Utilização da biópsia de mucosa e submucosa retal para o diagnóstico da Moléstia de Hirschsprung / Utilization of mucosal and submucosal rectal biopsy for the diagnosis of Hirschsprung\'s disease

Suellen Serafini

04 August 2017

Introdução: A moléstia de Hirschsprung (MH) se caracteriza pela ausência de neurônios intramurais em segmentos variáveis do intestino grosso, levando a suboclusão intestinal. Na forma mais frequente o reto-sigmoide está comprometido. A biopsia retal é o método histológico de escolha no diagnóstico da MH. O método da hematoxilina e eosina (HE) é classicamente utilizado na prática histopatológica. Nessa técnica, um fragmento de parede total do reto é processado através de parafinização, para posteriormente ser seccionado e corado por HE. Esta coloração evidencia células neurais em intestinos normais e troncos nervosos hipertrofiados nos casos de MH. É uma técnica muito simples, ainda hoje muito utilizada no diagnóstico da doença, necessitando de fragmentos grandes de reto para um maior acerto no diagnóstico. Este detalhe torna o diagnóstico do recém-nascido mais difícil. Outro método de coloração utilizado no diagnóstico da MH é o método histoquímico de pesquisa de atividade de Acetilcolinesterase (AChE). Nesta técnica é necessário apenas um pequeno fragmento de mucosa e submucosa que será congelado e depois processado. A pesquisa de AChE, nos casos de MH mostrará a presença desta enzima em quantidade aumentada, corando troncos e ou fibrilas de cor acastanhado. Este método já vem sendo utilizado pelo Instituto da Criança - HCFMUSP há mais de 30 anos e possui um acerto diagnóstico superior a 90%. Porém, por ser uma técnica mais elaborada, pouquíssimos centros no Brasil a utilizam no diagnóstico da MH. Um outro método mais recente, e que também pode ser realizado em fragmentos menores, é a marcação imunohistoquímica da calretinina, que permite a visualização dos neurônios do plexo submucoso e das fibrilas finas na região da lâmina própria em não doentes. Esta técnica também apresenta maior complexidade e, portanto, não é utilizada. A possibilidade de realizar o diagnóstico da MH através da coloração HE em fragmentos menores poderia ser uma alternativa para os serviços que não dispõe de técnicas mais especificas. Objetivos: Avaliar a concordância dos resultados obtidos pelo método de coloração HE e da calretinina com a pesquisa de atividade de AChE em fragmentos de mucosa e submucosa no diagnóstico da Moléstia de Hirschsprung. Métodos: Para este trabalho foram selecionados 50 casos arquivados em nosso laboratório. O material encontrava-se emblocado em parafina. Foram feitos 60 níveis de cada fragmento para o HE e mais 3 níveis para a calretinina. Essas lâminas foram analisadas em microscópio, fotografadas e classificadas como positivas para MH quando não foram encontradas células neurais e houve a presença de troncos nervosos, e em negativas nos casos de visualização dos neurônios. Foi realizado estudo cego por dois pesquisadores. Os resultados da leitura das lâminas foram comparados com o da AChE. Resultados: Dos 50 casos avaliados pela técnica do HE, apenas 5 discordaram do diagnóstico realizado pela AChE, com um valor de Kappa de 0,800 e acurácia 90%. Na comparação entre a calretinina e a AChE 8 casos discordaram, com um valor de Kappa de 0,676 e acurácia de 84%. Conclusões: A concordância obtida entre os métodos da AChE e HE foi satisfatória. Tornando possível a utilização do método do HE em 60 níveis de fragmento de mucosa e submucosa como alternativa para o diagnóstico da MH. A técnica imunohistoquímica da Calretinina não apresentou a concordância esperada com a pesquisa de atividade de AChE em nosso estudo / Introduction: Hirschsprung disease (HD) is characterized by the absence of intramural neurons in variable segments of the large intestine, leading to intestinal subocclusion. In the most frequent form the rectum-sigmoid is compromised. Rectal biopsy is the histological method of choice in the diagnosis of HD. The hematoxylin and eosin (HE) method is classically used in histopathological practice. In this technique, a full-thickness rectum wall fragment is processed through paraffinization, to be later sectioned and stained by HE. This staining shows neural cells in normal intestines and hypertrophied nerve trunks in cases of HD. It is a very simple technique, still used today in the diagnosis of the disease, requiring large fragments of the rectum for a better diagnosis. This detail makes the diagnosis of the newborn more difficult. The staining histochemical methods more used are the research of acetylcholinesterase activity (AChE) and staining of calretinin. However, these techniques are not available in all centers and the possibility of diagnosing HD through HE staining in smaller fragments could be valuable alternative for services that do not have more specific techniques. Objectives: To evaluate the concordance of the results obtained by the HE staining and the calretinin method with the investigation of AChE activity in fragments of mucosa and submucosa in the diagnosis of Hirschsprung\'s disease. Methods: For this study, 50 cases from our laboratory were selected. The material was embedded in paraffin. Sixty levels of each fragment were made for HE and other 3 levels for calretinin. These slides were analyzed under microscope, photographed and classified as positive for HD when no nerve cells were found and there were nerve trunks present, and in negative in cases of visualization of the neurons. A blind study was carried out by two researchers. The results of reading the slides were compared with that of AChE. Results: Of the 50 cases evaluated by the HE technique, only 5 disagreed with the diagnosis performed by AChE, with a Kappa value of 0.800 and accuracy of 90%. In the comparison between calretinin and AChE, 8 cases disagreed, with a Kappa value of 0.676 and an accuracy of 84%. Conclusions: The concordance of results from AChE and HE methods was satisfactory, allowing the possibility of the use of the HE method in fragments of mucosa and submucosa as valid alternative for the diagnosis of HD. The immunohistochemical technique of Calretinin did not show a good agreement with the AChE activity in our study

Acetilcolinesterase

Calretinina

Doença de Hirschsprung

Hematoxilina-eosina

Reto/biópsia

Submucosa

Calretinin

Hematoxylin-eosin

Hirschsprung's disease

Rectum/biopsy

Submucosa, Acetylcholinesterase

Utilização da biópsia de mucosa e submucosa retal para o diagnóstico da Moléstia de Hirschsprung / Utilization of mucosal and submucosal rectal biopsy for the diagnosis of Hirschsprung\'s disease

Serafini, Suellen

04 August 2017

Introdução: A moléstia de Hirschsprung (MH) se caracteriza pela ausência de neurônios intramurais em segmentos variáveis do intestino grosso, levando a suboclusão intestinal. Na forma mais frequente o reto-sigmoide está comprometido. A biopsia retal é o método histológico de escolha no diagnóstico da MH. O método da hematoxilina e eosina (HE) é classicamente utilizado na prática histopatológica. Nessa técnica, um fragmento de parede total do reto é processado através de parafinização, para posteriormente ser seccionado e corado por HE. Esta coloração evidencia células neurais em intestinos normais e troncos nervosos hipertrofiados nos casos de MH. É uma técnica muito simples, ainda hoje muito utilizada no diagnóstico da doença, necessitando de fragmentos grandes de reto para um maior acerto no diagnóstico. Este detalhe torna o diagnóstico do recém-nascido mais difícil. Outro método de coloração utilizado no diagnóstico da MH é o método histoquímico de pesquisa de atividade de Acetilcolinesterase (AChE). Nesta técnica é necessário apenas um pequeno fragmento de mucosa e submucosa que será congelado e depois processado. A pesquisa de AChE, nos casos de MH mostrará a presença desta enzima em quantidade aumentada, corando troncos e ou fibrilas de cor acastanhado. Este método já vem sendo utilizado pelo Instituto da Criança - HCFMUSP há mais de 30 anos e possui um acerto diagnóstico superior a 90%. Porém, por ser uma técnica mais elaborada, pouquíssimos centros no Brasil a utilizam no diagnóstico da MH. Um outro método mais recente, e que também pode ser realizado em fragmentos menores, é a marcação imunohistoquímica da calretinina, que permite a visualização dos neurônios do plexo submucoso e das fibrilas finas na região da lâmina própria em não doentes. Esta técnica também apresenta maior complexidade e, portanto, não é utilizada. A possibilidade de realizar o diagnóstico da MH através da coloração HE em fragmentos menores poderia ser uma alternativa para os serviços que não dispõe de técnicas mais especificas. Objetivos: Avaliar a concordância dos resultados obtidos pelo método de coloração HE e da calretinina com a pesquisa de atividade de AChE em fragmentos de mucosa e submucosa no diagnóstico da Moléstia de Hirschsprung. Métodos: Para este trabalho foram selecionados 50 casos arquivados em nosso laboratório. O material encontrava-se emblocado em parafina. Foram feitos 60 níveis de cada fragmento para o HE e mais 3 níveis para a calretinina. Essas lâminas foram analisadas em microscópio, fotografadas e classificadas como positivas para MH quando não foram encontradas células neurais e houve a presença de troncos nervosos, e em negativas nos casos de visualização dos neurônios. Foi realizado estudo cego por dois pesquisadores. Os resultados da leitura das lâminas foram comparados com o da AChE. Resultados: Dos 50 casos avaliados pela técnica do HE, apenas 5 discordaram do diagnóstico realizado pela AChE, com um valor de Kappa de 0,800 e acurácia 90%. Na comparação entre a calretinina e a AChE 8 casos discordaram, com um valor de Kappa de 0,676 e acurácia de 84%. Conclusões: A concordância obtida entre os métodos da AChE e HE foi satisfatória. Tornando possível a utilização do método do HE em 60 níveis de fragmento de mucosa e submucosa como alternativa para o diagnóstico da MH. A técnica imunohistoquímica da Calretinina não apresentou a concordância esperada com a pesquisa de atividade de AChE em nosso estudo / Introduction: Hirschsprung disease (HD) is characterized by the absence of intramural neurons in variable segments of the large intestine, leading to intestinal subocclusion. In the most frequent form the rectum-sigmoid is compromised. Rectal biopsy is the histological method of choice in the diagnosis of HD. The hematoxylin and eosin (HE) method is classically used in histopathological practice. In this technique, a full-thickness rectum wall fragment is processed through paraffinization, to be later sectioned and stained by HE. This staining shows neural cells in normal intestines and hypertrophied nerve trunks in cases of HD. It is a very simple technique, still used today in the diagnosis of the disease, requiring large fragments of the rectum for a better diagnosis. This detail makes the diagnosis of the newborn more difficult. The staining histochemical methods more used are the research of acetylcholinesterase activity (AChE) and staining of calretinin. However, these techniques are not available in all centers and the possibility of diagnosing HD through HE staining in smaller fragments could be valuable alternative for services that do not have more specific techniques. Objectives: To evaluate the concordance of the results obtained by the HE staining and the calretinin method with the investigation of AChE activity in fragments of mucosa and submucosa in the diagnosis of Hirschsprung\'s disease. Methods: For this study, 50 cases from our laboratory were selected. The material was embedded in paraffin. Sixty levels of each fragment were made for HE and other 3 levels for calretinin. These slides were analyzed under microscope, photographed and classified as positive for HD when no nerve cells were found and there were nerve trunks present, and in negative in cases of visualization of the neurons. A blind study was carried out by two researchers. The results of reading the slides were compared with that of AChE. Results: Of the 50 cases evaluated by the HE technique, only 5 disagreed with the diagnosis performed by AChE, with a Kappa value of 0.800 and accuracy of 90%. In the comparison between calretinin and AChE, 8 cases disagreed, with a Kappa value of 0.676 and an accuracy of 84%. Conclusions: The concordance of results from AChE and HE methods was satisfactory, allowing the possibility of the use of the HE method in fragments of mucosa and submucosa as valid alternative for the diagnosis of HD. The immunohistochemical technique of Calretinin did not show a good agreement with the AChE activity in our study

Acetilcolinesterase

Calretinin

Calretinina

Doença de Hirschsprung

Hematoxilina-eosina

Hematoxylin-eosin

Hirschsprung's disease

Rectum/biopsy

Reto/biópsia

Submucosa

Submucosa, Acetylcholinesterase

Connecting the Dots: Investigating the Effects of Trans-Synaptic Tau Transmission in the Hippocampus

Bamisile, Michael

01 January 2019

Tauopathy, which results from the oligomerization of misfolded tau protein in neurons, is a feature present in a number of neurodegenerative diseases and a hallmark of Alzheimer’s Disease (AD). Tau is an important phosphoprotein that regulates the assembly of microtubules, but tauopathy can occur when tau becomes hyperphosphorylated. Phosphorylation prevents tau from binding to tubulin, which results in cytosolic accumulation of tau and eventual oligomerization. This abnormal accumulation of tau leads to the spreading of hyperphosphorylated tau to downstream synaptically connected neurons through an unknown mechanism. In AD, the hippocampus is one of the first brain structures to be affected by tauopathy in humans. According to previous research, tauopathy occurs primarily between principal cells in the hippocampus. The involvement of local inhibitory interneurons in tauopathy and their potential role in AD is more controversial. Previous research suggests that tau pathogenesis primarily affects principal cells; however, given the importance, diversity, and function of interneurons in the hippocampus, it is important to gain a better understanding of the interneuron subtypes that may be impacted by the spread of trans-synaptic tau into the hippocampus. Understanding the involvement of interneurons in trans-synaptic tau transmission is important to understanding neurodegeneration in AD and other neurodegenerative disorders. To investigate this, both male and female genetically-modified mice underwent surgery to examine the trans-synaptic spread of pathogenic tau (EGFP-Tau P301L) from the entorhinal cortex to hippocampal neurons. Histology and imaging analysis of brain sections were performed to examine the hippocampal cells impacted by trans-synaptic spread of tau. Results show that pathogenic tau can trans-synaptically spread from presynaptic neurons in the entorhinal cortex into downstream hippocampal interneurons and also that hippocampal interneurons are capable of trans-synaptically spreading tau. Future studies examining the specific subtypes of hippocampal interneurons vulnerable to trans-synaptic spread of tau will be important for a better understanding of disease progression, which could lead to uncovering new therapeutic targets for neurodegenerative diseases, like AD, which are associated with tauopathy.

Alzheimer's Disease

neurodegeneration

trans-synaptic tau transmission

tau

hippocampus

entorhinal cortex

inhibitory interneurons

principal cells

VGAT

calretinin

Medicine and Health Sciences

Developmental Expression of Calcium Buffering Proteins in Central Auditory Pathways of Normal Hearing and Congenitally Deaf Mice

Deardorff, Adam S.

29 June 2010

No description available.

Biomedical Research

Neurology

Auditory Pathways

Calcium Buffering Proteins

Calretinin

Calbindin

Parvalbumin

Congenital Deafness

Synaptic Development

dn/dn mice

Origine, diversité et contrôle transcriptionnel des interneurones périglomérulaires calrétinines du bulbe olfactif / Origin, diversity and transcriptional coding of periglomerular calretinin interneurons

Gaborieau, Élodie

20 December 2017

Les cellules souches neurales (CSNs) de la zone sous-ventriculaire (ZSV) présentent une activité germinale intense tout au long de la vie d'un individu. Les CSNs postnatales sont régionalisées en microdomaines exprimant des facteurs de transcription spécifiques et générant des sous-types neuronaux distincts dans le bulbe olfactif (BO). Les interneurones calrétinine (CalR+) représentent la plus grande population d'interneurones périglomérulaires (PG) du BO produits après la naissance. Cependant, contrairement à d'autres, il existe peu d'informations concernant leur origine, leur diversité et leur fonction dans le BO, ainsi que les facteurs de transcription impliqués dans leur génération. Des études antérieures ont mis en évidence que les interneurones CalR + PG sont générés à la fois par les microdomaines médial et dorsal de la ZSV, et ont suggéré que le facteur de transcription Sp8 serait impliqué dans leur génération. Ce travail de thèse a eu pour objectif : 1) d'affiner les approches actuelles afin de manipuler l'expression génique dans les CSNs de la ZSV postnatale d'une manière contrôlée temporellement, 2) d'explorer l'origine et la fonction des interneurones CalR + périglomérulaires, 3) d'étudier le rôle du facteur de transcription Sp8 dans le codage transcriptionnel de la spécification des interneurones CalR + périglomérulaires ainsi que leur maturation. Ainsi, une approche d'électroporation postnatale classique a été affinée afin de pouvoir manipuler l'expression des gènes dans les CSNs de la ZSV et ainsi permettre de cartographier le devenir à long terme de la progénie des CSNs et de manipuler génétiquement ces CSNs à une étape précise de leur différentiation. Le perfectionnement de cette approche a permis d'identifier deux sous-populations d'interneurones CalR + présentant des origines spatiales et temporelles différentes après la naissance, ainsi que d'explorer les implications fonctionnelles et morphologiques de cette diversité. Ainsi, une fraction importante et non décrite d'interneurones CalR + PG présente des propriétés de neurones immatures (c'est-à-dire qu'elle reçoit peu d'entrées synaptiques et est faiblement excitable), remettant en question leur rôle dans le traitement de l'information olfactive. Enfin, des manipulations génétiques du facteur de transcription Sp8 à divers stades de la différenciation des interneurones CalR+ ont mis en évidence son rôle dans la survie à long terme des interneurones CalR + PG matures, tout en excluant un rôle dans leur spécification précoce. Ces résultats amène ainsi un éclairage nouveau sur l'origine, la diversité et le codage transcriptionnel des interneurones CalR + PG et appellent à une caractérisation plus précise de leur rôle dans le traitement de l'information olfactive / The subventricular zone (SVZ) is a brain region that shows intense germinal activity throughout postnatal life. The postnatal SVZ is subdivided in microdomains containing neural stem cells (NSCs) that express defined transcription factors and generate distinct neuronal subtypes in the olfactory bulb (OB). Calretinin-expressing (CalR+) interneurons represent the largest population of OB periglomerular interneurons produced after birth. Yet, in contrast to others, limited information exists regarding their origin, diversity and function in the OB, as well as the transcription factors that guide their generation. Previous studies highlighted that CalR+ PG interneurons are generated by both the medial and dorsal SVZ microdomains, and suggested that the transcription factor Sp8 is involved in their generation.This work aimed at 1) refining current approaches for manipulating gene expression in postnatal SVZ NSCs in a temporally controlled manner, 2) exploring the origin and the function of CalR+ periglomerular neurons, 3) investigating the role of Sp8 in the transcriptional coding of CalR+ periglomerular interneurons specification and maturation.Refinement of the classical electroporation approach allowed the long-term fate mapping and timely-controlled genetic manipulation of NSCs of the SVZ. Using this refined approach allowed identifying two subpopulations of CalR+ interneurons that show different spatial and temporal origins after birth, as well as to explore the functional and morphological correlates of this diversity. A large and previously non-described fraction of CalR+ periglomerular interneurons exhibits properties of immature neurons (i.e. little synaptic inputs and weak excitability), questioning their role in olfactory processing. Finally, genetic manipulations of the transcription factor Sp8 at different stages during CalR+ interneuron differentiation highlighted its role in the long-term survival of mature CalR+ periglomerular interneurons, while excluding a role in their early specification. Altogether these results shed new lights on the origin, diversity and transcriptional coding of CalR+ periglomerular i nterneurons and call for a characterization of their role in olfactory processing

Activité germinale postnatale

Cellules souches

Bulbe olfactif

Interneurones calrétinine

Facteur de transcription Sp8

Postnatal germinal activity

Neural stem cells

Olfactory bulb

Calretinin interneurons

Transcription factor Sp8

612.8

Caracteriza??o de subpopula??es de interneur?nios imunorreativos para prote?nas ligantes de c?lcio no c?rtex pr?-frontal do Sagui (Callithrix jacchus): distribui??o e morfologia

Silva, Joanilson Guimar?es

02 May 2011

Made available in DSpace on 2014-12-17T15:36:38Z (GMT). No. of bitstreams: 1 JoanilsonGS_TESE.pdf: 3996700 bytes, checksum: 8b3084030c1c254db2c08a440881ea9a (MD5) Previous issue date: 2011-05-02 / Conselho Nacional de Desenvolvimento Cient?fico e Tecnol?gico / Cortical interneurons are characterized by their distinct morphological, physiological and biochemical properties, acting as modulators of the excitatory activity by pyramidal neurons, for example. Various studies have revealed differences in both distribution and density of this cell group throughout distinct cortical areas in several species. A particular class of interneuron closely related to cortical modulation is revealed by the immunohistochemistry for calcium binding proteins calbindin (CB), calretinina (CR) and parvalbumin (PV). Despite the growing amount of studies focusing on calcium binding proteins, the prefrontal cortex of primates remains relatively little explored, particularly in what concerns a better understanding of the organization of the inhibitory circuitry across its subdivisions. In the present study we characterized the morphology and distribution of neurons rich in calcium-binding proteins in the medial, orbital and dorsolateral areas of the prefrontal cortex of the marmoset (Callithrix jacchus). Using both morphometric and stereological techniques, we found that CR-reactive neurons (mainly double bouquet and bipolar cells) have a more complex dendritic arborization than CB-reactive (bitufted and basket cells) and PV-reactive neurons (chandelier cells). The neuronal densities of CR- and CB-reactive cells are higher in the supragranular layers (II/III) whilst PV-reactive neurons, conversely, are more concentrated in the infragranular layers (V/VI). CR-reactive neurons were the predominant group in the three regions evaluated, being most prevalent in dorsomedial region. Our findings point out to fundamental differences in the inhibitory circuitry of the different areas of the prefrontal cortex in marmoset / Os interneur?nios do c?rtex cerebral s?o caracterizados por suas diferentes propriedades morfol?gicas, fisiol?gicas e bioqu?micas, atuando como moduladores da atividade excitat?ria cortical dos neur?nios piramidais, por exemplo. V?rios estudos revelaram diferen?as na distribui??o e densidade deste grupo celular ao longo de diferentes ?reas corticais em diversas esp?cies. Uma classe particular de interneur?nios intimamente relacionada ? modula??o cortical ? revelada pela imunohistoqu?mica para as prote?nas ligantes de c?lcio calbindina (CB), calretinina (CR) e parvalbumina (PV). Em que pese a quantidade crescente de estudos focando nas prote?nas ligantes de c?lcio, o c?rtex pr?frontal de primatas ainda permanece relativamente pouco explorado, especialmente no que se refere a um melhor entendimento da organiza??o do circuito inibit?rio ao longo de suas subdivis?es. No presente estudo caracterizamos a morfologia e a distribui??o desse grupo neuronal nas regi?es medial, orbital e dorso-lateral do c?rtex pr?-frontal do sagui (Callithrix jacchus). Utilizando par?metros morfom?tricos e t?cnicas estereol?gicas, evidenciamos que os neur?nios reativos a CR (especialmente c?lulas em duplo-buqu? e bipolares) possuem arboriza??o dendr?tica mais complexa quando comparados aos neur?nios reativos a CB (neur?nios de tufos duplos e c?lulas em cesto) e PV (c?lulas em candelabro). A densidade dos neur?nios reativos a CB e CR ? mais elevada nas camadas supragranulares (II/III), enquanto os neur?nios reativos a PV se concentram predominantemente nas camadas infragranulares (V/VI). Os neur?nios reativos a CR foram o grupo predominante nas tr?s regi?es avaliadas, sendo mais prevalente na regi?o dorsolateral. Nossos achados apontam para diferen?as cruciais no circuito inibit?rio ao longo das diferentes ?reas do c?rtex pr?-frontal do sagui

calbindina

calretinina

parvalbumina

c?rtex pr?-frontal

interneur?nios

morfometria

estereologia

calbindin

calretinin

parvalbumin

prefrontal cortex

interneurons

morphometry

stereology

Plasticité intermodale chez le hamster énucléé à la naissance : Études de la distribution des interneurones CaBPir dans les cortex visuel et auditif primaires.

Desgent, Sébastien

01 1900

La période postnatale et l’expérience sensorielle sont critiques pour le développement du système visuel. Les interneurones inhibiteurs exprimant l’acide γ-aminobutyrique (GABA) jouent un rôle important dans le contrôle de l’activité neuronale, le raffinement et le traitement de l’information sensorielle qui parvient au cortex cérébral. Durant le développement, lorsque le cortex cérébral est très susceptible aux influences extrinsèques, le GABA agit dans la formation des périodes critiques de sensibilité ainsi que dans la plasticité dépendante de l’expérience. Ainsi, ce système inhibiteur servirait à ajuster le fonctionnement des aires sensorielles primaires selon les conditions spécifiques d’activité en provenance du milieu, des afférences corticales (thalamiques et autres) et de l’expérience sensorielle. Certaines études montrent que des différences dans la densité et la distribution de ces neurones inhibiteurs corticaux reflètent les caractéristiques fonctionnelles distinctes entre les différentes aires corticales. La Parvalbumine (PV), la Calretinine (CR) et la Calbindine (CB) sont des protéines chélatrices du calcium (calcium binding proteins ou CaBPs) localisées dans différentes sous-populations d’interneurones GABAergiques corticaux. Ces protéines tamponnent le calcium intracellulaire de sorte qu’elles peuvent moduler différemment plusieurs fonctions neuronales, notamment l’aspect temporel des potentiels d’action, la transmission synaptique et la potentialisation à long terme. Plusieurs études récentes montrent que les interneurones immunoréactifs (ir) aux CaBPs sont également très sensibles à l’expérience et à l’activité sensorielle durant le développement et chez l’adulte. Ainsi, ces neurones pourraient avoir un rôle crucial à jouer dans le phénomène de compensation ou de plasticité intermodale entre les cortex sensoriels primaires. Chez le hamster (Mesocricetus auratus), l’énucléation à la naissance fait en sorte que le cortex visuel primaire peut être recruté par les autres modalités sensorielles, telles que le toucher et l’audition. Suite à cette privation oculaire, il y a établissement de projections ectopiques permanentes entre les collicules inférieurs (CI) et le corps genouillé latéral (CGL). Ceci a pour effet d’acheminer l’information auditive vers le cortex visuel primaire (V1) durant le développement postnatal. À l’aide de ce modèle, l’objectif général de ce projet de thèse est d’étudier l’influence et le rôle de l’activité sensorielle sur la distribution et l’organisation des interneurones corticaux immunoréactifs aux CaBPs dans les aires sensorielles visuelle et auditive primaires du hamster adulte. Les changements dans l’expression des CaBPs ont été déterminés d’une manière quantitative en évaluant les profils de distribution laminaire de ces neurones révélés par immunohistochimie. Dans une première expérience, nous avons étudié la distribution laminaire des CaBPs dans les aires visuelle (V1) et auditive (A1) primaires chez le hamster normal adulte. Les neurones immunoréactifs à la PV et la CB, mais non à la CR, sont distribués différemment dans ces deux cortex primaires dédiés à une modalité sensorielle différente. Dans une deuxième étude, une comparaison a été effectuée entre des animaux contrôles et des hamsters énucléés à la naissance. Cette étude montre que le cortex visuel primaire de ces animaux adopte une chimioarchitecture en PV similaire à celle du cortex auditif. Nos recherches montrent donc qu’une suppression de l’activité visuelle à la naissance peut influencer l’expression des CaBPs dans l’aire V1 du hamster adulte. Ceci suggère également que le type d’activité des afférences en provenance d’autres modalités sensorielles peut moduler, en partie, une circuiterie corticale en CaBPs qui lui est propre dans le cortex hôte ou recruté. Ainsi, nos travaux appuient l’hypothèse selon laquelle il serait possible que certaines de ces sous-populations d’interneurones GABAergiques jouent un rôle crucial dans le phénomène de la plasticité intermodale. / The postnatal period and sensory experience are critical for the development of the visual system. The inhibitory interneurons expressing the γ-aminobutyric acid (GABA) play an important role in the control of neural activity, refinement and treatment of sensory information which reaches the cerebral cortex. During development, when the cerebral cortex is very likely to be influenced by extrinsic factors, GABA acts in the formation of critical period of receptivity as well as in experience dependent plasticity. Thus, this inhibitory system adjusts the functioning of the primary sensory areas according to the specific conditions of activity from the environment, cortical afferents (e.g. of thalamic origin), and sensory experience. Several studies show that differences in the distribution and density of these inhibitory interneurons tend to reflect functional discrepancies between the different neocortical areas. Parvalbumin (PV), Calretinin (CR) and Calbindin (CB) are calcium-binding proteins (CaBPs) found in different sub-populations of GABAergic cortical interneurons. These proteins buffer intracellular calcium levels, which can in turn modulate several neural functions, notably the temporal aspect of action potentials, synaptic transmission and long-term potentiation. Several recent studies are showing that CaBPs immunoreactive (ir) interneurons are also very sensitive to experience and sensory activity during development and adulthood. Therefore, these neurons may have a critical role in intermodal plasticity or compensatory processes between primary sensory cortices. In the hamster (Mesocricetus auratus), after enucleation at birth, the primary visual cortex can be recruited by other sensory modalities such as touch and audition. After this type of visual deprivation, there is establishment of permanent ectopic projections between the inferior colliculus (IC) and the lateral geniculate nucleus (LGN). This phenomenon leads to the rerouting of auditory information to the primary visual cortex (V1) during postnatal development. By using this animal model, the general objective of this thesis is to study the influence and the role of sensory activity on the distribution and organization of cortical interneurons that display immunoreactivity for CaBPs in the primary visual and auditory sensory areas in adult hamsters. Changes in the expression of CaBPs were quantitatively determined by assessing the laminar distribution profiles of cell bodies revealed by immunohistochemistry. In the first experiment, we studied laminar distribution of CaBPs in the primary visual (V1) and auditory (A1) cortices of normal hamsters. PVir and CBir, but not CRir neurons, are distributed in a dissimilar fashion between the two primary cortices devoted to each sensory modality. In the second study, a comparison was performed between control animals and hamsters which were enucleated at birth. The results of this study show that the primary visual cortex of these animals adopts a PVir chemoarchitecture similar to that of the auditory cortex. Our research shows that the abolition of visual activity at birth can influence the expression of CaBPs in V1 of the adult hamster. The present results also suggest that the type of activity in afferents from other sensory modalities can at least in part modulate the cortical circuitry of CaBPs in the host or recruited cortex. Thus, our work supports the hypothesis that sub-populations of GABAergic interneurons may play a critical role in the intermodal cortical plasticity.

Activité sensorielle

Calbindine

Calretinine

Énucléation à la naissance

Hamster

Néocortex

Parvalbumine

Plasticité intermodale

Système auditif

Système visuel

Sensory activity

Calbindin

Calretinin

Enucleation at birth

Hamster

Neocortex

Parvalbumin

Intermodal plasticity

Auditory system

Visual system

Plasticité intermodale chez le hamster énucléé à la naissance : Études de la distribution des interneurones CaBPir dans les cortex visuel et auditif primaires

Desgent, Sébastien

01 1900

No description available.

Activité sensorielle

Calbindine

Calretinine

Énucléation à la naissance

Hamster

Néocortex

Parvalbumine

Plasticité intermodale

Système auditif

Système visuel

Sensory activity

Calbindin

Calretinin

Enucleation at birth

Hamster

Neocortex

Parvalbumin

Intermodal plasticity

Auditory system

Visual system