Novel Strategies for the Prevention of Post-Stroke Epilepsy and Sudden Unexpected Death in Epilepsy Patients

Adhikari, Yadav Prasad

10 1900

Indiana University-Purdue University Indianapolis (IUPUI) / Stroke is the second leading cause of mortality worldwide, accounting for 5.5 million deaths annually. In addition to its high mortality rate, stroke is the most common cause of acquired epilepsy. Three to thirty percent of stroke survivors develop post-stroke epilepsy. Although currently available therapies such as thrombolytics and mechanical thrombectomy prevent immediate mortality by restoring blood flow after stroke, these treatments do not target the cellular and molecular mechanisms that lead to post-stroke epileptogenesis. With the increasing number of stroke survivors, there is an urgent need for therapies that prevent epilepsy development in this population. Here, we showed that homeostatic plasticity is involved in the development of hyperexcitability after stroke and can be targeted to prevent the development of post-stroke epilepsy. Using two-photon calcium imaging, we found that homeostatic regulation leads to cortical hyperexcitability after stroke. We also found that activity enhancement by optogenetic and pharmacological approaches can target homeostatic plasticity to prevent post-stroke epilepsy. This study demonstrates the high translational potential of activity enhancement as a novel strategy to prevent post-stroke epilepsy through regulating cortical homeostatic plasticity. Sudden premature death is a leading cause of death in patients with medically refractory epilepsy. This unanticipated death of a relatively healthy person with epilepsy in which no structural or toxicological cause of death can be identified after postmortem analysis is referred to as sudden unexpected death in epilepsy patients (SUDEP). Respiratory failure during seizures is an important underlying mechanism of SUDEP. Here, we showed that LPS-induced peripheral inflammation is protective against SUDEP. This protection is mediated at least in part via enhancing serotonergic function in the brain stem. To the best of our knowledge, this is the first study demonstrating the relationship between peripheral inflammation and SUDEP prevention. / 2024-11-01

activity enhancement

D-cycloserine

homeostatic plasticity

inflammation

post-stroke epilepsy

SUDEP

Rab3A as a modulator of homeostatic synaptic plasticity

Koesters, Andrew G.

29 August 2014

No description available.

Biomedical Research

Neurobiology

Neurosciences

Physiology

Rab3A

homeostatic synaptic plasticity

GluR1

GluR2

AMPA receptor

CD24 in T lymphocyte homeostatic proliferation and autoimmune disease

Li, Ou

24 August 2005

No description available.

CD24

co-stimulatory molecule

T cell Homeostatic proliferation

EAE

autoimmune disease

Cortical Plasticity and Tinnitus

Chrostowski, Michal

10 1900

<p>Tinnitus is an auditory disorder characterized by the perception of a ringing, hissing or buzzing sound with no external stimulus. Because the most common cause of chronic tinnitus is hearing loss, this neurological disorder is becoming increasingly prevalent in our noise-exposed and ageing society. With no cure and a lack of effective treatments, there is a need for a comprehensive understanding of the neural underpinnings of tinnitus. This dissertation outlines the development and validation of a comprehensive theoretical model of cortical correlates of tinnitus that is used to shed light on the development of tinnitus and to propose improvements to tinnitus treatment strategies.</p> <p>The first study involved the development of a computational model that predicts how homeostatic plasticity acting in the auditory cortex responds to hearing loss. A subsequent empirical study validated a more biologically plausible version of this computational model. The goal of these studies was to determine whether and how a form of plasticity that maintains balance in neural circuits can lead to aberrant activity in the auditory cortex. The final study extends the validated computational model to develop a comprehensive theoretical framework characterizing the potential role of homeostatic and Hebbian plasticity in the development of most major cortical correlates of tinnitus.</p> <p>These theoretical and empirical studies provide a novel and complete description of how neural plasticity in adult auditory cortex can respond to hearing loss and result in the development of tinnitus correlates.</p> / Doctor of Philosophy (PhD)

auditory

cortical plasticity

tinnitus

homeostatic plasticity

hearing loss

Computational Neuroscience

Systems Neuroscience

Computational Neuroscience

Molecular Players in Preserving Excitatory-Inhibitory Balance in the Brain

Mao, Wenjie

07 December 2017

Information processing in the brain relies on a functional balance between excitation and inhibition, the disruption of which leads to network destabilization and many neurodevelopmental disorders, such as autism spectrum disorders. One of the homeostatic mechanisms that maintains the excitatory and inhibitory balance is called synaptic scaling: Neurons dynamically modulate postsynaptic receptor abundance through activity-dependent gene transcription and protein synthesis. In the first part of my thesis work, I discuss our findings that a chromatin reader protein L3mbtl1 is involved in synaptic scaling. We observed that knockout and knockdown of L3mbtl1 cause a lack of synaptic downscaling of glutamate receptors in hippocampal primary neurons and organotypic slice cultures. Genome-wide mapping of L3mbtl1 protein occupancies on chromatin identified Ctnnb1 and Gabra2 as downstream target genes of L3mbtl1-mediated transcriptional regulation. Importantly, partial knockdown of Ctnnb1 by itself prevents synaptic downscaling. Another aspect of maintaining E/I balance centers on GABAergic inhibitory neurons. In the next part of my thesis work, we address the role of the scaffold protein Shank1 in excitatory synapses onto inhibitory interneurons. We showed that parvalbumin-expressing interneurons lacking Shank1 display reduced excitatory synaptic inputs and decreased levels of inhibitory outputs to pyramidal neurons. As a consequence, pyramidal neurons in Shank1 mutant mice exhibit increased E/I ratio. This is accompanied by a reduced expression of an inhibitory synapse scaffolding protein gephyrin. These results provide novel insights into the roles of chromatin reader molecules and synaptic scaffold molecules in synaptic functions and neuronal homeostasis.

synaptic plasticity

homeostatic plasticity

homeostatic scaling

synaptic scaling

excitatory and inhibitory balance

hippocampus

epigenetics

chromatin reader

MBT

interneuron

parvalbumin

shank

synaptic scaffolding molecule

autism spectrum disorders

mouse model

Molecular and Cellular Neuroscience

Neuroplastische Effekte repetitiver anodaler transkranieller Gleichstromstimulation des motorische Kortex / Effects of neuroplasticity by repetitive anodal transcranial direct current stimulation on the human motor cortex

Hessenthaler, Silvia

28 January 2013

No description available.

610

Neuroplasticity

Brain stimulation

tDCS

l-LTP

repetitive anodal tDCS

homeostatic plasticity

Flunarizin

learning and memory

Computational Simulation and Analysis of Neuroplasticity

Yancey, Madison E.

03 June 2021

No description available.

Computer Science

Statistics

Neurosciences

Neurobiology

Mathematics

Biology

computer science

neuroscience

homeostatic synaptic plasticity

neuron

statistics

graphical user interface

software application

Impact de la maladie du greffon contre l’hôte sur la reconstitution immunitaire suite à une greffe de moelle osseuse allogénique

Gauthier, Simon-David

08 1900

La transplantation allogénique de cellules souches hématopoïétiques est une technique très efficace pour traiter différents cancers du sang. Malheureusement la réaction du greffon contre l’hôte (GVHD) demeure la cause principale de morbidité et de mortalité post-greffe. La GVHD entraîne une diminution de la reconstitution immunitaire ce qui accentue considérablement l’immunosuppression associée à ce traitement et de ce fait augmente les risques d’infection et de rechute. Notre laboratoire a démontré précédemment que les niveaux élevés d’IL-7 dans des hôtes lymphopéniques interféraient avec la capacité des cellules dendritiques (DC) à soutenir la prolifération homéostatique (PH) des lymphocytes T CD4+. Puisque les niveaux d’IL-7 sont aussi élevés dans un contexte de GVHD, nous avons émis l’hypothèse que la signalisation de l’IL-7 sur les DC pouvait contribuer à diminuer la reconstitution immunitaire des lymphocytes T CD4+. Pour répondre à cette question, nous avons utilisé le modèle murin de GVHD C57BL/6 (B6) dans B6D2F1. Afin de régénérer une niche hématopoïétique permissive à la PH des lymphocytes T CD4+, nous avons transplanté des souris B6D2F1 avec de la moelle osseuse de souris B6 IL-7Rα-/-. La GVHD a été induite en transférant des lymphocytes T B6 réactifs aux cellules B6D2F1. Dans les souris contrôles, la PH des lymphocytes T CD4+ est maintenue. Par contre, la PH est absente dans les souris en GVHD malgré la présence d’une niche périphérique qui ne répond pas à l’IL-7. L’absence de PH des lymphocytes T CD4+ durant la GVHD est associée à une diminution du nombre de DC. En utilisant un test de cytotoxicité in vivo nous démontrons que les DC B6 générées dans une hôte B6D2F1 sont éliminées par les lymphocytes T B6 alloréactifs. En conclusion, nos résultats démontrent que l’immunosuppression associée à la GVHD est en partie causée par une élimination des DC par les lymphocytes T allogéniques. Nous postulons donc que la perte des DC, et non la signalisation de l’IL-7 sur les DC, est le facteur limitant la PH des lymphocytes T CD4+ durant la GVHD. / Allogeneic hematopoietic stem cell transplantation (SCT) is an effective treatment for numerous types of haematological malignancies. However, graft-versus-host disease (GVHD) remains the major cause of morbidity and mortality following SCT. GVHD is associated with poor immune reconstitution and its adverse effect on T cell regeneration greatly exaggerates the immunodeficiency normally associated with SCT. As a result, patients experiencing GVHD present deficit in T cells that can last for several years. Our laboratory has demonstrated that elevated systemic IL-7 found during lymphopenia can interfere with the capacity of dendritic cells (DC) to support the homeostatic proliferation (HP) of CD4+ T cells. Since IL-7 levels are also elevated during GVHD, we hypothesized that IL-7 signaling in DC could also contribute to diminished T cell reconstitution in this setting. We used the well describe GVHD mouse model C57BL/6 (B6) into B6D2F1 to study the contribution of IL-7 signalling in DC on CD4+ T cell regeneration during GVHD. To regenerate a peripheral niche permissive for CD4+ T cells HP, we transplanted B6D2F1 mice with bone marrow (BM) from B6 IL-7Rα-/- mice. Finally, GVHD was induced with 1x106 of alloreactive B6 T cells. In control mice transplanted with IL-7Rα-/- BM cells, CD4+ T cells HP is efficiently supported. In contrast, CD4+ HP is completely abrogated in GVHD mice despite the presence of a peripheral niche that does not signal IL-7. Loss of CD4+ HP during GVHD was associated with diminished number of DC. Using an in vivo cytotoxic assay, we demonstrated that B6 DC can be eliminated by alloreactive B6 T cells when these cells developed into B6D2F1 hosts. In conclusion, our data demonstrates that the immunosuppression associated with GVHD is in part related to the elimination of donor-derived DC by donor alloreactive T cells. Therefore, we postulate that loss of DC, and not IL-7 signaling in DC, represents the limiting factor that contains CD4+ HP during GVHD.

GVHD

GVHD

reconstitution immunitaire

immune reconstitution

lymphocyte T CD4+

CD4+ T cells

cellule dendritique

dendritic cells

prolifération homéostatique

homeostatic proliferation

Development of regulatory T cells and induction of mucosa-specific homing

Siewert, Christiane

11 December 2007

Bei der Aufrechterhaltung des homeostatischen Gleichgewichts und der peripheren Selbst-Toleranz spielen CD4+CD25+ regulatorische T-Zellen (Tregs) eine wichtige Rolle. In Vorarbeiten wurden Subpopulationen von murinen CD4+ Tregs identifiziert, die sich durch die Expression des Integrins alphaE auszeichnen. Diese alphaE+ Treg Subpopulationen weisen einen Effektor/Memory-ähnlichen Phänotyp auf. In der vorliegenden Dissertation wurde untersucht, welche Bedingungen zur Entwicklung von alphaE+ Effektor/Memory Tregs in vivo führen und aus welchen Vorläuferzellen sie entstehen. Dabei zeigte sich, dass es sich bei den alphaE+ Tregs um Effektor/Memory T-Zellen handelt, die unter physiologischen Bedingungen in vivo ein hohes Maß an Zellteilung aufweisen, welche zum Teil abhängig von der bakteriellen Besiedelung des Darms ist. Darüber hinaus wurde beobachtet, dass alphaE+ Tregs nach oraler, antigen-spezifischer Aktivierung in den darm-assozierten lymphoiden Geweben sowohl aus konventionellen naiven CD4+ T-Zellen, als auch aus thymus-generierten naiven CD4+CD25+ Tregs entstehen können. Zusammenfassend deuten die erzielten Ergebnisse darauf hin, dass das spezifische mukosale Mikroenvironment sowohl die Expansion als auch Konvertierung von Tregs fördert und so eine wichtige Rolle für die Aufrechterhaltung der Homeostase von alphaE+Foxp3+ Tregs spielt. Zudem wurde in dieser Arbeit die Ausbildung von gewebespezifischen Homingrezeptor-Phänotypen von naiven CD4+CD25+ Tregs untersucht. In in vitro Kultur-Systemen zeigte sich, dass selektive Modulation von Tregs, ähnlich wie bei konventionellen T-Zellen, die Induktion von organspezifischen Migrationseigenschaften ermöglicht. So konnte eine effiziente Wanderung von Tregs in den Darm ausgelöst werden. Diese Daten legen den Schluss nahe, dass die Herstellung von Tregs mit spezifischen Wanderungseigenschaften eine Option für therapeutische Anwendungen in der adoptiven T-Zell Therapie sein könnte. / Regulatory CD4+CD25+ T cells (Tregs) play an important role in immune homeostasis and in the maintenance of self-tolerance. Previously, subsets of murine CD4+ Tregs characterised by expression of the integrin alphaE had been identified. These alphaE+ Treg subsets display an effector/memory-like phenotype. In the present study the circumstances favouring in vivo generation of effector/memory-like alphaE+ Tregs were analysed. The results presented here show that alphaE+ effector/memory-like Treg subsets contain a large fraction of cycling cells under physiologic conditions in healthy mice. This in vivo proliferation depended, at least in part, on intestinal commensal microflora. Furthermore, it was observed that alphaE+ Tregs not only developed by differentiation of naive-like CD4+CD25+ Tregs, but were also generated de novo from naive CD4+ T cells in the gut-associated lymphoid tissue upon oral antigen delivery. Taken together, these results indicate that the mucosal microenvironment favours both expansion and conversion of Tregs and thereby represents an important mechanism for the homeostatic maintenance of alphaE+Foxp3+ Tregs. In addition, susceptibility of naive CD4+CD25+ Tregs to acquire tissue-specific homing receptor phenotypes was investigated. In vitro culture systems demonstrated that Tregs, similarly to conventional T cells, could be configured with organ-selective homing properties allowing efficient targeting into the gut. These results suggest that generation of Tregs with specific homing properties for therapeutic purposes in adoptive T cell therapy might be a feasible option.

regulatorische T-Zellen

alphaE

homeostatische Proliferation

organspezifische Migration

regulatory T cells

alphaE

homeostatic proliferation

organ-specific migration

570 Biowissenschaften, Biologie

32 Biologie

WF 9895

ddc:570

Estudo das interações do lado da demanda com o mercado de energia elétrica no contexto das redes elétricas inteligentes / Study of interactions between the demand-side and the electricity market in the context of smart grids

Carrijo, Artur da Silva

18 December 2013

Made available in DSpace on 2017-07-10T17:11:46Z (GMT). No. of bitstreams: 1 DISSERTACAO ARTUR CARRIJO2.pdf: 2100488 bytes, checksum: 46e631e94e2bb6d4c69d8d2891f6e200 (MD5) Previous issue date: 2013-12-18 / The electricity market has many participants performing various roles. In the context of Smart Grids, it expands the number of participating agents and, consequently, the number, the competition and complexity of the interactions between them. The competition allows consumersto discover and explore energy sources of low cost but requires the consumer other interactions beyond the traditional relationship with the distribution company (distco). With the redefinition of the role of the consumer as a result of his active participation in the balance between supply and demand of energy, it becomes necessary to identify their interactions with the other participants, tasks, systems, subsystems and functions important to actively contribute to this balance. These interactions, called interfaces, are characterized by information that actors communicate itself to perform its functions of information collection and control tasks related to market equilibrium. The determination of these interfaces is not a trivial task because of the various alternatives for integration of the demand side. Different types and combinations of interactions between the supplier and its customers are possible. In this work will be used as a basis for discussion a concept of balance between generation and demand called homeostatic control, initially designed for a scenario of a vertically integrated monopoly. It will be studied the interactions of the consumer using the concept of homeostatic control expanded to consider the functions of demand control and integration of distributed generation and a market model that allows for consumer empowerment and within the paradigm of smart grids. / O mercado de energia elétrica possui diversos participantes exercendo vários papéis. No contexto das redes elétricas inteligentes, amplia-se o número de agentes participantes e, consequentemente, o número, a competição e a complexidade das interações entre eles. A competição permite aos consumidores descobrir e explorar fontes de baixo custo, mas requer do consumidor outras interações além da tradicional relação com a empresa distribuidora. Com a redefinição do papel do consumidor, resultado da participação ativa no processo de equilíbrio entre suprimento e demanda de energia, torna-se necessário identificar suas interações com os demais participantes, tarefas, sistemas, subsistemas e funções, importantes para que contribua ativamente com esse equilíbrio. Estas interações, denominadas interfaces, são caracterizadas pelas informações que os atores comunicam em si para executar suas funções de coleta de informações e tarefas de controle relacionadas ao equilíbrio do mercado. A determinação destas interfaces não é uma tarefa trivial em razão das diversas alternativas de integração do lado da demanda. São possíveis diferentes tipos e combinações de interações entre o fornecedor e seus clientes. Neste trabalho será utilizado como base de discussão um conceito de equilíbrio entre geração e demanda denominado controle homeostático, desenhado inicialmente para um cenário de monopólio verticalmente integrado. Serão estudadas as interações do consumidor utilizando o conceito de controle homeostático ampliado para considerar as funções de controle da demanda e a integração da geração distribuída em um modelo de mercado que permite o empoderamento do consumidor dentro do paradigma das redes elétricas inteligentes.

resposta da demanda

redes elétricas inteligentes

mercados de energia

controle homeostático

demand response

smart grids

energy markets

homeostatic control