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Structural and functional plasticity alterations at single spines in Fragile X SyndromePanzarino, Alexandra Marie January 2023 (has links)
In the mammalian brain, information is believed to be encoded at the cellular level through alterations in synaptic weights. Furthermore, changes in synaptic strength are correlated with structural changes at dendritic spines, such as growth and shrinkage, which may serve to shape inputs into functional domains and increase the computational power of neurons. Neuroanatomical alterations in dendritic spines have been described in humans with intellectual disability, further supporting the relationship between neuronal structure and function.
Fragile X Syndrome (FXS) is the most common single-gene neurodevelopmental disorder, and a hallmark feature of this disorder is the increased density of long spines in several brain regions including the hippocampus. Identification of FXS spines as filopodia-like has led to the theory that these spines are immature, and that altered spine development underlies the cognitive dysfunction in this disorder. However, the functional capacity of the long spines observed in FXS is not well understood.
For my thesis work, I used two photon imaging, glutamate uncaging and electrophysiology to perform a high-resolution characterization of dendritic spine structure, function, and plasticity in the hippocampus of the FXS mouse model in order to determine what gives rise to these alterations and how this contributes to the observed neuronal dysfunction in this disorder. From my dissertation research, I find that while Fmr1 KO neurons have region-specific alterations in both dendrite and spine morphology, the functional responses of single synapses in FXS mutant neurons are grossly normal. FXS spines respond proportionally to increased levels of glutamate release, and the linear relationship between structure and function is preserved at these synapses. In addition, structural plasticity, both growth and shrinkage, at single inputs is similar in magnitude to control neurons following synaptic potentiation and depression, respectively.
However, upon more detailed examination of structural plasticity, either at single or multiple inputs, I find several deficits. First, following structural plasticity, I observe aberrant heterosynaptic plasticity in Fmr1 KO neurons, where unstimulated mutant spines located in close proximity to activated spines become significantly larger compared to neighboring spines in control neurons, which showed no significant change in size. Next, competition for mGluR-LTD does not occur in Fmr1 KO neurons, leading to an increase in spines that undergo spine shrinkage.
I conclude from this work that while spine morphology is altered in FXS, spines develop with functional synapses that have the capacity to express bidirectional forms of structural plasticity. However, these spines undergo abnormal structural plasticity across stimulated inputs, leading to the expression of aberrant heterosynaptic structural plasticity. As activity is integrated across a dendritic branch, such excess plasticity observed in Fmr1 KO neurons could contribute to the altered spine morphology as well as cognitive dysfunction observed in FXS.
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Folate studies on cultured cells from patients with the fragile X syndromePopovich, Bradley W. (Bradley Wayne) January 1982 (has links)
No description available.
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Activation of TLR4 by Tenascin C through the induction of Interleukin-6 in the Fragile X Mouse Model / IL-6 Secretion by Astrocytes in Fragile X MiceKrasovska, Victoria January 2018 (has links)
Fragile X syndrome (FXS) is identified by abnormal dendrite morphology and altered synaptic protein expression. Astrocyte secreted factors such as Tenascin C (TNC), may contribute to the synaptic changes, including maturation of the synapse. TNC is a known endogenous ligand of toll-like receptor 4 (TLR4) that has been shown to induce the expression of pro-inflammatory cytokines such as interleukin-6 (IL-6). At the molecular level, elevated IL-6 promotes excitatory synapse formation and increases dendrite spine length. With these molecular changes linked to the phenotype of FXS, we examined the expression and the mechanism of the endogenous TLR4 activator TNC, and its downstream target IL-6 in astrocytes from the FMR1 KO mouse model. Secreted TNC and IL-6 were significantly increased in FMR1 KO astrocytes. Exogenous TNC and lipopolysaccharide (LPS) stimulation of TLR4 induced secreted IL-6, whereas the antagonist of TLR4 (LPS-RS) had an opposing effect. Cortical protein expression of TNC and IL-6 were also significantly elevated in the postnatal FMR1 KO mouse. These results identify TNC as an endogenous ligand of TLR4, capable of effecting IL-6 secretion by astrocytes. In addition, there was an increase in the number of VGLUT1/PSD95 positive synaptic puncta of both WT and FMR1 KO neurons when plated with astrocyte conditioned media from FMR1 KO astrocytes, compared to those plated with media from wild type astrocytes. By assessing the cellular mechanisms involved, a novel therapeutic option could be made available to target abnormalities of synaptic function seen in FXS. / Thesis / Master of Science (MSc) / Autism spectrum disorders (ASDs) are neurodevelopmental disorders which arise from genetic and environmental factors. In the brain, a type of cell called the astrocyte is responsible for proper brain growth and development. Astrocytes release factors that promote inflammation, causing disruption of brain functions that control learning, memory and behaviour. Such factors released by astrocytes are capable of binding to their receptors, in turn impacting downstream targets, which have physiological effects.
This research used various biological and genetic techniques to determine if the mechanism of an astrocyte-specific factor called Tenascin C (TNC) is impaired in the Fragile X mouse model. In a normal astrocyte, TNC with its binding partner is able to release molecules responsible for inflammation. Such molecules have been shown to increase the number synapses, where neurons and astrocytes exchange information, to control brain function.
This proposed research would be the first to determine a role for TNC in ASDs. By assessing the cellular mechanisms involved between TNC and its binding partner, a novel therapeutic option could be made available in ASDs.
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Astrocytic Deficits in Maintaining Oxidative Homeostasis in the Fragile X Syndrome CortexVandenberg, Gregory January 2020 (has links)
Fragile X Syndrome (FXS) is caused by the instability of a CGG-repeated tract at the 5’ end of the Fmr1 transcript. This instability causes silencing of the gene coding for FMRP. Higher levels of reactive oxygen species, lipid peroxidation, and protein oxidation within brain tissue have been found to be associated with the disease. These imbalances, along with altered levels of components of the glutathione system, provide evidence for increased oxidative stress. Astrocytes, glial cells within the brain, have many functions within neurodevelopment. Specifically, they regulate growth and synaptic contacts of neurons, regulate the level of excitability of synapses, and protect neurons at high levels of activity. To protect neurons from oxidative stress, astrocytes maintain oxidative homeostasis through their mitochondrial electron transport and antioxidant systems. This study examines the relationship between oxidative stress and FXS by assessing mitochondrial function and the antioxidant system of astrocytes. Using the Fmr1 knockout (KO) mouse model, mitochondrial respiration, and reactive oxygen species (ROS) production was analyzed in cultured cortical astrocytes. Astrocytes collected from male and female mice were analyzed under both normoxic and hypoxic conditions. In addition, western blots were conducted on both cortical tissue and cultured cortical astrocytes to determine potential differences in enzyme expression. Results indicate elevations of leak state respiration and ROS production in Fmr1 KO cultured cortical astrocytes alongside alterations in antioxidant and NADPH-oxidase expression. Characterization of mitochondrial function and the antioxidant system of astrocytes will be highly valuable to the understanding of glial roles during brain development and could provide future insight to direct clinically relevant studies of FXS and other neurodevelopment disorders. / Thesis / Master of Science (MSc) / Fragile X Syndrome (FXS) is the most common genetic cause of intellectual disability. It is characterized by the loss of FMRP, an important protein in brain development. Within the FXS brain there is evidence of oxidative stress. The cells that maintain oxidative homeostasis in the brain are astrocytes. Astrocytes are glial cells important for brain development. This thesis evaluated astrocytes' ability to maintain oxidative homeostasis in the FXS cortex. The findings of this thesis provide important insights into our understanding of FXS pathology and will help direct clinically relevant studies of FXS and other neurodevelopmental disorders.
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Hippocampal metabotropic glutamate receptor long-term depression in health and disease: focus on mitogen-activated protein kinase pathwaysSanderson, T.M., Hogg, Ellen L., Collingridge, G.L., Corrêa, Sonia A.L. 05 April 2016 (has links)
Yes / Group I metabotropic glutamate receptor (mGluR) dependent long-term depression (LTD) is a major form of synaptic plasticity underlying learning and memory. The molecular mechanisms involved in mGluR-LTD have been investigated intensively for the last two decades. In this 60th anniversary special issue article, we review the recent advances in determining the mechanisms that regulate the induction, transduction and expression of mGluR-LTD in the hippocampus, with a focus on the mitogen-activated protein kinase (MAPK) pathways. In particular we discuss the requirement of p38 MAPK and extracellular signal-regulated kinase 1/2 (ERK 1/2) activation. The recent advances in understanding the signaling cascades regulating mGluR-LTD are then related to the cognitive impairments observed in neurological disorders, such as fragile X syndrome and Alzheimer's disease.
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Microbial Derived Modulators of Host Health and BehaviorMavros, Chrystal Felicia January 2024 (has links)
The human body is home to complex microbial communities that are fundamental to our physiology. Utilizing mouse models, behavior assays, gene expression analyses, and probiotic interventions, this research explores the intricate relationship between the gut microbiome, the central nervous system, and the immune system.
I discuss a strain of Escherichia coli Nissle engineered to produce serotonin, revealing its impact on gut function and immune response. I also evaluate butyrate’s potential to alleviate symptoms of Fragile X Syndrome, highlighting the gut-brain axis. Additionally, I study a strain of Bifidobacterium adolescentis and its role in metabolizing bile acids and modulating host immune cells and stress.
Collectively, these studies address the complex interplay between the gut microbiome and host health and behavior, illuminating the therapeutic potential of microbiome manipulation and setting the stage for novel interventions in neurodevelopmental disorders and immune function regulation.
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Étude ouverte pour évaluer l'efficacité et l'innocuité de la lovastatine chez les individus atteints du syndrome du X fragile / Lovastatine as a behavior treatment in children and adults with Fragile X Syndrome : Phase I studyCaku, Artuela January 2015 (has links)
Résumé : Le syndrome du X fragile (SXF) est la première cause de déficience intellectuelle héréditaire et résulte de mutations dans le gène FMR1 menant à l’absence d’expression de la protéine FMRP. Chez la souris déficiente en FMRP (KO-fmr1), des travaux récents ont montré une suractivation de la voie ERK qui jouerait un rôle important dans la physiopathologie du SXF. La lovastatine est un inhibiteur de la HMG-CoA réductase, utilisée pour traiter l’hypercholestérolémie. Parmi ses effets pléiotropes, elle inhiberait également ERK. Nous avons émis l’hypothèse que la lovastatine pourrait compenser en partie l’absence de FMRP et avoir des effets cognitifs positifs chez les individus avec SXF. Objectifs: Évaluer l’efficacité de la lovastatine à réduire le score global de l’ABC-C (Aberrant Behavior Checklist-Community), ainsi que le score de chaque sous-domaine d’ABC-C. Vérifier l’innocuité de la lovastatine pendant le traitement. Méthodes : Une étude prospective, non-randomisée a été réalisée sur une période de 12 semaines. Seize participants avec SXF (âgés de 10 à 31 ans), ont reçu des doses croissantes de la lovastatine (20 mg et 40 mg). Résultats : Des améliorations ont été observées au niveau du comportement aberrant soit le score total de l’ABC-C (p=0.005), ainsi que les sousdomaines: Hyperactivité (p=0.002), Léthargie(p=0.011), Stéréotypie (p=0.025) et Retrait social (p=0.003). Comme attendu, la lovastatine a été bien toléré sans aucun effet indésirable grave observé. Conclusion : Nos résultats suggèrent que la lovastatine peut avoir des effets bénéfices chez les individus avec le SXF. Une étude randomisée, placébocontrôlée est nécessaire pour valider nos trouvailles. / Abstract : Background: Fragile X Syndrome (FXS) results from dynamic mutations leading ultimately to the absence of expression of the Fragile X Mental Retardation Protein (FMRP). It is characterized by synaptic upregulated protein synthesis and immature dendritic spines associated with altered brain plasticity and cognitive functions. Recent work in Fmr1 knockout mice has shown that lovastatin, an inhibitor of Ras-ERK1/2, normalized hippocampus protein synthesis. We hypothesize that lovastatin, as a diseasemodifying drug, would counterweigh the absence of FMRP and improve brain development and learning abilities. Here we report a phase I study to assess the safety and efficacy of lovastatin in individuals with FXS. Methods: A total of 15 subjects (13 males, 6-31 years old) were treated with escalating doses of lovastatin (up to 40 mg) for three months. Their behaviour were assessed before and after treatment using the Aberrant Behavioral Checklist – Community (ABC-C) total score (primary outcome), as well as domains of the FXS validated version of the ABC-C (secondary outcomes). Results: The treatment was well tolerated and minimal adverse effects were reported. Significant improvement in the primary outcome (P < 0.005), as well as in secondary outcomes, were observed in the majority of the subjects (12/15). Conclusions: We believe long-term sustained treatment with diseased-modifying drugs would be necessary in order to improve behaviour and learning. Lovastatin, well known for its long-term security profile, reveals itself as a strong candidate to that purposes. Nevertheless, a larger placebo-controlled trial of lovastatin in this population is warranted in order to confirm its efficacy.
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Functional Dysregulation in Stress-Induced Modulation of Synaptic Plasticity in a Mouse Model of Fragile X SyndromeGhilan, Mohamed 30 April 2015 (has links)
The fragile X mental retardation protein (FMRP) is an important regulator of protein translation, and a lack of FMRP expression leads to a cognitive disorder known as fragile X syndrome (FXS). Clinical symptoms characterizing FXS include learning impairments and heightened anxiety in response to stressful situations. The Fmr1-/y mouse has previously been shown to have deficits in context discrimination and novel object recognition tasks, which primarily rely on the dentate gyrus (DG) region of the hippocampal formation, but not in the Morris water maze (MWM) or the elevated plus-maze tasks, which primarily depend on the Cornu Ammonis (CA1) region. Furthermore, previous research has demonstrated N-methyl-D-aspartate receptor (NMDAR)-associated synaptic plasticity impairments in the DG but not in the CA1. However, the impact of acute stress on synaptic plasticity in the Fmr1-/y hippocampus has not been examined. The current study sought to extend previous behavioural investigations in the Fmr1-/y mouse, as well as examine the impact of stress on activation of the hypothalamic-pituitary-adrenal (HPA)-axis and on hippocampal synaptic plasticity. To further characterize hippocampus-dependent behaviour in this mouse model, the DG-dependent metric change spatial processing and CA1-dependent temporal order discrimination tasks were evaluated. The results reported here support previous findings and demonstrate that Fmr1-/y mice have performance deficits in the DG-dependent task but not in the CA1-dependent task, suggesting that previously reported subregional differences in NMDAR-associated synaptic plasticity deficits in the hippocampus of the Fmr1-/y mouse model may also manifest as selective behavioural deficits in hippocampus-dependent tasks. In addition, following acute stress, mice lacking FMRP showed a faster elevation of the glucocorticoid corticosterone and a more immediate impairment in long-term potentiation (LTP) in the DG. Stress-induced LTP impairments were rescued by administering the glucocorticoid receptor (GR) antagonist RU38486. Administration of RU38486 also enhanced LTP in Fmr1-/y mice in the absence of acute stress to wild-type levels, and this enhancement was blocked by application of the NMDAR antagonist 2-amino-5-phosphonopentanoic acid. These results suggest that a loss of FMRP results in enhanced GR signalling that may adversely affect NMDAR-dependent synaptic plasticity in the DG. Finally, synaptic plasticity alterations reported in this work were found to be specific to the DG and were unidirectional, i.e., restricted to LTP, as NMDAR- and metabotropic glutamate receptor (mGluR)-LTD were both unaffected by acute stress in the DG or the CA1 regions. This study offers new insights into synaptic plasticity impairments in the Fmr1-/y mouse model, and suggests stress and GRs as important contributors to learning and memory deficits in FXS. / Graduate
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ANÁLISE MOLECULAR DE PACIENTES COM SUSPEITA DA SÍNDROME DO X-FRÁGILAmancio, Andreia Pires 31 January 2013 (has links)
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Previous issue date: 2013-01-31 / The Intellectual Disability (DM) is defined as an incomplete level of intellectual
development, and its manifestation usually occurs before 18 years of age. It is one of
the most common neuropsychiatric disorders, with a prevalence of 5% in our
population. The Fragile X syndrome (FXS) is the most common cause of inherited
mental retardation worldwide, and the second most common genetic cause of mental
retardation. The phenotype of FXS is associated with mutations in FMR1 (Fragile X
Mental Retardation-linked type 1), which is caused by the expansion of repetition of a
trinucleotide sequence (CGG) in the regulatory region of the FMR1 gene, located on
chromosome X (Xq27 .3). The importance of clinical recognition and specific
diagnosis of FXS comes from the fact that theoretically all cases are hereditary and
familial. In this context, this study aimed to validate the molecular genetic diagnosis
simplified and cost, for patients suspected of FXS in the Laboratory of Cytogenetics
and Molecular Genetics (LaGene) of the Department of Health of the State of Goiás
in Goiânia using the PCR technique. We selected 35 patients referred by medical
service of public health to LaGene with clinical indication for diagnosis of FXS. The
patients' DNA was extracted and subjected to two PCR methods, here called PCR
Screening (PCR-T) and PCR for Pre-mutation (PCR-P). The new methodology, PCRT,
88% produced conclusive results against 100% conclusiveness of the standard
technique (PCR-P) and getting a p> 0.11. The alleles amplified by PCR-P allowed
the diagnosis of pre-mutation in a sample. From these observations we propose a
strategy for the diagnosis of the syndrome using PCR-P research in pre-mutation
individuals in parents with inconclusive results. Given the successful results and
improved the PCR, including the new and easy diagnosis of pre-mutation samples
not completed by the technique of drawing, we suggest the implementation of both
PCR genetics laboratory in the State of Goiás (LaGene ) for the diagnosis of FXS. / A Deficiência Mental (DM) é definida como sendo um nível incompleto do
desenvolvimento intelectual, e sua manifestação ocorre normalmente antes dos 18
anos de idade. É um dos transtornos neuropsiquiátricos mais comuns, com uma
prevalência de 5% na população brasileira. A síndrome do X-Frágil (SXF) é a causa
mais comum de retardo mental hereditário em todo o mundo, e a segunda causa
genética mais frequente de deficiência mental. O fenótipo da SXF está associado a
mutações no gene FMR1 (Fragile X-linked Mental Retardation type 1), que é
causada pela expansão da repetição de uma sequência de trinucleotídeos (CGG) na
região reguladora do gene FMR1, localizado no cromossomo X (Xq27.3). A
importância do reconhecimento clínico e diagnóstico específico da SXF vem do fato
de que teoricamente todos os casos são hereditários e familiais. Nesse contexto,
este estudo teve como objetivo validar o diagnóstico genético-molecular simplificado
e de baixo custo, para pacientes com suspeita da SXF no Laboratório de
Citogenética e Genética Molecular (LaGene) da Secretaria Estadual de Saúde do
Estado de Goiás, na cidade de Goiânia, utilizando a técnica de PCR. Foram
selecionados 35 pacientes encaminhados pelo serviço médico da rede pública de
saúde ao LaGene com indicação clínica de diagnóstico da SXF. O DNA desses
pacientes foi extraído e submetido a dois métodos de PCR, aqui denominados PCR
de Triagem (PCR-T) e PCR para Pré-mutação (PCR-P). A nova metodologia, PCRT,
produziu 88% de resultados conclusivos contra 100% de conclusividade pela
técnica padrão (PCR-P) e obtendo um p>0,11. Os alelos amplificados pela PCR-P
possibilitou o diagnóstico de pré-mutação em uma amostra. A partir destas
observações propõe-se uma estratégia para o diagnóstico da síndrome utilizando a
PCR-P na pesquisa de pré-mutação em pais de indivíduos com resultados
inconclusivos. Considerando os resultados bem sucedidos e aprimorados da técnica
de PCR, incluindo o novo e fácill diagnóstico da pré-mutação de amostras não
concluídas pela técnica de triagem, sugere-se a implementação de ambas as PCR
no laboratório de genética do Estado de Goiás (LaGene) para o diagnóstico da SXF.
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Psychanalyse et génétique médicale : une rencontre possible à partir du syndrome du chromosome X fragile / Psychoanalysis and medical genetics: a possible encounter from the fragile X syndromeVarela, Andrea Sousa 05 October 2017 (has links)
Cette thèse part de la proposition d\'une rencontre possible entre psychanalyse et génétique médicale par le biais des soins offerts aux enfants porteurs de syndromes génétiques, notamment le syndrome de l\'X fragile. Nous avons trouvé dans les recherches en épigénétique une voie de rapprochement de ces différents champs du savoir. L\'idée selon laquelle l\'environnement est capable de modifier l\'expression des gènes représente la rupture d\'un certain déterminisme génétique autrefois accepté, et ouvre un espace où penser la singularité. Notre travail propose d\'élargir le concept d\'environnement, en y considérant la relation de l\'enfant avec l\'Autre, lieu du langage, comme opérateur de marques sur son corps : marques symboliques, constituées dès le tout début de la rencontre de l\'infans et de ceux qui s\'occupent de lui. C\'est justement dans cet espace d\'échange avec l\'Autre qu\'a lieu l\'émergence d\'un sujet. Nous avons opté pour les concepts de sujet et de transfert pour soutenir l\'articulation de la clinique psychanalytique et de la génétique médicale en ce qui concerne le traitement. Nous avons donc exposé trois cas cliniques issus de notre pratique, d\'enfants traversés par le diagnostic de l\'X fragile afin d\'illustrer de quelle manière les conceptions de sujet et de transfert se reflètent dans la clinique. Tenant compte que la psychothérapie est également prise comme objet d\'étude de l\'épigénétique, et qu\'elle est donc considérée comme un environnement capable de provoquer, voire de renverser des marques épigénétiques, l\'enjeu de notre travail repose sur la proposition suivante : et pourquoi pas la psychanalyse également ? La psychothérapie psychanalytique, ancrée sur le transfert, ne peut-elle pas, elle aussi, laisser des marques sur le petit patient / The current thesis assumes a possible encounter between psychoanalysis and medical genetics based on the treatment applied to children carrying genetic syndromes such as the Fragile X Syndrome. Epigenetic studies are a way to approximate different knowledge fields. The assumption that the environment is able to change gene expression strays from the genetic determinism we once believed and opens the way for us to reason about singularity. The proposition in the present study lies on expanding the concept of environment, by taking into consideration the relation between the child and the Other in the environment in question, as well as the place of language as the operator marking the childs body. These symbolic marks start emerging in the first encounter between the infans and caregivers. The subject emerges precisely 3 within an environment of exchanges that is set with the Other. The concepts of subject and transference were chosen to support the treatment articulation between psychoanalytic clinic and medical genetics. Thus, the present study reports three clinical cases followed by the authors, which involved children diagnosed with fragile X syndrome. These cases illustrate how the aforementioned concepts affect the clinical practice. Since psychotherapy has also been taken as the object of epigenetic studies, and as it is considered an environment able to cause, and even reverse, epigenetic marks, the current study relies on the following proposition: why not psychoanalysis as well? Can the psychoanalytic psychotherapy, anchored in the concept of transference, leave marks on the little patient too?
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