MicroRNAs' role in brain development and disease

Fineberg, Sarah Kathryn

01 May 2010

MicroRNA (miRNA) function is required for normal animal development, in particular in stem cell and precursor populations. I hypothesize that miRNAs are similarly required for stem cell maintenance and appropriate fate commitment in the brain. To test the requirement for global microRNA production, I depleted the microRNA biosynthetic enzyme DICER in the developing mouse brain. I found that DICER loss in embryonic neural progenitor cells leads to embryonic lethality with microcephaly. By histological analysis, I found defects in both neural progenitor cell maintenance and cell differentiation. I also identified new candidate microRNAs for this phenotype by profiling miRNAs in DICER-depleted and control cells. Three microRNAs which are good candidates to modulate nervous differentiation are miR-23b, -182, and -34a. I describe the expression pattern and functional characterization of these candidates. In particular, miR-34a depletes neuron production after progenitor cell differentiation in culture, likely by modulating cell cycling and Notch pathway genes.

corticogenesis

Dicer

differentiation

microRNA

neural progenitor cell

Notch

Biophysics

Oscillatory expression of Hes1 regulates cell proliferation and neuronal differentiation in the embryonic brain / Hes1遺伝子の発現振動は胎生期の脳において細胞増殖や神経分化を制御する

Ochi, Shohei

25 May 2020

京都大学 / 0048 / 新制・課程博士 / 博士(医学) / 甲第22639号 / 医博第4622号 / 新制||医||1044(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 林 康紀, 教授 伊佐 正, 教授 斎藤 通紀 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

Hes1

neural development

neural progenitor cell

oscillation

490

Aberrant hippocampal neurogenesis contributes to learning and memory deficits in a mouse model of repetitive mild traumatic brain injury

Greer, Kisha

02 October 2019

Adult hippocampal neurogenesis, or the process of creating new neurons in the dentate gyrus (DG) of the hippocampus, underlies learning and memory capacity. This cognitive ability is essential for humans to operate in their everyday lives, but cognitive disruption can occur in response to traumatic insult such as brain injury. Previous findings in rodent models have characterized the effect of moderate traumatic brain injury (TBI) on neurogenesis and found learning and memory shortfalls correlated with limited neurogenic capacity. While there are no substantial changes after one mild TBI, research has yet to determine if neurogenesis contributes to the worsened cognitive outcomes of repetitive mild TBI. Here, we examined the effect of neurogenesis on cognitive decline following repetitive mild TBI by utilizing AraC to limit the neurogenic capacity of the DG. Utilizing a BrdU fate-labeling strategy, we found a significant increase in the number of immature neurons that correlate learning and memory impairment. These changes were attenuated in AraC-treated animals. We further identified endothelial cell (EC)-specific EphA4 receptor as a key mediator of aberrant neurogenesis. Taken together, we conclude that increased aberrant neurogenesis contributes to learning and memory deficits after repetitive mild TBI. / Doctor of Philosophy / In the United States, millions of people experience mild traumatic brain injuries, or concussions, every year. Patients often have a lower ability to learn and recall new information, and those who go on to receive more concussions are at an increased risk of developing long-term memory-associated disorders such as dementia and chronic traumatic encephalopathy. Despite the high number of athletes and military personnel at risk for these disorders, the underlying cause of long-term learning and memory shortfalls associated with multiple concussions remains ill defined. In the brain, the hippocampus play an important role in learning and memory and is one of only two regions in the brain where new neurons are created from neural stem cells through the process of neurogenesis. Our study seeks to address the role of neurogenesis in learning and memory deficits in mice. These findings provide the foundation for future, long-term mechanistic experiments that uncover the aberrant or uncontrolled processes that derail neurogenesis after multiple concussions. In short, we found an increase in the number of newborn immature neurons that we classify as aberrant neurogenesis. Suppressing this process rescued the learning and memory problems in a rodent model of repeated concussion. These findings improve our understanding of the processes that contribute to the pathophysiology of TBI.

multiple concussions

neural stem cell

neural progenitor cell

neuroblast

hippocampus

Effects of Altered Gtf2i and Gtf2ird1 Expression on the Growth of Neural Progenitors and Organization of the Mouse Cortex

Oh, Hyemin

09 December 2013

Williams Beuren syndrome Syndrome (WBS) and 7q11.23 Duplication Syndrome (Dup7) are rare neurodevelopmental disorders associated with a range of cognitive and behavioural symptoms, caused by the deletion and duplication, respectively, of 26 genes on human chromosome 7q11.23. I have studied the effects of deletion or duplication of two candidate genes, GTF2I and GTF2IRD1, on neural stem cell growth and neurogenesis using cultured primary neuronal precursors from mouse models with gene copy number changes. I found that the number of neuronal precursors and committed neurons was directly related to the copy number of these genes in the mid-gestation embryonic cortex. I further found that in late-gestation embryos, cortical thickness was altered in a similar gene dose-dependent manner, in combination with layer-specific changes in neuronal density. I hypothesize that some of the neurological features of WS and Dup7 stem from these impairments in early cortical development.

Neurodevelopmental disorder

Williams-Beuren Syndrome

Neural progenitor cell

neural stem cell

Neuroscience

0317

Effects of Altered Gtf2i and Gtf2ird1 Expression on the Growth of Neural Progenitors and Organization of the Mouse Cortex

Oh, Hyemin

09 December 2013

Williams Beuren syndrome Syndrome (WBS) and 7q11.23 Duplication Syndrome (Dup7) are rare neurodevelopmental disorders associated with a range of cognitive and behavioural symptoms, caused by the deletion and duplication, respectively, of 26 genes on human chromosome 7q11.23. I have studied the effects of deletion or duplication of two candidate genes, GTF2I and GTF2IRD1, on neural stem cell growth and neurogenesis using cultured primary neuronal precursors from mouse models with gene copy number changes. I found that the number of neuronal precursors and committed neurons was directly related to the copy number of these genes in the mid-gestation embryonic cortex. I further found that in late-gestation embryos, cortical thickness was altered in a similar gene dose-dependent manner, in combination with layer-specific changes in neuronal density. I hypothesize that some of the neurological features of WS and Dup7 stem from these impairments in early cortical development.

Neurodevelopmental disorder

Williams-Beuren Syndrome

Neural progenitor cell

neural stem cell

Neuroscience

0317

Functional studies of the Quaking gene : Focus on astroglia and neurodevelopment

Radomska, Katarzyna

January 2014

The RNA-binding protein Quaking (QKI) plays a fundamental role in post-transcriptional gene regulation during mammalian nervous system development. QKI is well known for advancing oligodendroglia differentiation and myelination, however, its functions in astrocytes and embryonic central nervous system (CNS) development remain poorly understood. Uncovering the complete spectrum of QKI molecular and functional repertoire is of additional importance in light of growing evidence linking QKI dysfunction with human disease, including schizophrenia and glioma. This thesis summarizes my contribution to fill this gap of knowledge.         In a first attempt to identify the QKI-mediated molecular pathways in astroglia, we studied the effects of QKI depletion on global gene expression in the human astrocytoma cell line. This work revealed a previously unknown role of QKI in regulating immune-related pathways. In particular, we identified several putative mRNA targets of QKI involved in interferon signaling, with possible implications in innate cellular antiviral defense, as well as tumor suppression. We next extended these investigations to human primary astrocytes, in order to more accurately model normal brain astrocytes. One of the most interesting outcomes of this analysis was that QKI regulates expression of transcripts encoding the Glial Fibrillary Acidic Protein, an intermediate filament protein that mediates diverse biological functions of astrocytes and is implicated in numerous CNS pathologies. We also characterized QKI splice variant composition and subcellular expression of encoded protein isoforms in human astrocytes. Finally, we explored the potential use of zebrafish as a model system to study neurodevelopmental functions of QKI in vivo. Two zebrafish orthologs, qkib and qki2, were identified and found to be widely expressed in the CNS neural progenitor cell domains. Furthermore, we showed that a knockdown of qkib perturbs the development of both neuronal and glial populations, and propose neural progenitor dysfunction as the primary cause of the observed phenotypes.        To conclude, the work presented in this thesis provides the first insight into understanding the functional significance of the human QKI in astroglia, and introduces zebrafish as a novel tool with which to further investigate the importance of this gene in neural development.

QKI

RNA-binding protein

astrocyte

interferon

GFAP

neurodevelopment

zebrafish

neural progenitor cell

Mesenchymal Stromal Cells to Treat Lung and Brain Injury in Neonatal Models of Chronic Lung Disease

Lithopoulos, Marissa Athena

13 May 2021

Preterm birth (<37 weeks) is the world’s principal cause of death of children <5 years of age. Bronchopulmonary dysplasia (BPD) is the most common complication of preterm birth. BPD is characterized by an arrest in alveolar and vascular development within the lung. It is a multifactorial disease, caused by a combination of supplemental oxygen, mechanical ventilation, and inflammation. BPD is also an independent risk factor for abnormal neurodevelopment. The link between BPD and abnormal neurodevelopment is poorly understood and there are currently no effective cures for these complications. We hypothesized that a crucial cell population for brain development, i.e., the neural progenitor cell (NPC) is functionally impaired in BPD and that this impairment is associated with abnormal neurodevelopment. Based on our previous findings, we also predicted that human umbilical cord-mesenchymal stromal cell (UC-MSC) extracellular vesicles (EVs), could mitigate both the lung and brain injuries in experimental BPD. We utilized several animal models of BPD, across multiple species, to determine the effects of hyperoxia, mechanical ventilation, and inflammation on the developing lungs and brain. We also utilized UC- MSC therapy to mitigate these injuries. We discovered that hyperoxia exposure damages the developing lungs as well as the brain, leading to cerebrovascular and NPC impairments, as well as reduced neurogenesis. These impairments were associated with neurobehavioural deficits in adulthood. Furthermore, we found that inflammation in combination with mechanical ventilation and hyperoxia also impairs NPC function. Importantly, we demonstrated that UC-MSC EVs can reduce inflammation, improve vascular growth, restore lung growth, and mitigate impairments in NPC self-renewal. This work highlights novel mechanisms of BPD-associated abnormal neurodevelopment and offers potential regenerative medicine therapies to alleviate these outcomes for this vulnerable population.

Mesenchymal stromal cells

Neonatal lung disease

Bronchopulmonary dysplasia

Neural progenitor cell

Neurodevelopment

Extracellular vesicles

The Roles of ERK1 and ERK2 MAP Kinase in Neural Development and Disease

Samuels, Ivy S.

22 July 2008

No description available.

Biomedical Research

Mitogen-activated protein kinase

cortical development

neural progenitor cell

Induction of neurogenesis in the neocortex after ischemic brain injury by manipulation of endogenous neural progenitors

Cancelliere, Alessandro

13 July 2009

No description available.

Biomedical Research

neurogenesis

ischemia

neural progenitor cell

neocortex,

IGF-I, stroke

Transcriptional Insights for Spinal Cord Injury and Neural Precursor Cell Therapy: Toward a Novel Optogenetics-Based Treatment for cAMP Neuronal Induction

Martínez Rojas, Beatriz

08 March 2024

[ES] La lesión medular traumática (LM) se refiere a una condición neurológica en la que un insulto mecánico interrumpe la adecuada comunicación de impulsos nerviosos a través del sistema nervioso central (SNC), resultando en la pérdida de función locomotora por debajo del área lesionada. Lamentablemente, en la actualidad aún no existe cura efectiva para restaurar la funcionalidad después de una LM. La búsqueda de un tratamiento eficiente sigue siendo un gran desafío debido a nuestra aún incompleta comprensión de la multitud de procesos biológicos desencadenados por la lesión. La terapia celular destaca como la aproximación más recurrente para el tratamiento de la LM. En las últimas décadas, se han explorado varias estrategias celulares, siendo una de las más prometedoras el trasplante de células progenitoras neurales (CPN). Muchos estudios preclínicos demostrado el potencial del trasplante de CPN para proporcionar una recuperación motora en modelos animales, sin embargo, las mejoras funcionales en ensayos clinicos humanos son limitadas. Por lo tanto, aún se deben realizar esfuerzos para descubrir la cascada precisa de procesos moleculares a lo largo de la fisiopatología de LM, así como el mecanismo subyacente de los CPN. En ese contexto, el Capítulo 1 del presente trabajo tuvo como objetivo proporcionar una caracterización de los cambios en el perfil transcripcional medular a lo largo de las diferentes etapas temporales de una lesión severa contusiva. Además, hemos descrito el impacto transcripcional del trasplante de CPN en ratas lesionadas. Hemos demostrado que mientras la LM conllevó una fuerte desregulación de varios componentes de señalización de AMPc (entre ellos EPAC2), el trasplante de CPN pudo restaurar estas alteraciones transcripcionales. Para explorar el papel de EPAC2 en el mecanismo terapéutico mediado por CPN, realizamos un experimento de inhibición sostenida de EPAC2 mediante la administración de ESI-05. En comparación con los animales solo trasplantados, los animales CPN +ESI-05 mostraron un aumento en el área de cicatriz, una exacerbación de la polarización de la microglía hacia un perfil inflamatorio y una ampliación de la brecha de neuronas preservadas a lo largo de la lesión, sugiriendo que el trnasplante de CPN en el contexto de LM implican un mecanismo dependiente de EPAC2, reduciendo la neuroinflamación y proporcionando un entorno neuro-permisivo. El Capítulo 2 explora el potencial del AMPc para la regeneración de la LM. Hemos diseñado una estrategia innovadora para inducir AMPc en las neuronas corticoespinales a través de la activación optogenética de un adenilato ciclasa foto-inducible (bPAC). La estimulación optogenética en ratas con una hemisección dorsal torácica promovió una recuperación locomotora en comparación con el grupo control. Además, la estimulación de bPAC aumentó el número de neuronas marcadas retrógradamente desde el segmento lumbar tanto en la corteza motora como en la formación rafe-reticular, pero no en el núcleo rojo.La inmunotinción del tracto rafespinal mostró que la estimulación de bPAC aumenta el ratio de axones serotonérgicos caudales a la lesión correlacionando con una mejora funcional. Por último, la depleción del sistema serotoninérgico mediante la administración de 5,7-Dihydroxytryptamina suprimió la abolió la mejora mediada por bPAC, confirmando la implicación de la vía serotoninérgica en la recuperación de los animales estimulados. En resumen, se han proporcionado nuevos conocimientos sobre los cambios transcripcionales que ocurren a lo largo de la progresión de la LM y tras el trasplante de CPN, con énfasis en la señalización de AMPc. La manipulación optogenética de AMPc en las neuronas corticoespinales después de la LM ha demostrado ser efectiva para la recuperación funcional y permitido descubrir una ruta cortical alternativa a través del tracto descendente serotoninérgico / [CA] Lesió medul·lar traumàtica (LM) es una condició neurològica en la qual un traumatisme interromp la comunicació adequada dels impulsos a través del sistema nerviós central (SNC), amb el resultat de la pèrdua de la funció locomotora per baix de la zona lesionada. Lamentablement, en l'actualitat encara no hi ha una cura efectiva per a restaurar completament la funcionalitat de la medul·la espinal després de la lesió. La recerca d'un tractament eficient per a la LM roman un repte complex a causa de la nostra comprensió encara incompleta de la gran quantitat de processos biològics desencadenats per la lesió primària. La teràpia cel·lular destaca com l'aproximació més recurrent per al tractament de la LM. En les dècades passades, s'ha explorat diverses estratègies basades en cèl·lules i una de les més prometedores és el trasplantament de cèl·lules progenitores neurals (CPN). Molts estudis preclínics han demostrat el potencial del trasplantament de CPN per proporcionar una recuperació motora en models animals, no obstant això, les millores funcionals en pacients humans tractats són limitades. Per tant, encara s'han de fer esforços per a descobrir la cascada precisa de processos moleculars al llarg de la fisiopatologia de la LM, així com el mecanisme subjacent dels CPN. El Capítol 1 del present treball va tindre com a objectiu proporcionar una caracterització dels canvis en el perfil transcripcional espinal al la llarga de les diferents etapes temporals de una lesió contusiva. A més, s'ha descrit l'impacte transcripcional del trasplantament d'CPN en animals lesionats. S'ha demostrat que mentre la LM va causar una forta desregulació de diversos components de senyalització de AMPc (sent EPAC2 el gen més regulat a la baixa), el transplantament de CPN van ser capaç de restaurar les alteracions derivades de la LM. Per a explorar el paper d'EPAC2 en el mecanisme terapèutic mediat per CPN, es va realitzar un experiment de inhibició sostinguda d'EPAC2 degut a l'administració d'ESI en animals lesionats. En comparació amb els animals només trasplantats, els animals CPN+ESI-05 van mostrar un augment de l'àrea de cicatriu, una exacerbació de la polarització de les micròglies cap a un perfil inflamatori i una ampliació de la bretxa de neurones preservades a través de la lesió.Aquests resultats suggereixen que el trasplantament de CPN en el context de la LM involucren un mecanisme depenent d'EPAC2, reduint la neuroinflamació i proporcionant un entorn més neuropermissiu. El Capítol 2 va tindre com objectiu explotar el potencial de regeneració de AMPc dissenyant una nova estratègia per a les induccions artificials de AMPc en les neurones corticoespinals mitjançant l'activació optogenètica d'una adenilat ciclasa fotoinduïble (bPAC). L'estimulació diària de AMPc en rates que pateixen una hemisècció dorsal toràcica va promoure una recuperació en comparació amb els control. L'estimulació de bPAC va augmentar el nombre de neurones marcades retrògradament des del segment lumbar, tant a l'escorça motora com a la formació rafe-reticular, però no al nucli roig. A més, la immunotinció del tracte rafespinal va mostrar que l'estimulació de bPAC va augmentar la ràtio d'axons serotoninèrgic cabals a la lesió, cosa que es va correlacionar significativament amb una millora dels paràmetres funcionals. Finalment, la depleció del sistema serotoninèrgic mitjançant l'administració de 5,7-Dihydroxytryptamina va abolir la millora mediada per bPAC, confirmant la implicació de la via serotoninèrgica en la recuperació. En resum, la investigació ha proporcionat coneixements sobre els canvis transcripcionals que tenen lloc a la llarga de la progressió de la LM i després del trasplantament de CPN, amb un èmfasi especial en la senyalització d'AMPc. La manipulació optogenètica d'AMPc a les neurones corticoespinals després de la LM ha demostrat ser efectiva per a la recuperació funcional i ha permès descobrir una ruta cortical alternativa a través del tracte descendent serotoninèrg / [EN] Traumatic spinal cord injury (SCI) refers to a neurological condition in which a mechanic insult disrupts the proper communication of the impulses through the central nervous system (CNS), resulting on the loss of locomotor function below the injured area. Unfortunately, nowadays there is still no effective cure to completely restore the functionality of the spinal cord after the injury. Cell therapy is the most recurring approach for SCI treatment. In the past decades several cell-based strategies have been explored, being one of the most promising the transplantation of neural progenitor cells (NPCs). Many pre-clinical studies evidenced the potential of the NPCs transplantation to provide a substantial motor recovery in animal models, yet functional improvements in clinical trials have been limited. Therefore, efforts still need to be made in disclosing the precise cascade of molecular processes along SCI pathophysiology as well as the NPCs underlying mechanism. In that context, Chapter 1 of the present work aimed to provide a comprehensive characterization of the spinal transcriptional changes along the different temporal stages of rats suffering a severe contusive injury. Additionally, we have described the transcriptional impact of acute and subacute NPCs transplantation in injured animals. Interestingly we have shown that while SCI caused a strong dysregulation of several cAMP-signaling components (being EPAC2 the most downregulated gene), NPCs was able to restore SCI-derived alterations over this pathway with EPAC2 significant upregulation. In order to further explore EPAC2 role in NPCs-mediated therapeutical mechanism we performed a loss-of-function experiment by sustained EPAC2 inhibition via ESI-05 administration along with NPCs transplantation after SCI. Compared with only transplanted animals, NPCs+ESI-05 animals showed increased scar area, exacerbated microglia polarization into an inflammatory profile and widened gaps of preserved neurons across the lesion. Overall, these results suggest that NPC therapeutic mechanisms in the context of SCI involve an EPAC2-dependent mechanism, reducing neuroinflammation and providing a neuro-permissive environment. Chapter 2 aimed to further explore cAMP potential for SCI regeneration. We designed a novel strategy for artificial cAMP inductions in corticospinal neurons via optogenetic activation of a photoinducible adenylyl cyclase (bPAC). Daily optogenetic cAMP stimulation in rats suffering a thoracic dorsal hemisection, which completely disrupt the dorsal aspect of the corticospinal tract (CST), promoted and early and sustained locomotor recovery compared to non-treated control animals. We have shown that bPAC stimulation increased the number of retrograde traced neurons from the lumbar segment both in the motor cortex and the raphe-reticular formation, but not in the red nuclei. Moreover, immunolabelling of the raphespinal tract by 5-HT showed that bPAC stimulation increased the ratio of descending serotoninergic axons caudal to the injury which significantly correlated with improved functional parameters. Our results from corticobulbar projection study, WGA trans-synaptic tracing, and P-CREB analysis suggest that bPAC modulation of cortico-serotonergic pathway might occurs at the brainstem level. Lastly, the serotonergic system depletion by 5,7-Dihydroxytryptamine administration suppressed bPAC-mediated recovery, confirming the implication of the serotonergic tract in the recovery of stimulated animals. In summary, our research has provided new insights into the transcriptional changes that occur along SCI progression and after NPCs transplantation with a special emphasis on cAMP signaling. Optogenetic cAMP manipulation in corticospinal neurons after SCI has proven to be effective for functional recovery and allowed to unveil a cortical rerouting pathway through the serotonergic descending tract. / This research was funded by FEDER/Ministerio de Ciencia e Innovación – Agencia Estatal de Investigación [RTI2018-095872-BC21/ERDF]. Part of the equipment employed in this work was funded by Generalitat Valenciana and cofinanced with ERDF funds (OP ERDF of Comunitat Valenciana 2014– 2020) and the UE; Fondo Europeo de Desarrollo Regional (FEDER) incluido en el Programa Operativo FEDER de la Comunidad Valenciana 2014-2020. B. MartinezRojas was supported by a grant from the Conselleria de Educación, Investigación, Cultura y Deporte de la Generalitat Valenciana and the European Social Fundation ACIF/2019/120. / Martínez Rojas, B. (2024). Transcriptional Insights for Spinal Cord Injury and Neural Precursor Cell Therapy: Toward a Novel Optogenetics-Based Treatment for cAMP Neuronal Induction [Tesis doctoral]. Universitat Politècnica de València. https://doi.org/10.4995/Thesis/10251/202972

Movilidad

Locomotion

Neural Progenitor Cell Transplantation

Regeneración

Regeneration

cAMP

Optogenética

Optogenetics

Lesión medular

Spinal Cord Injury

BIOLOGIA CELULAR