPP as an uncommon diagnostic possibility in the limping child. [ABSTRACT FROM AUTHOR]

Published

2022

14. Understanding What You Have Found: A Family With a Mutation in the LAMA1 Gene With Literature Review.

Author

Elmas, Muhsin, Gogus, Basak, and Solak, Mustafa

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *BRAIN diseases, *CEREBELLAR ataxia, *CEREBELLUM diseases, *GAIT disorders, *GENETIC mutation

Abstract

Introduction: Cerebellar dysplasia with cysts (CDC) is an imaging finding which is typically seen with in individuals with dystroglycanopathy. One of the diseases causing this condition is "Poretti-Boltshauser Syndrome; PTBHS" (OMIM #615960). Homozygous or compound heterozygous mutations in the LAMA1 gene cause this disease. Case presentation: 7 years old twin siblings consulted to the medical genetics department because of walking problems and cerebellar examination findings. Management and Outcome: Clinical and radiological findings of the patient suggested a syndrome with recessive inheritance. Whole exome sequencing (WES) test was performed for definitive diagnosis. As a result of the patient's WES analysis, a homozygous mutation was detected in the LAMA1 gene. Discussion: When determining the inheritance pattern of genetic diseases, if parents have consanquinity, this situation leads us to recessive inheritance diseases. Even if we are not consanquinity, but they say the same village, it is necessary to pay attention to the diseases of the recessive group. Whole exome sequencing analysis results in large amount of data generation. A good clinical evaluation is required to detect the mutation as a result of large data. To understand what we have found, we need to know what we are looking for. [ABSTRACT FROM AUTHOR]

Published

2020

15. Maternal polycystic ovary syndrome and risk of neuropsychiatric disorders in offspring: prenatal androgen exposure or genetic confounding?

Author

Cesta, Carolyn E., Öberg, Anna S., Ibrahimson, Abraham, Yusuf, Ikram, Larsson, Henrik, Almqvist, Catarina, D'Onofrio, Brian M., Bulik, Cynthia M., Fernández de la Cruz, Lorena, Mataix-Cols, David, Landén, Mikael, and Rosenqvist, Mina A.

Subjects

*GENETICS of autism, *NEUROLOGICAL disorders -- Genetic aspects, *RISK factors of attention-deficit hyperactivity disorder, *AUTISM risk factors, *ANDROGENS, *ATTENTION-deficit hyperactivity disorder, *CHRONIC diseases, *CONFIDENCE intervals, *LONGITUDINAL method, *NEUROLOGICAL disorders, *PREGNANCY complications, *PSYCHOSES, *REGRESSION analysis, *RISK assessment, *SEX distribution, *POLYCYSTIC ovary syndrome, *TIC disorders, *TOURETTE syndrome, *PROPORTIONAL hazards models, *PRENATAL exposure delayed effects, *ODDS ratio, *DISEASE complications, *DISEASE risk factors

Abstract

Background: Maternal polycystic ovary syndrome (PCOS) has been proposed as a model for investigating the role of prenatal androgen exposure in the development of neuropsychiatric disorders. However, women with PCOS are at higher risk of developing psychiatric conditions and previous studies are likely confounded by genetic influences. Methods: A Swedish nationwide register-based cohort study was conducted to disentangle the influence of prenatal androgen exposure from familial confounding in the association between maternal PCOS and offspring attention-deficit/hyperactivity disorder (ADHD), autism spectrum disorders (ASD), and Tourette's disorder and chronic tic disorders (TD/CTD). PCOS-exposed offspring (n = 21 280) were compared with unrelated PCOS-unexposed offspring (n = 200 816) and PCOS-unexposed cousins (n = 17 295). Associations were estimated with stratified Cox regression models. Results: PCOS-exposed offspring had increased risk of being diagnosed with ADHD, ASD, and TD/CTD compared with unrelated PCOS-unexposed offspring. Associations were stronger in girls for ADHD and ASD but not TD/CTD [ADHD: adjusted hazard ratio (aHR) = 1.61 (95% confidence interval (CI) 1.31–1.99), ASD: aHR = 2.02 (95% CI 1.45–2.82)] than boys [ADHD: aHR = 1.37 (95% CI 1.19–1.57), ASD: aHR = 1.46 (95% CI 1.21–1.76)]. For ADHD and ASD, aHRs for girls were stronger when compared with PCOS-unexposed cousins, but slightly attenuated for boys. Conclusions: Estimates were similar when accounting for familial confounding (i.e. genetics and environmental factors shared by cousins) and stronger in girls for ADHD and ASD, potentially indicating a differential influence of prenatal androgen exposure v. genetic factors. These results strengthen evidence for a potential causal influence of prenatal androgen exposure on the development of male-predominant neuropsychiatric disorders in female offspring of women with PCOS. [ABSTRACT FROM AUTHOR]

Published

2020

16. Mitochondrial Disorders of the Nervous System: A Review.

Author

Set, Kallol K., Sen, Kuntal, Huq, A. H. M., and Agarwal, Rajkumar

Subjects

*DIAGNOSIS of neurological disorders, *NEUROLOGICAL disorders -- Genetic aspects, *ADENOSINE triphosphate, *DNA, *MITOCHONDRIAL pathology, *ELECTRON transport, *GENETIC counseling, *GENETIC mutation, *NEUROLOGICAL disorders, *NEURORADIOLOGY, *NEURAL conduction, *PHOSPHORYLATION, *QUALITY of life, *GENETIC testing, *TRICARBOXYLIC acids, *DIAGNOSIS, *GENETICS, *THERAPEUTICS

Abstract

The article discusses the basic concepts of mitochondrial function, genetics, and clinical features of the nervous system. The article also provides an overview of diagnosis and treatment of mitochondrial disorders affecting the nervous system. The dilemma of diagnosing a mitochondrial disease can present with any symptom in any organ at any age. It is noted that referral should be made to a neurologist and a geneticist with experience in mitochondrial diseases.

Published

2019

17. Rare variants in the neuronal ceroid lipofuscinosis gene MFSD8 are candidate risk factors for frontotemporal dementia.

Author

Geier, Ethan G., Bourdenx, Mathieu, Storm, Nadia J., Cochran, J. Nicholas, Sirkis, Daniel W., Hwang, Ji-Hye, Bonham, Luke W., Ramos, Eliana Marisa, Diaz, Antonio, Van Berlo, Victoria, Dokuru, Deepika, Nana, Alissa L., Karydas, Anna, Balestra, Maureen E., Huang, Yadong, Russo, Silvia P., Spina, Salvatore, Grinberg, Lea T., Seeley, William W., and Myers, Richard M.

Subjects

*NEURONAL ceroid-lipofuscinosis, *NEUROLOGICAL disorders -- Genetic aspects, *FRONTOTEMPORAL dementia

Abstract

Pathogenic variation in MAPT, GRN, and C9ORF72 accounts for at most only half of frontotemporal lobar degeneration (FTLD) cases with a family history of neurological disease. This suggests additional variants and genes that remain to be identified as risk factors for FTLD. We conducted a case-control genetic association study comparing pathologically diagnosed FTLD patients (n = 94) to cognitively normal older adults (n = 3541), and found suggestive evidence that gene-wide aggregate rare variant burden in MFSD8 is associated with FTLD risk. Because homozygous mutations in MFSD8 cause neuronal ceroid lipofuscinosis (NCL), similar to homozygous mutations in GRN, we assessed rare variants in MFSD8 for relevance to FTLD through experimental follow-up studies. Using post-mortem tissue from middle frontal gyrus of patients with FTLD and controls, we identified increased MFSD8 protein levels in MFSD8 rare variant carriers relative to non-variant carrier patients with sporadic FTLD and healthy controls. We also observed an increase in lysosomal and autophagy-related proteins in MFSD8 rare variant carrier and sporadic FTLD patients relative to controls. Immunohistochemical analysis revealed that MFSD8 was expressed in neurons and astrocytes across subjects, without clear evidence of abnormal localization in patients. Finally, in vitro studies identified marked disruption of lysosomal function in cells from MFSD8 rare variant carriers, and identified one rare variant that significantly increased the cell surface levels of MFSD8. Considering the growing evidence for altered autophagy in the pathogenesis of neurodegenerative disorders, our findings support a role of NCL genes in FTLD risk and suggest that MFSD8-associated lysosomal dysfunction may contribute to FTLD pathology. [ABSTRACT FROM AUTHOR]

Published

2019

18. Rare Variants in Tissue Inhibitor of Metalloproteinase 2 as a Risk Factor for Schizophrenia: Evidence From Familial and Cohort Analysis.

Author

John, Jibin, Sharma, Aditya, Kukshal, Prachi, Bhatia, Triptish, Nimgaonkar, Vishwajit L, Deshpande, Smita N, and Thelma, B K

Subjects

SCHIZOPHRENIA risk factors, DIAGNOSIS of schizophrenia, GENETICS of schizophrenia, NEUROLOGICAL disorders -- Genetic aspects, MENTAL illness genetics, COMPUTER simulation, BIOCHEMISTRY, SEQUENCE analysis, ANIMAL experimentation, PHENOMENOLOGICAL biology, GENETIC polymorphisms, TISSUE inhibitors of metalloproteinases, GENOMES, ODDS ratio, LONGITUDINAL method, MICE

Abstract

Candidate gene and genome-wide association study based common risk variant identification is being complemented by whole exome sequencing (WES)/whole genome sequencing based rare variant discovery in elucidation of genetic landscape of schizophrenia (SZ), a common neuropsychiatric disorder. WES findings of de novo mutations in case-parent trios have further implied genetic etiology, but do not explain the high genetic risk in general populations. Conversely, WES in multiplex families may be an insightful strategy for the identification of highly penetrant rare variants in SZ and possibly enhance our understanding of disease biology. In this study, we analyzed a 5-generation Indian family with multiple members affected with SZ by WES. We identified a rare heterozygous missense variant (NM_003255: c.506C>T; p.Pro169Leu; MAF = 0.0001) in Tissue Inhibitor of Metalloproteinase 2 (TIMP2, 17q25.3) segregating with all 6 affected individuals but not with unaffected members. Linkage analysis indicated a maximum logarithm of the odds score of 1.8, θ = 0 at this locus. The variant was predicted to be damaging by various in silico tools and also disrupt the structural integrity by molecular dynamics simulations. WES based screening of an independent SZ cohort (n = 370) identified 4 additional rare missense variants (p.Leu20Met, p.Ala26Ser, p.Lys48Arg and p. Ile217Leu) and a splice variant rs540397728 (NM_003255:c.232-5T>C), also predicted to be damaging, increasing the likelihood of contribution of this gene to SZ risk. Extensive biochemical and knockout mouse studies suggesting involvement of TIMP2 in neurodevelopmental and behavioral deficits, together with genetic evidence for TIMP2 conferring SZ risk from this study may have possible implications for new therapeutics. [ABSTRACT FROM AUTHOR]

Published

2019

19. Spastic paraplegia due to SPAST mutations is modified by the underlying mutation and sex.

Author

Parodi, Livia, Fenu, Silvia, Barbier, Mathieu, Banneau, Guillaume, Duyckaerts, Charles, Montcel, Sophie Tezenas du, Monin, Marie-Lorraine, Said, Samia Ait, Guegan, Justine, Tallaksen, Chantal M E, Tezenas du Montcel, Sophie, Ait Said, Samia, Sablonniere, Bertrand, Brice, Alexis, Stevanin, Giovanni, Depienne, Christel, Durr, Alexandra, and SPATAX network

Subjects

*FAMILIAL spastic paraplegia, *GENETIC mutation, *NEUROLOGICAL disorders -- Genetic aspects, *PHENOTYPES, *STATISTICAL correlation

Abstract

Hereditary spastic paraplegias (HSPs) are rare neurological disorders caused by progressive distal degeneration of the corticospinal tracts. Among the 79 loci and 65 spastic paraplegia genes (SPGs) involved in HSPs, mutations in SPAST, which encodes spastin, responsible for SPG4, are the most frequent cause of both familial and sporadic HSP. SPG4 is characterized by a clinically pure phenotype associated with restricted involvement of the corticospinal tracts and posterior columns of the spinal cord. It is rarely associated with additional neurological signs. However, both age of onset and severity of the disorder are extremely variable. Such variability is both intra- and inter-familial and may suggest incomplete penetrance, with some patients carrying mutations remaining asymptomatic for their entire life. We analysed a cohort of 842 patients with SPG4-HSP to assess genotype-phenotype correlations. Most patients were French (89%) and had a family history of SPG4-HSP (75%). Age at onset was characterized by a bimodal distribution, with high inter-familial and intra-familial variability, especially concerning first-degree relatives. Penetrance of the disorder was 0.9, complete after 70 years of age. Penetrance was lower in females (0.88 versus 0.94 in males, P = 0.01), despite a more diffuse phenotype with more frequent upper limb involvement. Seventy-seven per cent of pathogenic mutations (missense, frameshift, splice site, nonsense, and deletions) were located in the AAA cassette of spastin, impairing its microtubule-severing activity. A comparison of the missense and truncating mutations revealed a significantly lower age at onset for patients carrying missense mutations than those carrying truncating mutations, explaining the bimodal distribution of the age at onset. The age at onset for patients carrying missense mutations was often before 10 years, sometimes associated with intellectual deficiency. Neuropathological examination of a single case showed degeneration of the spinocerebellar and spinocortical tracts, as well as the posterior columns. However, there were numerous small-diameter processes among unusually large myelinated fibres in the corticospinal tract, suggesting marked regeneration. In conclusion, this large cohort of 842 individuals allowed us to identify a significantly younger age at onset in missense mutation carriers and lower penetrance in females, despite a more severe disorder. Neuropathology in one case showed numerous small fibres suggesting regeneration. [ABSTRACT FROM AUTHOR]

Published

2018

20. The expression of neurological soft signs in two African populations with first-episode schizophrenia.

Author

Ojagbemi, Akin, Chiliza, Bonginkosi, Bello, Toyin, Asmal, Laila, Esan, Oluyomi, Emsley, Robin, and Gureje, Oye

Subjects

*DIAGNOSIS of neurological disorders, *NEUROLOGICAL disorders -- Genetic aspects, *DIAGNOSIS of schizophrenia, *GENETICS of schizophrenia, *ANTIPSYCHOTIC agents, *BLACK people, *STATISTICAL correlation, *GENE expression, *PATHOLOGICAL psychology, *REGRESSION analysis, *SYMPTOMS, *SEVERITY of illness index

Abstract

Information about patterns of expression of neurological soft signs (NSS) in schizophrenia among individuals belonging to the same genetic ancestry may provide new insight for the understanding of the disease’s genetic functions. This study aimed to investigate whether patterns of NSS expression in first episode schizophrenia are comparable in populations with dissimilar genetic ancestry. A sample of 207 patients with first episode schizophrenia were examined using the Neurological Evaluation Scale before they were exposed to anti-psychotics. They were allocated to two African ancestry groups: Black (81 Yoruba Nigerians, and 18 Xhosa South Africans), and non-Black (98 Coloured, and 10 White South Africans). Assessments were carried out using validated measures of clinical characteristics of schizophrenia. We determined the frequency, severity, factor structure, and association of NSS with clinical characteristics. Factor derived categories were compared using the Pearson’s (r) and Tucker’s congruence methods. The associations between factor derived categories and clinical characteristics of schizophrenia were determined using Pearson’s correlations and multiple regression analyses. Neurological soft signs were more frequent and more severe in the Black African ancestry group. Also, the factor structure and presentation of NSS in the two ancestry groups were significantly different. Neurological soft signs, especially motor sequencing and cognitive-perceptual abnormalities, were independently associated with disorganization psychopathologies in all the participant groups. Differences in the profile of NSS in Black compared with non-Black African ancestry patients with first episode schizophrenia may suggest differing patterns of expression of NSS in schizophrenia according to genetic ancestry. [ABSTRACT FROM AUTHOR]

Published

2018

21. Nonfunctional mutant Wrn protein leads to neurological deficits, neuronal stress, microglial alteration, and immune imbalance in a mouse model of Werner syndrome.

Author

Hui, Chin Wai, St-Pierre, Marie-Kim, Detuncq, Jérôme, Aumailley, Lucie, Dubois, Marie-Julie, Couture, Vanessa, Skuk, Daniel, Marette, André, Tremblay, Jacques P., Lebel, Michel, and Tremblay, Marie-Ève

Subjects

*WERNER'S syndrome, *GENETIC mutation, *NEUROLOGICAL disorders -- Genetic aspects, *HELICASES, *OXIDATIVE stress, *MICROGLIA, *CYTOKINES, *GENETICS

Abstract

Highlights • WrnΔhel/Δhel mice develop several behavioral deficits during aging. • WRN mutation induces oxidative stress in prefrontal cortex of aged WrnΔhel/Δhel mice. • Altered central and peripheral immune functions may be responsible for these changes. Abstract Werner syndrome (WS) is a premature aging disorder caused by mutations in a RecQ-family DNA helicase, WRN. Mice lacking part of the helicase domain of the WRN orthologue exhibit many phenotypic features of WS, including metabolic abnormalities and a shorter lifespan. Yet, little is known about the impact of WRN mutations on the central nervous system in both humans and mouse models of WS. In the current study, we have performed a longitudinal behavioral assessment on mice bearing a Wrn helicase deletion. Behavioral tests demonstrated a loss of motor activity and coordination, reduction in perception, increase in repetitive behavior, and deficits in both spatial and social novelty memories in Wrn mutant mice compared to age-matched wild type mice. These neurological deficits were associated with biochemical and histological changes in the brain of aged Wrn mutant mice. Microglia, resident immune cells that regulate neuronal plasticity and function in the brain, were hyper-ramified in multiple regions involved with the behavioral deficits of Wrn mutant mice. Furthermore, western analyses indicated that Wrn mutant mice exhibited an increase of oxidative stress markers in the prefrontal cortex. Supporting these findings, electron microscopy studies revealed increased cellular aging and oxidative stress features, among microglia and neurons respectively, in the prefrontal cortex of aged Wrn mutant mice. In addition, multiplex immunoassay of serum identified significant changes in the expression levels of several pro- and anti-inflammatory cytokines. Taken together, these findings indicate that microglial dysfunction and neuronal oxidative stress, associated with peripheral immune system alterations, might be important driving forces leading to abnormal neurological symptoms in WS thus suggesting potential therapeutic targets for interventions. [ABSTRACT FROM AUTHOR]

Published

2018

22. Noncoding RNAs in disease.

Author

Lekka, Evangelia and Hall, Jonathan

Subjects

*NON-coding RNA, *MICRORNA, *NEUROLOGICAL disorders -- Genetic aspects, *CARDIOVASCULAR diseases, *PATHOLOGICAL physiology

Abstract

Noncoding RNAs are emerging as potent and multifunctional regulators in all biological processes. In parallel, a rapidly growing number of studies has unravelled associations between aberrant noncoding RNA expression and human diseases. These associations have been extensively reviewed, often with the focus on a particular microRNA (miRNA) (family) or a selected disease/pathology. In this Mini‐Review, we highlight a selection of studies in order to demonstrate the wide‐scale involvement of miRNAs and long noncoding RNAs in the pathophysiology of three types of diseases: cancer, cardiovascular and neurological disorders. This research is opening new avenues to novel therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2018

23. Convergent molecular defects underpin diverse neurodegenerative diseases.

Author

Tofaris, George K. and Buckley, Noel J.

Subjects

NEURODEGENERATION, DISEASES in older people, NEUROLOGICAL disorders -- Genetic aspects, PROTEIN folding, ALZHEIMER'S disease, PARKINSON'S disease, PHYSIOLOGY, GENETICS

Abstract

In our ageing population, neurodegenerative disorders carry an enormous personal, societal and economic burden. Although neurodegenerative diseases are often thought of as clinicopathological entities, increasing evidence suggests a considerable overlap in the molecular underpinnings of their pathogenesis. Such overlapping biological processes include the handling of misfolded proteins, defective organelle trafficking, RNA processing, synaptic health and neuroinflammation. Collectively but in different proportions, these biological processes in neurons or non-neuronal cells lead to regionally distinct patterns of neuronal vulnerability and progression of pathology that could explain the disease symptomology. With the advent of patient-derived cellular models and novel genetic manipulation tools, we are now able to interrogate this commonality despite the cellular complexity of the brain in order to develop novel therapeutic strategies to prevent or arrest neurodegeneration. Here, we describe broadly these concepts and their relevance across neurodegenerative diseases. [ABSTRACT FROM AUTHOR]

Published

2018

24. The Kaleidoscope of Microglial Phenotypes.

Author

Dubbelaar, Marissa L., Kracht, Laura, Eggen, Bart J. L., and Boddeke, Erik W. G. M.

Subjects

KALEIDOSCOPES, NEUROLOGICAL disorders -- Genetic aspects, MICROGLIA, HUMAN phenotype, GENE expression, CENTRAL nervous system

Abstract

Gene expression analyses of microglia, the tissue-resident macrophages of the central nervous system (CNS), led to the identification of homeostatic as well as neurological disease-specific gene signatures of microglial phenotypes. Upon alterations in the neural microenvironment, either caused by local insults from within the CNS (during neurodegenerative diseases) or by macroenvironmental incidents, such as social stress, microglia can switch phenotypes—generally referred to as “microglial activation.” The interplay between the microenvironment and its influence on microglial phenotypes, regulated by (epi)genetic mechanisms, can be imagined as the different colorful crystal formations (microglial phenotypes) that change upon rotation (microenvironmental changes) of a kaleidoscope. In this review, we will discuss microglial phenotypes in relation to neurodevelopment, homeostasis, in vitro conditions, aging, and neurodegenerative diseases based on transcriptome studies. By overlaying these disease-specific microglial signatures, recent publications have identified a specific set of genes that is differentially expressed in all investigated diseases, called a microglial core gene signature with multiple diseases. We will conclude this review with a discussion about the complexity of this microglial core gene signature associated with multiple diseases. [ABSTRACT FROM AUTHOR]

Published

2018

25. Gene expression profiles in neurological tissues during West Nile virus infection: a critical meta-analysis.

Author

Kosch, Robin, Delarocque, Julien, Claus, Peter, Becker, Stefanie C., and Jung, Klaus

Subjects

*NERVOUS system abnormalities, *WEST Nile virus, *NEUROLOGICAL disorders -- Genetic aspects, *GENE ontology, *GENE expression, *PHYSIOLOGY

Abstract

Background: Infections with the West Nile virus (WNV) can attack neurological tissues in the host and alter gene expression levels therein. Several individual studies have analyzed these changes in the transcriptome based on measurements with DNA microarrays. Individual microarray studies produce a high-dimensional data structure with the number of studied genes exceeding the available sample size by far. Therefore, the level of scientific evidence of these studies is rather low and results can remain uncertain. Furthermore, the individual studies concentrate on different types of tissues or different time points after infection. A general statement regarding the transcriptional changes through WNV infection in neurological tissues is therefore hard to make. We screened public databases for transcriptome expression studies related to WNV infections and used different analysis pipelines to perform meta-analyses of these data with the goal of obtaining more stable results and increasing the level of evidence. Results: We generated new lists of genes differentially expressed between WNV infected neurological tissues and control samples. A comparison with these genes to findings of a meta-analysis of immunological tissues is performed to figure out tissue-specific differences. While 5.879 genes were identified exclusively in the neurological tissues, 15 genes were found exclusively in the immunological tissues, and 44 genes were commonly detected in both tissues. Most findings of the original studies could be confirmed by the meta-analysis with a higher statistical power, but some genes and GO terms related to WNV were newly detected, too. In addition, we identified gene ontology terms related to certain infection processes, which are significantly enriched among the differentially expressed genes. In the neurological tissues, 17 gene ontology terms were found significantly different, and 2 terms in the immunological tissues. Conclusions: A critical discussion of our findings shows benefits but also limitations of the meta-analytic approach. In summary, the produced gene lists, identified gene ontology terms and network reconstructions appear to be more reliable than the results from the individual studies. Our meta-analysis provides a basis for further research on the transcriptional mechanisms by WNV infections in neurological tissues. [ABSTRACT FROM AUTHOR]

Published

2018

26. Clinical, genetic and neuropathological characterization of spinocerebellar ataxia type 37.

Author

Corral-Juan, Marc, Serrano-Munuera, Carmen, Rábano, Alberto, Cota-González, Daniel, Segarra-Roca, Anna, Ispierto, Lourdes, Cano-Orgaz, Antonio Tomás, Adarmes, Astrid D., Méndez-del-Barrio, Carlota, Jesús, Silvia, Mir, Pablo, Volpini, Victor, Alvarez-Ramo, Ramiro, Sánchez, Ivelisse, and Matilla-Dueñas, Antoni

Subjects

*SPINOCEREBELLAR ataxia, *NEUROLOGICAL disorders, *SPASMS, *MOTOR neurons, *STATISTICAL correlation, *NEUROLOGICAL disorders -- Genetic aspects, *CELLULAR signal transduction, *DNA, *GENE expression, *GENES, *GENETIC mutation

Abstract

The autosomal dominant spinocerebellar ataxias (SCAs) consist of a highly heterogeneous group of rare movement disorders characterized by progressive cerebellar ataxia variably associated with ophthalmoplegia, pyramidal and extrapyramidal signs, dementia, pigmentary retinopathy, seizures, lower motor neuron signs, or peripheral neuropathy. Over 41 different SCA subtypes have been described evidencing the high clinical and genetic heterogeneity. We previously reported a novel spinocerebellar ataxia type subtype, SCA37, linked to an 11-Mb genomic region on 1p32, in a large Spanish ataxia pedigree characterized by ataxia and a pure cerebellar syndrome distinctively presenting with early-altered vertical eye movements. Here we demonstrate the segregation of an unstable intronic ATTTC pentanucleotide repeat mutation within the 1p32 5' non-coding regulatory region of the gene encoding the reelin adaptor protein DAB1, implicated in neuronal migration, as the causative genetic defect of the disease in four Spanish SCA37 families. We describe the clinical-genetic correlation and the first SCA37 neuropathological findings caused by dysregulation of cerebellar DAB1 expression. Post-mortem neuropathology of two patients with SCA37 revealed severe loss of Purkinje cells with abundant astrogliosis, empty baskets, occasional axonal spheroids, and hypertrophic fibres by phosphorylated neurofilament immunostaining in the cerebellar cortex. The remaining cerebellar Purkinje neurons showed loss of calbindin immunoreactivity, aberrant dendrite arborization, nuclear pathology including lobulation, irregularity, and hyperchromatism, and multiple ubiquitinated perisomatic granules immunostained for DAB1. A subpopulation of Purkinje cells was found ectopically mispositioned within the cerebellar cortex. No significant neuropathological alterations were identified in other brain regions in agreement with a pure cerebellar syndrome. Importantly, we found that the ATTTC repeat mutation dysregulated DAB1 expression and induced an RNA switch resulting in the upregulation of reelin-DAB1 and PI3K/AKT signalling in the SCA37 cerebellum. This study reveals the unstable ATTTC repeat mutation within the DAB1 gene as the underlying genetic cause and provides evidence of reelin-DAB1 signalling dysregulation in the spinocerebellar ataxia type 37. [ABSTRACT FROM AUTHOR]

Published

2018

27. Electro-behavioral phenotype and cell injury following exposure to paraoxon-ethyl in mice: Effect of the genetic background.

Author

Baccus, Benjamin, Auvin, Stéphane, and Dorandeu, Frédéric

Subjects

*PARAOXON, *CELLS, *PHENOTYPES, *NEUROLOGICAL disorders -- Genetic aspects, *LABORATORY mice, *WOUNDS & injuries

Abstract

Organophosphorus compounds (OP) are irreversible inhibitors of both central and peripheral cholinesterases (ChE). They still represent a major health issue in some countries as well as a terrorist and military threat. In order to design appropriate medical counter-measures, a better understanding of the pathophysiology of the poisoning is needed. Little to nothing is known regarding the impact of the genetic background on OP-induced seizures and seizure-related cell injury. Using two different mouse strains, Swiss and C57BL/6J, exposed to a convulsing dose of the OP pesticide paraoxon-ethyl (POX), our study focused on seizure susceptibility, especially the occurrence of SE and related mortality. We also evaluated the initial neuropathological response and SE-induced cell injury. Following the administration of 2.4 mg/kg POX, more Swiss mice experienced SE than C57BL/6J (55.6% versus 17.2%) but the duration of their SE, based on EEG recordings, was shorter (64.3 ± 19.5 min versus 180.8 ± 36.8 min). No significant difference was observed between strains regarding mortality (33% versus 14%). In both strains limited cell injury was observed in the medial temporal cortex, the dentate gyrus and the CA3 field without inter-strain differences (Fluorojade C-positive cells/mm 2 ). Conversely, only C57BL/6J mice showed cell injury in the CA1 field. There was no obvious correlation between the number of Fluorojade C-positive cells and the duration of the EEG discharges. Our work suggests some differences between Swiss and C57BL/6J mice and lay ground to further studies on the impact of strains in the development of central nervous system toxicity of OP. [ABSTRACT FROM AUTHOR]

Published

2018

28. Neurodevelopmental synaptopathies: Insights from behaviour in rodent models of synapse gene mutations.

Author

Luo, J., Norris, R.H., Gordon, S.L., and Nithianantharajah, J.

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *GENETIC mutation, *SYNAPSES, *AUTISM spectrum disorders, *LABORATORY rodents

Abstract

The genomic revolution has begun to unveil the enormous complexity and heterogeneity of the genetic basis of neurodevelopmental disorders such as such epilepsy, intellectual disability, autism spectrum disorder and schizophrenia. Increasingly, human mutations in synapse genes are being identified across these disorders. These neurodevelopmental synaptopathies highlight synaptic homeostasis pathways as a convergence point underlying disease mechanisms. Here, we review some of the key pre- and postsynaptic genes in which penetrant human mutations have been identified in neurodevelopmental disorders for which genetic rodent models have been generated. Specifically, we focus on the main behavioural phenotypes that have been documented in these animal models, to consolidate our current understanding of how synapse genes regulate key behavioural and cognitive domains. These studies provide insights into better understanding the basis of the overlapping genetic and cognitive heterogeneity observed in neurodevelopmental disorders. [ABSTRACT FROM AUTHOR]

Published

2018

29. Genetic strategies to tackle neurological diseases in fruit flies.

Author

Şentürk, Mümine and Bellen, Hugo J

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *DROSOPHILA melanogaster, *GENETIC models, *NEURODEGENERATION, *PATHOGENIC microorganisms, *PHYSIOLOGY

Abstract

Drosophila melanogaster is a genetic model organism that has contributed to the discovery of numerous genes whose human homologues are associated with diseases. The development of sophisticated genetic tools to manipulate its genome accelerates the discovery of the genetic basis of undiagnosed human diseases and the elucidation of molecular pathogenic events of known and novel diseases. Here, we discuss various approaches used in flies to assess the function of the fly homologues of disease-associated genes. We highlight how systematic and combinatorial approaches based on recently established methods provide us with integrated tool sets that can be applied to the study of neurodevelopmental and neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2018

30. MicroRNA Changes in Firefighters.

Author

Jeong, Kyoung Sook, Zhou, Jin, Griffin, Stephanie C., Jacobs, Elizabeth T., Dearmon-Moore, Devi, Zhai, Jing, Littau, Sally R., Gulotta, John, Moore, Paul, Peate, Wayne F., Richt, Crystal M., and Burgess, Jefferey L.

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *AGE distribution, *TUMOR suppressor genes, *ETHNIC groups, *FIRE fighters, *GENETIC polymorphisms, *OBESITY, *SURVIVAL, TUMOR genetics

Abstract

Objectives: Firefighters have elevated cancer incidence and mortality rates. MicroRNAs play prominent roles in carcinogenesis, but have not been previously evaluated in firefighters. Methods: Blood from 52 incumbent and 45 new recruit nonsmoking firefighters was analyzed for microRNA expression, and the results adjusted for age, obesity, ethnicity, and multiple comparisons. Results: Nine microRNAs were identified with at least a 1.5-fold significant difference between groups. All six microRNAs with decreased expression in incumbent firefighters have been reported to have tumor suppressor activity or are associated with cancer survival, and two of the three microRNAs with increased expression in incumbent firefighters have activities consistent with cancer promotion, with the remaining microRNA associated with neurological disease. Conclusion: Incumbent firefighters showed differential microRNA expression compared with new recruits, providing potential mechanisms for increased cancer risk in firefighters. [ABSTRACT FROM AUTHOR]

Published

2018

31. Subcortical neurodegeneration in chorea: Similarities and differences between chorea-acanthocytosis and Huntington's disease.

Author

Liu, Jia, Heinsen, Helmut, Grinberg, Lea T., Alho, Eduardo, Jr.Amaro, Edson, Pasqualucci, Carlos A., Rüb, Udo, den Dunnen, Wilfred, Arzberger, Thomas, Schmitz, Christoph, Kiessling, Maren, Bader, Benedikt, Danek, Adrian, and Amaro, Edson Jr.

Subjects

*NEURODEGENERATION, *HUNTINGTON disease, *NEUROLOGICAL disorders -- Genetic aspects, *GLIOSIS, *THALAMIC nuclei, *BASAL ganglia, *COMPARATIVE studies, *DEGENERATION (Pathology), *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *THALAMUS, *EVALUATION research, *ATROPHY

Abstract

Introduction: Chorea-acanthocytosis (ChAc) and Huntington's disease (HD) are neurodegenerative conditions that share clinical and neuropathological features, despite their distinct genetic etiologies.Methods: In order to compare these neuropathologies, serial gallocyanin-stained brain sections from three subjects with ChAc were analyzed and compared with our previous studies of eight HD cases, in addition to three hemispheres from two male controls.Results: Astrogliosis was much greater in the ChAc striatum, as compared to that found in HD, with dramatic increase in total striatal glia numbers and the number of glia per striatal neuron. Striatal astrocytes are most likely derived from the striatal subependymal layer in ChAc, which showed massive proliferation. The thalamic centromedian-parafascicular complex is reciprocally connected to the striatum and is more heavily affected in HD than in ChAc.Conclusion: The distinct patterns of selective vulnerability and gliosis observed in HD and ChAc challenge simplistic views on the pathogenesis of these two diseases with rather similar clinical signs. The particular roles played by astroglia in ChAc and in HD clearly need to be elucidated in more detail. [ABSTRACT FROM AUTHOR]

Published

2018

32. PRRT2 controls neuronal excitability by negatively modulating Na+ channel 1.2/1.6 activity.

Author

Fruscione, Floriana, Valente, Pierluigi, Sterlini, Bruno, Romei, Alessandra, Baldassari, Simona, Fadda, Manuela, Prestigio, Cosimo, Giansante, Giorgia, Sartorelli, Jacopo, Rossi, Pia, Rubio, Alicia, Gambardella, Antonio, Nieus, Thierry, Broccoli, Vania, Fassio, Anna, Baldelli, Pietro, Corradi, Anna, Zara, Federico, and Benfenati, Fabio

Subjects

*PROLINE, *MEMBRANE proteins, *NEUROLOGICAL disorders -- Genetic aspects, *GENETIC mutation, *ELECTROPHYSIOLOGY techniques, *SEIZURES (Medicine), *SODIUM metabolism, *SPASMS, *ANIMAL experimentation, *BRAIN, *GENE expression, *IMMUNOASSAY, *MICE, *NEURAL transmission, *NEURONS, *NEUROPLASTICITY, *PHENOTYPES, *GENETICS

Abstract

See Lerche (doi:10.1093/brain/awy073) for a scientific commentary on this article.Proline-rich transmembrane protein 2 (PRRT2) is the causative gene for a heterogeneous group of familial paroxysmal neurological disorders that include seizures with onset in the first year of life (benign familial infantile seizures), paroxysmal kinesigenic dyskinesia or a combination of both. Most of the PRRT2 mutations are loss-of-function leading to haploinsufficiency and 80% of the patients carry the same frameshift mutation (c.649dupC; p.Arg217Profs*8), which leads to a premature stop codon. To model the disease and dissect the physiological role of PRRT2, we studied the phenotype of neurons differentiated from induced pluripotent stem cells from previously described heterozygous and homozygous siblings carrying the c.649dupC mutation. Single-cell patch-clamp experiments on induced pluripotent stem cell-derived neurons from homozygous patients showed increased Na+ currents that were fully rescued by expression of wild-type PRRT2. Closely similar electrophysiological features were observed in primary neurons obtained from the recently characterized PRRT2 knockout mouse. This phenotype was associated with an increased length of the axon initial segment and with markedly augmented spontaneous and evoked firing and bursting activities evaluated, at the network level, by multi-electrode array electrophysiology. Using HEK-293 cells stably expressing Nav channel subtypes, we demonstrated that the expression of PRRT2 decreases the membrane exposure and Na+ current of Nav1.2/Nav1.6, but not Nav1.1, channels. Moreover, PRRT2 directly interacted with Nav1.2/Nav1.6 channels and induced a negative shift in the voltage-dependence of inactivation and a slow-down in the recovery from inactivation. In addition, by co-immunoprecipitation assays, we showed that the PRRT2-Nav interaction also occurs in brain tissue. The study demonstrates that the lack of PRRT2 leads to a hyperactivity of voltage-dependent Na+ channels in homozygous PRRT2 knockout human and mouse neurons and that, in addition to the reported synaptic functions, PRRT2 is an important negative modulator of Nav1.2 and Nav1.6 channels. Given the predominant paroxysmal character of PRRT2-linked diseases, the disturbance in cellular excitability by lack of negative modulation of Na+ channels appears as the key pathogenetic mechanism. [ABSTRACT FROM AUTHOR]

Published

2018

33. Analysis of the expression pattern of the schizophrenia-risk and intellectual disability gene TCF4 in the developing and adult brain suggests a role in development and plasticity of cortical and hippocampal neurons.

Author

Jung, Matthias, Häberle, Benjamin M., Tschaikowsky, Tristan, Wittmann, Marie-Theres, Balta, Elli-Anna, Stadler, Vivien-Charlott, Zweier, Christiane, Dörfler, Arnd, Gloeckner, Christian Johannes, and Lie, D. Chichung

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *GENETICS of schizophrenia, *TRANSCRIPTION factors

Abstract

Background: Haploinsufficiency of the class I bHLH transcription factor TCF4 causes Pitt-Hopkins syndrome (PTHS), a severe neurodevelopmental disorder, while common variants in the TCF4 gene have been identified as susceptibility factors for schizophrenia. It remains largely unknown, which brain regions are dependent on TCF4 for their development and function. Methods: We systematically analyzed the expression pattern of TCF4 in the developing and adult mouse brain. We used immunofluorescent staining to identify candidate regions whose development and function depend on TCF4. In addition, we determined TCF4 expression in the developing rhesus monkey brain and in the developing and adult human brain through analysis of transcriptomic datasets and compared the expression pattern between species. Finally, we morphometrically and histologically analyzed selected brain structures in Tcf4-haploinsufficient mice and compared our morphometric findings to neuroanatomical findings in PTHS patients. Results: TCF4 is broadly expressed in cortical and subcortical structures in the developing and adult mouse brain. The TCF4 expression pattern was highly similar between humans, rhesus monkeys, and mice. Moreover, Tcf4 haploinsufficiency in mice replicated structural brain anomalies observed in PTHS patients. Conclusion: Our data suggests that TCF4 is involved in the development and function of multiple brain regions and indicates that its regulation is evolutionary conserved. Moreover, our data validate Tcf4-haploinsufficient mice as a model to study the neurodevelopmental basis of PTHS. [ABSTRACT FROM AUTHOR]

Published

2018

34. Functional dissection of astrocyte-secreted proteins: Implications in brain health and diseases.

Author

Jha, Mithilesh Kumar, Kim, Jong-Heon, Song, Gyun Jee, Lee, Won-Ha, Lee, In-Kyu, Lee, Ho-Won, An, Seong Soo A., Kim, SangYun, and Suk, Kyoungho

Subjects

*ASTROCYTES, *BRAIN diseases, *CENTRAL nervous system -- Immunology, *NEUROLOGICAL disorders -- Genetic aspects, *PROTEOMICS

Abstract

Astrocytes, which are homeostatic cells of the central nervous system (CNS), display remarkable heterogeneity in their morphology and function. Besides their physical and metabolic support to neurons, astrocytes modulate the blood-brain barrier, regulate CNS synaptogenesis, guide axon pathfinding, maintain brain homeostasis, affect neuronal development and plasticity, and contribute to diverse neuropathologies via secreted proteins. The identification of astrocytic proteome and secretome profiles has provided new insights into the maintenance of neuronal health and survival, the pathogenesis of brain injury, and neurodegeneration. Recent advances in proteomics research have provided an excellent catalog of astrocyte-secreted proteins. This review categorizes astrocyte-secreted proteins and discusses evidence that astrocytes play a crucial role in neuronal activity and brain function. An in-depth understanding of astrocyte-secreted proteins and their pathways is pivotal for the development of novel strategies for restoring brain homeostasis, limiting brain injury/inflammation, counteracting neurodegeneration, and obtaining functional recovery. [ABSTRACT FROM AUTHOR]

Published

2018

35. Immediate Early Genes Anchor a Biological Pathway of Proteins Required for Memory Formation, Long-Term Depression and Risk for Schizophrenia.

Author

Marballi, Ketan K. and Gallitano, Amelia L.

Subjects

NEUROLOGICAL disorders -- Genetic aspects, PROTEIN analysis, SCHIZOPHRENIA, MEMORY, MENTAL depression, SINGLE nucleotide polymorphisms, GENOMES, GENETICS

Abstract

While the causes of myriad medical and infectious illnesses have been identified, the etiologies of neuropsychiatric illnesses remain elusive. This is due to two major obstacles. First, the risk for neuropsychiatric disorders, such as schizophrenia, is determined by both genetic and environmental factors. Second, numerous genes influence susceptibility for these illnesses. Genome-wide association studies have identified at least 108 genomic loci for schizophrenia, and more are expected to be published shortly. In addition, numerous biological processes contribute to the neuropathology underlying schizophrenia. These include immune dysfunction, synaptic and myelination deficits, vascular abnormalities, growth factor disruption, and N-methyl- D-aspartate receptor (NMDAR) hypofunction. However, the field of psychiatric genetics lacks a unifying model to explain how environment may interact with numerous genes to influence these various biological processes and cause schizophrenia. Here we describe a biological cascade of proteins that are activated in response to environmental stimuli such as stress, a schizophrenia risk factor. The central proteins in this pathway are critical mediators of memory formation and a particular form of hippocampal synaptic plasticity, long-term depression (LTD). Each of these proteins is also implicated in schizophrenia risk. In fact, the pathway includes four genes that map to the 108 loci associated with schizophrenia: GRIN2A, nuclear factor of activated T-cells (NFATc3), early growth response 1 (EGR1) and NGFI-A Binding Protein 2 (NAB2); each of which contains the “Index single nucleotide polymorphism (SNP)" (most SNP) at its respective locus. Environmental stimuli activate this biological pathway in neurons, resulting in induction of EGR immediate early genes: EGR1, EGR3 and NAB2. We hypothesize that dysfunction in any of the genes in this pathway disrupts the normal activation of Egrs in response to stress. This may result in insufficient electrophysiologic, immunologic, and neuroprotective, processes that these genes normally mediate. Continued adverse environmental experiences, over time, may thereby result in neuropathology that gives rise to the symptoms of schizophrenia. By combining multiple genes associated with schizophrenia susceptibility, in a functional cascade triggered by neuronal activity, the proposed biological pathway provides an explanation for both the polygenic and environmental influences that determine the complex etiology of this mental illness. [ABSTRACT FROM AUTHOR]

Published

2018

36. Hypomyelinating disorders in China: The clinical and genetic heterogeneity in 119 patients.

Author

Ji, Haoran, Li, Dongxiao, Wu, Ye, Zhang, Quanli, Gu, Qiang, Xie, Han, Ji, Taoyun, Wang, Huifang, Zhao, Lu, Zhao, Haijuan, Yang, Yanling, Feng, Hongchun, Xiong, Hui, Ji, Jinhua, Yang, Zhixian, Kou, Liping, Li, Ming, Bao, Xinhua, Chang, Xingzhi, and Zhang, Yuehua

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *MYELINATION, *MAGNETIC resonance imaging of the brain, *CHINESE people, *GENE amplification, *DISEASES

Abstract

Objective: Hypomyelinating disorders are a group of clinically and genetically heterogeneous diseases characterized by neurological deterioration with hypomyelination visible on brain MRI scans. This study was aimed to clarify the clinical and genetic features of HMDs in Chinese population. Methods: 119 patients with hypomyelinating disorders in Chinese population were enrolled and evaluated based on their history, clinical manifestation, laboratory examinations, series of brain MRI with follow-up, genetic etiological tests including chromosomal analysis, multiplex ligation probe amplification, Sanger sequencing, targeted enrichment-based next-generation sequencing and whole exome sequencing. Results: Clinical and genetic features of hypomyelinating disorders were revealed. Nine different hypomyelinating disorders were identified in 119 patients: Pelizaeus-Merzbacher disease (94, 79%), Pelizaeus-Merzbacher-like disease (10, 8%), hypomyelination with atrophy of the basal ganglia and cerebellum (3, 3%), GM1 gangliosidosis (5, 4%), GM2 gangliosidosis (3, 3%), trichothiodystrophy (1, 1%), Pol III-related leukodystrophy (1, 1%), hypomyelinating leukodystrophy type 9 (1, 1%), and chromosome 18q deletion syndrome (1, 1%). Of the sample, 94% (112/119) of the patients were genetically diagnosed, including 111 with mutations distributing across 9 genes including PLP1, GJC2, TUBB4A, GLB1, HEXA, HEXB, ERCC2, POLR3A, and RARS and 1 with mosaic chromosomal change of 46, XX,del(18)(q21.3)/46,XX,r(18)(p11.32q21.3)/45,XX,-18. Eighteen novel mutations were discovered. Mutations in POLR3A and RARS were first identified in Chinese patients with Pol III-related leukodystrophy and hypomyelinating leukodystrophy, respectively. Significance: This is the first report on clinical and genetic features of hypomyelinating disorders with a large sample of patients in Chinese population, identifying 18 novel mutations especially mutations in POLR3A and RARS in Chinese patients, expanding clinical and genetic spectrums of hypomyelinating disorders. [ABSTRACT FROM AUTHOR]

Published

2018

37. Statistical genetics and its application to neuroimmunology.

Author

Ogawa, Kotaro and Okada, Yukinori

Subjects

*SINGLE nucleotide polymorphisms, *GENETICS of multiple sclerosis, *NEUROLOGICAL disorders -- Genetic aspects, *LOCUS (Genetics), *META-analysis, *HLA histocompatibility antigens

Abstract

Abstract: Statistical genetics is a field involving the analysis of genetic data. With the development of next‐generation sequencing and single‐nucleotide polymorphism microarrays, the amount of genetic data is increasing rapidly. Genome‐wide association studies are one example of the successful application of an approach based on statistical genetics. To shed light on neuroinflammatory diseases, such as multiple sclerosis, >100 000 people have been enrolled in the genome‐wide association study meta‐analysis, and 200 loci associated with multiple sclerosis have been detected. To utilize these genetic data for clinical medicine, development of novel methods of statistical genetics is warranted. Human leukocyte antigen imputation and in silico drug repositioning are good examples of such approaches. [ABSTRACT FROM AUTHOR]

Published

2018

38. CDK5-mediated phosphorylation of Sirt2 contributes to depressive-like behavior induced by social defeat stress.

Author

Zhang, Zheng, Zhang, Pei, Qi, Guang-Jian, Jiao, Feng-Juan, Wang, Qing-Zhi, Yan, Jian-Guo, He, Feng, Zhang, Qian, Lv, Ze-Xi, Peng, Xiang, Cai, Hong-Wei, Chen, Xiaoqian, Sun, Ning, and Tian, Bo

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *MENTAL depression, *PHOSPHORYLATION, *SIRTUINS, *PSYCHOLOGICAL stress, *DISEASE relapse

Abstract

Major depressive disorder (MDD) is a common, severe and recurrent psychiatric disorder worldwide; however, the underlying neuropathological mechanisms remain elusive. Histone deacetylases (HDACs) appear to play an essential role in depression. As the class III HDACs, Sirt1 and Sirt2 have attracted the most interest in the nervous system. Indeed, chronic stress decreased Sirt1 activity and down-regulated Sirt1 gene expression in MDD. Nevertheless, there is a paucity of literature on the role of Sirt2. To study the role of Sirt2 we established a MDD mouse model in wild type and Sirt2 knockout C57BL/6 mice using social defeat stress (SDS). We found that a lack of Sirt2 blocked the development of SDS-induced depressive-like behavior. Moreover, SDS led to Sirt2 phosphorylation in the amygdala without changing total Sirt2 levels, and blocking the phosphorylation of Sirt2 by CDK5 at serine residues 368 and 372 prevented SDS-induced depressive-like behavior and Sirt2 nuclear import. We also discovered that SDS-induced Sirt2 phosphorylation was involved in VTA-amygdala modulation using TetTag-pharmacogenetic method. These results suggest that CDK5 mediates phosphorylation of Sirt2 in the amygdala and contributes to the depressive-like behavior induced by SDS. This study highlights that inhibiting CDK5-dependent phosphorylation of Sirt2 at serine residues 368 and 372 by myristoylated membrane-permeabilising peptide (Sirt2-p), rather than using non-specific sirtuin inhibitors, may be a novel strategy for treating depression. [ABSTRACT FROM AUTHOR]

Published

2018

39. Anhedonia Following Early-Life Adversity Involves Aberrant Interaction of Reward and Anxiety Circuits and Is Reversed by Partial Silencing of Amygdala Corticotropin-Releasing Hormone Gene.

Author

Bolton, Jessica L., Molet, Jenny, Regev, Limor, Chen, Yuncai, Rismanchi, Neggy, Haddad, Elizabeth, Yang, Derek Z., Obenaus, Andre, and Baram, Tallie Z.

Subjects

*ANHEDONIA, *CORTICOTROPIN releasing hormone, *GENE silencing, *NEUROLOGICAL disorders -- Genetic aspects, *PSYCHOLOGICAL stress, *DIFFUSION tensor imaging

Abstract

Background Anhedonia, the diminished ability to experience pleasure, is an important dimensional entity linked to depression, schizophrenia, and other emotional disorders, but its origins and mechanisms are poorly understood. We have previously identified anhedonia, manifest as decreased sucrose preference and social play, in adolescent male rats that experienced chronic early-life adversity/stress (CES). Here we probed the molecular, cellular, and circuit processes underlying CES-induced anhedonia and tested them mechanistically. Methods We examined functional brain circuits and neuronal populations activated by social play in adolescent CES and control rats. Structural connectivity between stress- and reward-related networks was probed using high-resolution diffusion tensor imaging, and cellular/regional activation was probed using c-Fos. We employed viral-genetic approaches to reduce corticotropin-releasing hormone ( Crh ) expression in the central nucleus of the amygdala in anhedonic rats, and tested for anhedonia reversal in the same animals. Results Sucrose preference was reduced in adolescent CES rats. Social play, generally considered an independent measure of pleasure, activated brain regions involved in reward circuitry in both control and CES groups. In CES rats, social play activated Crh -expressing neurons in the central nucleus of the amygdala, typically involved in anxiety/fear, indicating aberrant functional connectivity of pleasure/reward and fear circuits. Diffusion tensor imaging tractography revealed increased structural connectivity of the amygdala to the medial prefrontal cortex in CES rats. Crh -short hairpin RNA, but not control short hairpin RNA, given into the central nucleus of the amygdala reversed CES-induced anhedonia without influencing other emotional measures. Conclusions These findings robustly demonstrate aberrant interactions of stress and reward networks after early-life adversity and suggest mechanistic roles for Crh -expressing amygdala neurons in emotional deficits portending major neuropsychiatric disorders. [ABSTRACT FROM AUTHOR]

Published

2018

40. Phenotypic and Molecular Spectrum of Aicardi-Goutières Syndrome: A Study of 24 Patients.

Author

Al Mutairi, Fuad, Alfadhel, Majid, Nashabat, Marwan, El-Hattab, Ayman W., Ben-Omran, Tawfeg, Hertecant, Jozef, Eyaid, Wafaa, Ali, Rehab, Alasmari, Ali, Kara, Majdi, Al-Twaijri, Waleed, Filimban, Rana, Alshenqiti, Abduljabbar, Al-Owain, Mohammed, Faqeih, Eissa, and Alkuraya, Fowzan S.

Subjects

*AICARDI-Goutieres syndrome, *NEUROLOGICAL disorders -- Genetic aspects, *PHENOTYPES, *MOLECULAR diagnosis, *GENETIC mutation, *AUTOIMMUNE diseases, *BRAIN, *CONSANGUINITY, *SEIZURES (Medicine), *EPILEPSY, *ESTERASES, *NERVOUS system abnormalities, *NEUROLOGICAL disorders, *SPASMS, *SPASTICITY, *ATROPHY, *DISEASE complications

Abstract

Background: Aicardi-Goutières syndrome is a rare genetic neurological disorder with variable clinical manifestations. Molecular detection of specific mutations is required to confirm the diagnosis. The aim of this study was to review the clinical and molecular diagnostic findings in 24 individuals with Aicardi-Goutières syndrome who presented during childhood in an Arab population.Materials and Methods: We reviewed the records of 24 patients from six tertiary hospitals in different Arab countries. All included patients had a molecular diagnosis of Aicardi-Goutières syndrome.Results: Six individuals with Aicardi-Goutières syndrome (25%) had a neonatal presentation, whereas the remaining patients presented during the first year of life. Patients presented with developmental delay (24 cases, 100%); spasticity (24 cases, 100%); speech delay (23 cases, 95.8%); profound intellectual disability (21 cases, 87.5%); truncal hypotonia (21 cases, 87.5%); seizures (eighteen cases, 75%); and epileptic encephalopathy (15 cases, 62.5%). Neuroimaging showed white matter abnormalities (22 cases, 91.7%), cerebral atrophy (75%), and small, multifocal calcifications in the lentiform nuclei and deep cerebral white matter (54.2%). Homozygous mutations were identified in RNASEH2B (54.2%), RNASEH2A (20.8%), RNASEH2C (8.3%), SAMHD1 (8.3%), TREX1 (4.2%), and heterozygous mutations in IFIH1 (4.2%), with c.356A>G (p.Asp119Gly) in RNASEH2B being the most frequent mutation. Three novel mutations c.987delT and c.625 + 1G>A in SAMHD1 gene and c.961G>T in the IFIHI1 gene were identified.Conclusions: This is the largest molecularly confirmed Aicardi-Goutières syndrome cohort from Arabia. By presenting these clinical and molecular findings, we hope to raise awareness of Aicardi-Goutières syndrome and to demonstrate the importance of specialist referral and molecular diagnosis. [ABSTRACT FROM AUTHOR]

Published

2018

41. Effect of Whole Exome Sequencing in Diagnosis of Inborn Errors of Metabolism and Neurogenetic Disorders.

Author

SHAKIBA, Marjan and KERAMATIPOUR, Mohammad

Subjects

INBORN errors of metabolism diagnosis, NEUROLOGICAL disorders -- Genetic aspects, INFORMATION storage & retrieval systems, MEDICAL databases, MEDLINE, ONLINE information services, SYSTEMATIC reviews, SEQUENCE analysis

Abstract

Objective Inborn errors of metabolism are complex disorders with huge variability in clinical manifestations. Decreasing cost of whole exome sequencing (WES) in recent years, made it affordable. Therefore, we witnessed an increase in using WES in diagnosis of genetic diseases, including inherited metabolic disorders. Materials & Methods A systematic search was done in well-known databases including Medline, Google, Cochrane, and PubMed until 1 Oct 2017. We reviewed the articles addressing the use of WES in diagnosis of metabolic and neurogenetic diseases to evaluate its impact in diagnosis of these conditions. Results WES is an effective technology with remarkable impact in diagnosis of metabolic and neurologic diseases, especially in complex cases. Diagnostic yield of WES for these conditions has large variety, ranging from 16% to 68% with an increase during recent years. WES can provide fresh valuable information about new disease, new variants and phenotypes. Careful analysis and interpretation of data obtained by WES and precise evaluation of correlation between clinical manifestation and WES findings are necessary to achieve a correct diagnosis. Conclusion WES is effective and useful technology for diagnosis of metabolic and neurogenetic diseases, especially in complex or unsolved cases. [ABSTRACT FROM AUTHOR]

Published

2018

42. Neuro-ichthyotic syndromes: A case series.

Author

Incecık, Faruk, Herguner, Ozlem, Ozbek, Mehmet, Gungor, Serdal, Yılmaz, Mustafa, Rizzo, Wiliam, and Mert, Gülen

Subjects

NEUROLOGICAL disorders -- Genetic aspects, CONSANGUINITY, DEAFNESS, DORFMAN-Chanarin syndrome, ICHTHYOSIS, PEOPLE with intellectual disabilities, NEUROLOGICAL disorders, SJOGREN'S syndrome, SPHINGOLIPIDOSES, GENETIC testing, SYMPTOMS, RETROSPECTIVE studies, GENETICS

Abstract

Background: The neuro-ichthyotic diseases are clinically and genetically heterogeneous. The purpose of this study was to evaluate the clinical and neuroradiological findings and to analyze mutation in 15 patients with neuro-ichthyotic diseases. Materials and Methods: We retrospectively analyzed the records of 15 patients with the diagnosis of neuro-ichthyotic diseases. Results: Eight female and seven male patients (age range 11 months–52 years) were investigated. There were eight patients with Sjögren–Larsson syndrome (SLS), five patients with multiple sulfatase deficiency (MSD), one patient with Chanarin–Dorfman’s syndrome, and one patient with mental retardation, enteropathy, deafness, neuropathy, ichthyosis, and keratodermia (MEDNIK) syndrome. Parental consanguinity was found in all the patients except one. All patients had ichthyosis. Diagnosis was performed with genetic study. Conclusions: Because biochemical and clinical findings are variable, the diagnosis is difficult in most of the cases. Detailed skin and physical examinations are mandatory in these patients. Genetic tests are necessary for accurate diagnosis. [ABSTRACT FROM AUTHOR]

Published

2018

43. Cocaine alters Homer1 natural antisense transcript in the nucleus accumbens.

Author

Sartor, Gregory C., Powell, Samuel K., Velmeshev, Dmitry, Lin, David Y., Magistri, Marco, Wiedner, Hannah J., Malvezzi, Andrea M., Andrade, Nadja S., Faghihi, Mohammad A., and Wahlestedt, Claes

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *COCAINE, *NUCLEUS accumbens, *PHYSIOLOGICAL adaptation, *CHROMATIN, *GENE expression, *PHYSIOLOGY

Abstract

Natural antisense transcripts (NATs) are an abundant class of long noncoding RNAs that have recently been shown to be key regulators of chromatin dynamics and gene expression in nervous system development and neurological disorders. However, it is currently unclear if NAT-based mechanisms also play a role in drug-induced neuroadaptations. Aberrant regulation of gene expression is one critical factor underlying the long-lasting behavioral abnormalities that characterize substance use disorder, and it is possible that some drug-induced transcriptional responses are mediated, in part, by perturbations in NAT activity. To test this hypothesis, we used an automated algorithm that mines the NCBI AceView transcriptomics database to identify NAT overlapping genes linked to addiction. We found that 22% of the genes examined contain NATs and that expression of Homer1 natural antisense transcript ( Homer1-AS ) was altered in the nucleus accumbens (NAc) of mice 2 h and 10 days following repeated cocaine administration. In in vitro studies, depletion of Homer1-AS lead to an increase in the corresponding sense gene expression, indicating a potential regulatory mechanisms of Homer1 expression by its corresponding antisense transcript. Future in vivo studies are needed to definitely determine a role for Homer1-AS in cocaine-induced behavioral and molecular adaptations. [ABSTRACT FROM AUTHOR]

Published

2017

44. Aberrant DNA methylation in lymphocytes of children with neurodevelopmental disorders.

Author

Naumova, O., Rychkov, S., Odintsova, V., Kornilov, S., Shabalina, E., Antsiferova, D., Zhukova, O., and Grigorenko, E.

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *DNA methylation, *LYMPHOCYTES, *EPIGENETICS, *GENETIC regulation, *CENTRAL nervous system diseases

Abstract

Recent research in the field of genomics and epigenetics has provided evidence that alterations in the system of epigenetic regulation are highly involved in the molecular etiology of neurodegenerative and neuropathic disorders. However, there is a gap in knowledge on the epigenetic perturbations that may accompany the CNS impairments during the development in the prenatal period and their manifestation as a congenital encephalopathy in the early postnatal period of child development. The present study is one of the first attempts aimed at addressing this gap. Here, we present data on genome-wide profiles of DNA methylation obtained using the Illumina HumanMethylation450 microarray in peripheral blood cells in a sample of young children (up to four years of age) diagnosed with congenital encephalopathy. We provide evidence on systematic alterations in the epigenome-predominant hypermethylation of gene promoter associated CpG islands-related to the CNS impairment in children. Specifically, we found significant DNA methylation changes in genes involved in DNA-dependent transcription regulation and transcription factor binding, with a key role of the transcription factor JUN; in genes controlling cellular response to hypoxia; and in genes involved in the control of neuronal development, functioning, and death. [ABSTRACT FROM AUTHOR]

Published

2017

45. The Ability of the Eating Assessment Tool-10 to Detect Aspiration in Patients With Neurological Disorders.

Author

Arslan, Selen Serel, Demir, Numan, Kılınç, Hasan E., and Karaduman, Aynur A.

Subjects

*DEGLUTITION disorders, *PATHOLOGICAL psychology, *NEUROLOGICAL disorders -- Genetic aspects, *QUALITY of life, *DIAGNOSIS, *DISEASE risk factors, *THERAPEUTICS

Abstract

Background/Aims Dysphagia is common in patients with neurological disorders. There is a need to identify patients at risk early by a useful clinical tool to prevent its serious complications. The study aims to determine the ability of the Turkish version of Eating Assessment Tool-10 (T-EAT-10) to detect aspiration in patients with neurological disorders. Methods Two hundred fifty-nine patients with neurological disorders who had complaints about swallowing difficulty and referred for a swallowing evaluation were included. Oropharyngeal dysphagia was evaluated with the T-EAT-10 and videofluoroscopic swallowing study in the same day. The penetration-aspiration scale (PAS) was used to document the penetration and aspiration severity. Results The mean age of the patients was 59.72 ± 17.24 years (minimum [min] = 18, maximum [max] = 96), of which 57.1% were male. The mean T-EAT-10 of patients who had aspiration (PAS > 5) was 25.91 ± 10.31 (min = 1, max = 40) and the mean T-EAT-10 of patients who did not have aspiration (PAS < 6) was 15.70 ± 10.54 (min = 0, max = 40) (P < 0.001). Patients with a T-EAT-10 score higher than 15 were 2.4 times more likely to aspirate. A linear correlation was found between T-EAT-10 and PAS scores of the patients (r = 0.416, P < 0.001). The sensitivity of a T-EAT-10 higher than 15 in detecting aspiration was 81.0% and the specificity was 58.0%. A T-EAT-10 score of higher than 15 has a positive predictive value of 72.0% and a negative predictive value of 69.0%. Conclusion The T-EAT-10 can be used to detect unsafe airway protection in neurology clinics to identify and refer dysphagic patients for further evaluation. [ABSTRACT FROM AUTHOR]

Published

2017

46. Subjects at Risk for Genetic Late-Onset Neurological Diseases: Objective Knowledge.

Author

Leite, Ângela, Leite, Fernanda, and Dinis, Maria alzira P.

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *POLYNEUROPATHIES, *HEMOCHROMATOSIS, *HUNTINGTON disease, *GENETIC disorders, *DISEASE risk factors

Abstract

Background/Aims: This study addresses the objective knowledge about the disease of subjects at risk for 3 genetic late-onset neurological diseases (LOND): familial amyloid polyneuropathy (FAP) TTR V30M, Huntington disease (HD), and Machado-Joseph disease (MJD). Methods: Subjects at risk for FAP, HD, and MJD submitted to genetic counseling to know their status (carrier or non-carrier) and subjects at risk for hereditary hemochromatosis (HH), the control group, completed a sociodemographic questionnaire and answered the open-ended question: "What do you know about this disease?." Results: From 10 categories of answers, references to the disease, quantitative answers, references to the family, and metaphors stood out. References to the disease, references to the family, and metaphors were mentioned more often by subjects at risk for LOND than by subjects at risk for HH (control group). Conclusion: The disease itself and its meaning as well as sick relatives play a key role in the objective knowledge about LOND. Thus, genetic counseling protocols of subjects at risk for LOND should include questions concerning family knowledge and disease experience. [ABSTRACT FROM AUTHOR]

Published

2017

47. Functional Mechanisms of Microsatellite DNA in Eukaryotic Genomes.

Author

Bagshaw, Andrew T. M.

Subjects

*MICROSATELLITE repeats, *NEUROLOGICAL disorders -- Genetic aspects, *NEUROLOGICAL emergencies, *EUKARYOTIC cell genetics, *EUKARYOTIC genomes, *MESSENGER RNA

Abstract

Microsatellite repeat DNA is best known for its length mutability, which is implicated in several neurological diseases and cancers, and often exploited as a genetic marker. Less well-known is the body of work exploring the widespread and surprisingly diverse functional roles of microsatellites. Recently, emerging evidence includes the finding that normal microsatellite polymorphism contributes substantially to the heritability of human gene expression on a genome-wide scale, calling attention to the task of elucidating the mechanisms involved. At present, these are underexplored, but several themes have emerged. I review evidence demonstrating roles for microsatellites in modulation of transcription factor binding, spacing between promoter elements, enhancers, cytosine methylation, alternative splicing, mRNA stability, selection of transcription start and termination sites, unusual structural conformations, nucleosome positioning and modification, higher order chromatin structure, noncoding RNA, and meiotic recombination hot spots. [ABSTRACT FROM AUTHOR]

Published

2017

48. BPAG1, a distinctive role in skin and neurological diseases.

Author

Ali, Arshad, Hu, Lifang, Zhao, Fan, Qiu, Wuxia, Wang, Pai, Ma, Xiaoli, Zhang, Yan, Chen, Lei, and Qian, Airong

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *SKIN disease genetics, *CYTOSKELETAL proteins, *CELL junctions, *DYSTONIN, *CELL adhesion

Abstract

Spectraplakins are multifunctional cytoskeletal linker proteins that act as important communicators, connecting cytoskeletal components with each other and to cellular junctions. Bullous pemphigoid antigen 1 (BPAG1)/dystonin is a member of spectraplakin family and expressed in various tissues. Alternative splicing of BPAG1 gene produces various isoforms with unique structure and domains. BPAG1 plays crucial roles in numerous biological processes, such as cytoskeleton organization, cell polarization, cell adhesion, and cell migration as well as signaling transduction. Genetic mutation of BPAG1 isoforms is the miscreant of epidermolysis bullosa and multifarious, destructive neurological diseases. In this review, we summarize the recent advances of BPAG1’s role in various biological processes and in skin and neurological diseases. [ABSTRACT FROM AUTHOR]

Published

2017

49. A novel KCNA1 mutation in a patient with paroxysmal ataxia, myokymia, painful contractures and metabolic dysfunctions.

Author

Imbrici, Paola, Altamura, Concetta, Gualandi, Francesca, Mangiatordi, Giuseppe Felice, Neri, Marcella, De Maria, Giovanni, Ferlini, Alessandra, Padovani, Alessandro, D'Adamo, Maria Cristina, Nicolotti, Orazio, Pessia, Mauro, Conte, Diana, Filosto, Massimiliano, and Desaphy, Jean-Francois

Subjects

*GENETIC mutation, *ATAXIA, *NEUROLOGICAL disorders -- Genetic aspects, *METABOLIC disorders, *GENETIC code, *GENETICS

Abstract

Episodic ataxia type 1 (EA1) is a human dominant neurological syndrome characterized by continuous myokymia, episodic attacks of ataxic gait and spastic contractions of skeletal muscles that can be triggered by emotional stress and fatigue. This rare disease is caused by missense mutations in the KCNA1 gene coding for the neuronal voltage gated potassium channel Kv1.1, which contributes to nerve cell excitability in the cerebellum, hippocampus, cortex and peripheral nervous system. We identified a novel KCNA1 mutation, E283K, in an Italian proband presenting with paroxysmal ataxia and myokymia aggravated by painful contractures and metabolic dysfunctions. The E283K mutation is located in the S3–S4 extracellular linker belonging to the voltage sensor domain of Kv channels. In order to test whether the E283K mutation affects Kv1.1 biophysical properties we transfected HEK293 cells with WT or mutant cDNAs alone or in a 1:1 combination, and recorded relative potassium currents in the whole-cell configuration of patch-clamp. Mutant E283K channels display voltage-dependent activation shifted by 10 mV toward positive potentials and kinetics of activation slowed by ~ 2 fold compared to WT channels. Potassium currents resulting from heteromeric WT/E283K channels show voltage-dependent gating and kinetics of activation intermediate between WT and mutant homomeric channels. Based on homology modeling studies of the mutant E283K, we propose a molecular explanation for the reduced voltage sensitivity and slow channel opening. Overall, our results suggest that the replacement of a negatively charged residue with a positively charged lysine at position 283 in Kv1.1 causes a drop of potassium current that likely accounts for EA-1 symptoms in the heterozygous carrier. [ABSTRACT FROM AUTHOR]

Published

2017

50. Inherited 2q23.1 microdeletions involving the MBD5 locus.

Author

Tadros, Shereen, Wang, Rubin, Waters, Jonathan J., Waterman, Christine, Collins, Amanda L., Collinson, Morag N., Ahn, Joo W., Josifova, Dragana, Chetan, Ravi, and Kumar, Ajith

Subjects

*NEUROLOGICAL disorders -- Genetic aspects, *GENETIC mutation, *MUSCLE dysmorphia, *MOSAICISM, *PHENOTYPES

Abstract

Background Microdeletions of 2q23.1 disrupting MBD5 and loss of function mutations of MBD5 cause MBD5-Associated Neurodevelopmental disorders ( MAND). Nearly all reported patients have been isolated cases of de novo origin. Methods This study investigates three families with inherited MBD5 mutations from three different Regional Genetics Centres in the UK. Results Two of the parents in the study had MBD5 deletions in a mosaic form. The parent with an MBD5 deletion in an apparently nonmosaic form has a psychiatric disorder in the absence of developmental delay or dysmorphism. Conclusions Inherited forms of MBD5 deletions are rare, but do occur, especially in a mosaic form. The phenotypic spectrum of MAND may be wider than previously thought. [ABSTRACT FROM AUTHOR]

Published

2017