Global ETD Search

151	Análise histológica e funcional de xenotransplante de células-tronco da orelha interna de camundongos em cócleas de cobaias com perda auditiva induzida / Histological and functional analysis of inner ear stem cell xenotransplantation in the cochlea of guinea pigs with induced hearing loss Luiz Carlos de Melo Barboza Junior 05 September 2012 (has links) Introdução: Em mamíferos, a morte das células sensoriais (células ciliadas) da orelha interna acarreta perda auditiva neurossensorial permanente. Neste estudo, investigou-se se, após o transplante, as células-tronco (CT) da orelha interna de camundongos neonatos podem sobreviver e integrar nos giros basais das cócleas de cobaias submetidas à surdez induzida por neomicina. O potencial efeito do transplante celular na função auditiva também foi avaliada. Métodos: Oito cobaias foram submetidas à injeção de neomicina transtimpânica para indução de surdez. Após 7 dias, os animais foram aleatoriamente divididos em dois grupos. No grupo estudo (n=4), as CT da orelha interna de camundongos neonatos (meio de cultura com 105 CT LacZ+) foram transplantadas através de uma cocleostomia no giro basal de cobaias surdas. O grupo controle (n=4) recebeu somente meio de cultura. Após 14 dias do transplante, o efeito funcional foi avaliado por meio de pesquisa dos potenciais evocados auditivos e os animais foram sacrificados. A presença e a distribuição das CT transplantadas foram avaliadas por imunofluorescência dos cortes longitudinais das cócleas do grupo estudo. Testes não paramétricos foram usados para a análise estatística. Resultados: A ação da neomicina na cavidade timpânica proporcionou dano às células ciliadas e aumento significativo dos limiares auditivos antes do transplante celular. Não houve diferenças significantes dos limiares auditivos antes e após o transplante celular nas cobaias individualmente. Algumas CT transplantadas foram observadas em todas as escalas dos giros basais das cócleas lesadas, e parte destas células expressaram Miosina VIIA, um marcador de célula ciliada. Algumas CT transplantadas se integraram na membrana basilar da cóclea hospedeira. Nenhuma evidência de infiltração inflamatória nas cobaias transplantadas foi observada, apesar do uso de xenotransplante. Conclusões: Embora, após o transplante, os limiares auditivos não tenham sido alterados, os experimentos mostraram sobrevivência, migração, expressão de marcadores de células ciliadas e integração das CT transplantadas / Background: In mammals, damage to sensory receptor cells (hair cells) of the inner ear results in permanent sensorineural hearing loss. Here we investigate whether, after transplantation, neonatal mouse inner ear stem cells (mIESCs) can survive and integrate into basal turns of neomycin-injured guinea pig cochleas. We also studied the potential effects of the cell transplantation on the auditory function. Methods: Eight adult guinea pigs were deafened by intratympanic neomycin delivery. After 7 days, the animals were randomly divided in two groups. Study group (n=4) received transplantation to the scala tympani of 1 X 105 LacZ-positive mIESCs in culture medium. Control group (n=4) received culture medium only. Fourteen days after the transplantation, functional analyses were performed by auditory brainstem responses (ABR) and the animals were sacrificed. The presence and distribution of mIESCs were evaluated by immunohistochemistry of longitudinal sections of the cochlea from the study group. Non-parametric tests were used for statistical analysis. Results: The intratympanic neomycin delivery damaged hair cells and increased auditory thresholds prior to cell transplantation. There were no significant differences between auditory brainstem thresholds before and after transplantation in individual guinea pigs. Some mIESCs have been observed in all scalae of basal turns of the injured cochleas, and a proportion of those cells expressed the hair cell marker myosin VIIa. Some transplanted mIESCs integrated in the cochlear basilar membrane. There was no evidence of inflammatory infiltration in any of the guinea pigs. Conclusions: Although implanted mIESCs showed no obvious effect on auditory thresholds, our experiments showed survival, migration, expression of hair cell marker and integration of transplanted cells Camundongos Células-tronco Cobaias Cóclea Perda auditiva Regeneração Terapia celular Transplante de células Xenotransplante Cell therapy Cell transplantation Cochlea Guinea pigs Hearing loss Mice Regeneration Stem cells Xenotransplantation
152	Análise histológica e funcional de xenotransplante de células-tronco da orelha interna de camundongos em cócleas de cobaias com perda auditiva induzida / Histological and functional analysis of inner ear stem cell xenotransplantation in the cochlea of guinea pigs with induced hearing loss Barboza Junior, Luiz Carlos de Melo 05 September 2012 (has links) Introdução: Em mamíferos, a morte das células sensoriais (células ciliadas) da orelha interna acarreta perda auditiva neurossensorial permanente. Neste estudo, investigou-se se, após o transplante, as células-tronco (CT) da orelha interna de camundongos neonatos podem sobreviver e integrar nos giros basais das cócleas de cobaias submetidas à surdez induzida por neomicina. O potencial efeito do transplante celular na função auditiva também foi avaliada. Métodos: Oito cobaias foram submetidas à injeção de neomicina transtimpânica para indução de surdez. Após 7 dias, os animais foram aleatoriamente divididos em dois grupos. No grupo estudo (n=4), as CT da orelha interna de camundongos neonatos (meio de cultura com 105 CT LacZ+) foram transplantadas através de uma cocleostomia no giro basal de cobaias surdas. O grupo controle (n=4) recebeu somente meio de cultura. Após 14 dias do transplante, o efeito funcional foi avaliado por meio de pesquisa dos potenciais evocados auditivos e os animais foram sacrificados. A presença e a distribuição das CT transplantadas foram avaliadas por imunofluorescência dos cortes longitudinais das cócleas do grupo estudo. Testes não paramétricos foram usados para a análise estatística. Resultados: A ação da neomicina na cavidade timpânica proporcionou dano às células ciliadas e aumento significativo dos limiares auditivos antes do transplante celular. Não houve diferenças significantes dos limiares auditivos antes e após o transplante celular nas cobaias individualmente. Algumas CT transplantadas foram observadas em todas as escalas dos giros basais das cócleas lesadas, e parte destas células expressaram Miosina VIIA, um marcador de célula ciliada. Algumas CT transplantadas se integraram na membrana basilar da cóclea hospedeira. Nenhuma evidência de infiltração inflamatória nas cobaias transplantadas foi observada, apesar do uso de xenotransplante. Conclusões: Embora, após o transplante, os limiares auditivos não tenham sido alterados, os experimentos mostraram sobrevivência, migração, expressão de marcadores de células ciliadas e integração das CT transplantadas / Background: In mammals, damage to sensory receptor cells (hair cells) of the inner ear results in permanent sensorineural hearing loss. Here we investigate whether, after transplantation, neonatal mouse inner ear stem cells (mIESCs) can survive and integrate into basal turns of neomycin-injured guinea pig cochleas. We also studied the potential effects of the cell transplantation on the auditory function. Methods: Eight adult guinea pigs were deafened by intratympanic neomycin delivery. After 7 days, the animals were randomly divided in two groups. Study group (n=4) received transplantation to the scala tympani of 1 X 105 LacZ-positive mIESCs in culture medium. Control group (n=4) received culture medium only. Fourteen days after the transplantation, functional analyses were performed by auditory brainstem responses (ABR) and the animals were sacrificed. The presence and distribution of mIESCs were evaluated by immunohistochemistry of longitudinal sections of the cochlea from the study group. Non-parametric tests were used for statistical analysis. Results: The intratympanic neomycin delivery damaged hair cells and increased auditory thresholds prior to cell transplantation. There were no significant differences between auditory brainstem thresholds before and after transplantation in individual guinea pigs. Some mIESCs have been observed in all scalae of basal turns of the injured cochleas, and a proportion of those cells expressed the hair cell marker myosin VIIa. Some transplanted mIESCs integrated in the cochlear basilar membrane. There was no evidence of inflammatory infiltration in any of the guinea pigs. Conclusions: Although implanted mIESCs showed no obvious effect on auditory thresholds, our experiments showed survival, migration, expression of hair cell marker and integration of transplanted cells Camundongos Cell therapy Cell transplantation Células-tronco Cobaias Cochlea Cóclea Guinea pigs Hearing loss Mice Perda auditiva Regeneração Regeneration Stem cells Terapia celular Transplante de células Xenotransplantation Xenotransplante
153	Auditory Filters Measured at Neighboring Center Frequencies Fagelson, Marc A., Champlin, C. A. 01 June 1997 (has links) Auditory filters were derived in 20 normal-hearing human listeners at center frequencies (CFs) of 913, 1095, 3651, and 4382 Hz using the roex (p,r) method. Comparisons were made between slopes of the filters' skirts at the neighboring CFs with filter output levels of 45 and 70 dB. The same comparisons were made with regard to filter equivalent rectangular bandwidth (ERB). In the 1000-Hz region, the low-frequency slopes (Pl) of filters centered at 913 and 1095 Hz were significantly correlated at both stimulus levels, while the high-frequency slopes (Pu) were similar only at the high test level. In the 4000-Hz region, for sinusoids of 3651 and 4382 Hz, the level effect was clearer as both Pu and Pl values diverged at the low level but were related at high levels. The ERBs centered at the same CFs displayed a similar level dependence. At the stimulus level most likely to be affected by an active feedback mechanism, auditory filters centered at nearly the same frequency displayed quite distinct frequency selectivity, and this trend was stronger in the 4000-Hz region than the 1000-Hz region. The findings suggest that a saturating, active cochlear mechanism may not be distributed evenly, or contribute to peripheral tuning with equal effectiveness throughout the length of the partition. humans adult female male auditory threshold cochlea loudness perception perceptual masking pitch discrimination psychoacoustics reference values sound spectrography Audiology and Speech-Language Pathology Speech Pathology and Audiology
154	Mécanismes et Thérapies des Surdités Neurosensorielles Poirrier, Anne-Lise 14 September 2010 (has links) Au cours de ces années de Doctorat, nous avons étudié les effets ototoxiques de certains médicaments et les moyens de prévenir les surdités neuro-sensorielles quils peuvent induire. Parmi ces molécules, nous nous sommes concentrés sur les plus couramment utilisées en pratique clinique : les antibiotiques de la famille des aminoglycosides et le cisplatine, un agent anti-cancéreux. Lintroduction de notre travail replace la surdité dans son contexte de santé publique. En particulier, nous décrivons pourquoi les médicaments ototoxiques sont utilisés et dans quelles circonstances. Nous présentons la structure de loreille interne et nous tentons dexpliquer sa vulnérabilité aux molécules ototoxiques. Nous abordons ensuite les moyens de prévention et/ou de traitement de ces atteintes neuro-sensorielles pharmaco-induites. Outre les moyens classiques de prévention, que sont les facteurs trophiques et les antioxydants, nous décrivons de nouvelles voies dapproche que sont les voies de signalisation impliquant la protéine kinase C ou la cascade dactivation RhoA/ROCK. La présentation de notre travail original sarticule autour de deux parties. Dans la première partie, nous rapportons les résultats obtenus au cours de notre étude de la toxicité des aminoglycosides et du cisplatine chez la souris et le cobaye in vivo. Nous avons mis en évidence une différence de vulnérabilité significative entre ces deux espèces face à lagression ototoxique. Cette différence existe au niveau fonctionnel, mis en évidence par létude des potentiels évoqués auditifs, et au niveau anatomique, étudié en histologie et en immunohistochimie. Nous en discutons les implications en recherche et en pratique clinique. Dans la seconde partie, nous étudions les moyens de prévenir cette surdité in vivo et in vitro. Nous avons utilisé un modèle de surdité par aminoglycoside chez le cobaye. Nous avons testé et validé une technique de perfusion intra-cochléaire in vivo. Nous avons observé les effets de deux molécules expérimentales : la Bryostatine 1, un activateur de la protéine kinase C, et un inhibiteur de la voir RhoA-ROCK. Leffet protecteur de ces molécules est actuellement limité au ganglion spiral, dont la survie est essentielle à tout traitement dimplantation prothétique et de réadaptation. Nous discutons des perspectives en médecine humaine dans notre conclusion. In this work, we focused our attention on the effects of main ototoxic drugs i.e. aminoglycosides and cisplatin in mammals. We identified new avenues for the prevention of this toxicity. In the introduction, we described how and why ototoxic drugs are used. We then described potential otoprotective strategies in neurosensory deafness. Among them, trophic factors and antioxidant molecules have been widely used. New otoprotective approaches do exist, implying the protein kinase C or RhoA/ROCK signalling. Our original work was presented in two parts. In the first part, we reported the in vivo effects of aminoglycosides and cisplatin in two mammalian species: mice and guinea pigs. Contrarily to guinea pigs, evidence of mice resistance to ototoxicity was found at a functional level, assessed by auditory brainstem responses, and at an anatomical level, studied by immunohistochemistry. We discussed the implication of such differences in research and in clinical practice. In the second part, we studied the effect of two potential otoprotective molecules: Bryostatine 1, an activator of the protein kinase C, and Y-27632, a Rho kinase inhibitor. We showed that these molecules are protecting spiral ganglion neurons both in vitro and in vivo. Survival of spiral ganglion neurons is crucial in the management and rehabilitation of deafness. The potential perspectives of these results in human medicine were discussed. Ototoxicity/ototoxicite cochlea/cochlee Aminoglycoside Y-27632. mouse/souris protein kinase C/proteine kinase C Rho kinase hearing/audition Bryostatin 1/bryostatine 1 Cisplatin/cisplatine guinea pig/cobaye
155	Topical anesthesia of the tympanic membrane : an experimental animal study Schmidt, Sten-Hermann January 1987 (has links) Myringotomy plays an important role in otological therapy. The procedure requires an efficient anesthesia, which can be obtained without general anesthesia. However, the use of local anesthetics on the tympanic membrane (TM) has been abandoned in many places, as general anesthesia has been readily available. In the present study the effects of some commonly used topical anesthetics on the TM structure and inner ear were tested in an animal model (rat and guinea pig).Four different anesthetic compounds—Xylocaine®, Bonain's liquid, phenol and Emla®—were applied to the TMs of the animals, which were sacrificed 10 minutes to 5 months after application. Morphological effects regarding time after treatment and number of applications were elucidated. At sacrifice the tissue was fixed and the TMs analysed by light microscopy (LM) and transmission electron microscopy (TEM). In nine animals phenol, Xylocaine® Spray or Emla® was applied to the round window niche and ABR recordings were made at 24 h to 6 months after exposure. After the final ABR evaluation the animals were sacrificed and the cochleae prepared for LM and scanning electron microscopy (SEM).On the TM phenol and Bonain's liquid caused instant destruction of the keratinizing stratified squamous epithelium followed by long-lasting hyperplasia of this epithelium and the underlying connective tissue. A pronounced hyperplasia of these two layers was also noted for the Xylocaine® Spray group, but without immediate destruction of the keratinizing epithelium. The extent of structural changes differed in relation to the extent of spreading of the agent. Emla® showed little, if any, sign of epithelial reaction and had no effect on the connective tissue. Regarding the inner ear Emla®, Xylocaine® Spray and phenol induced significantly impaired ABR thresholds mainly affecting the higher frequencies. However, the impaired ABR thresholds were reversible and at the end of the experiment there was no significant impairment compared to the control data. All agents, except Xylocaine®, damaged the hair cells in the basal part of the cochlea as shown by cytocochleogram and SEM analysis.Instant destruction of the epidermis seems to be necessary for an instant anesthetic effect. All agents caused profound connective tissue reactions. The manner of application, depending on the physical properties of the agent, determined the extent of the structural changes. The changes of the connective tissue were concentrated to the submucosal layer, which seems to be the area for reconstruction of the damaged TM. All agents caused functional inner ear changes. With the exception of Xylocaine® they also caused morphological alterations of the cochlea. The functional changes were partly reversible. Topical anesthetics applied to the TM should be used with caution and when used in an appropriate manner they can be considered safe, especially in an inflamed middle ear, with a thickened round window membrane, which should prevent the agents from reaching the inner ear structures. / digitalisering@umu Topical anesthesia middle ear tympanic membrane cochlea collagen fibres lidocaine 96 % phenol Bonain's liquid auditory brainstem response ototoxicity cytocochleogram scanning electron microscopy rat guinea pig
156	The feasibility of including Distortion Product Otoacoustic Emissions (DPOAEs) in the annual medical surveillance test battery for the identification of noise-induced hearing loss in a group of workers in a beverage manufacturing industry. Reddy, Tarryn Marisca. 29 November 2013 (has links) The study investigated the feasibility of including DPOAEs in the annual medical surveillance test battery for the identification of NIHL in a group of employees in a manufacturing industry in KwaZulu-Natal. Feasibility was investigated by exploring the sensitivity, specificity and predictive efficiency of DPOAEs, the ability of DPOAEs to detect subtle noise-induced cochlea changes, the test-retest reliability of DPOAEs and lastly, the duration of time taken to conduct the DPOAE test bilaterally. A cross-sectional and repeated measures within-in participant design was utilized in the study. A purposive convenience sampling technique was used, as well as a stratified sampling approach in order to realize objective two of the study. The study consisted of 60 participants, which were further stratified into four test groups, i.e. Group A: 0-3 years, Group B: 3.1-6 years and Group C: 6.1-9 years and Group D: 9.1-13 years of working within the beverage manufacturing industry. A high sensitivity and negative predictive value was reported in the current study, suggesting that DPOAEs may be able to identify those who present with subtle cochlea changes as a result of exposure to occupational noise. The sensitivity of DPOAEs was 100% at 1, 2, 4, 6 and 8kHz in the right ear and at 4 and 6kHz in the left ear. The specificity of DPOAEs in the current study ranged between 55%-97% across the frequency range in the right ear and 49%-88% in the left ear. A negative predictive value of 100% was obtained bilaterally across the frequency range, except at 8kHz in the left ear. Visual inspection of the DPgram in the current study revealed a bilateral reduction in DPOAE amplitudes for all test groups in the high frequency region of the DP-Gram, namely, 5477Hz and 7303Hz, in the absence of a statistically significant difference (p>0.05). A greater frequency range appears to be affected in this group of workers, indicating that the type of noise, namely, impulse noise, may result in cochlea changes. Corresponding changes on the pure tone audiogram were not observed, however, noise notch configurations were observed for the groups with a longer history of noise exposure. This was not seen bilaterally as is typically expected with NIHL. Good test-retest reliability across the frequency range obtained in the current study further indicates the feasibility of including DPOAEs in the annual medical surveillance test battery. Additionally, the current study calculated an average of 86 seconds (1 minute 26 seconds) to conduct the DPOAE test bilaterally, confirming that DPOAEs are a quick test to administer. The findings of this study suggest that DPOAEs may be used to monitor early subtle noise-induced cochlea changes for workers exposed to noise in the beverage manufacturing industry as part of the annual medical surveillance test battery. / Thesis (M.Comm.Path.)-University of KwaZulu-Natal, Westville, 2013. Deafness, Noise induced. Noise--Health aspects. Noise--Measurement. Noise--Physiological effect. Theses--Physiotherapy. Noise-induced hearing loss. Subtle cochlea changes. Pure tone audiometry.
157	Sound Encoding in the Mouse Cochlea: Molecular Physiology and Optogenetic Stimulation Jing, Zhizi 23 October 2013 (has links) No description available. 570 sound encoding auditory nerve fiber cochlea Bassoon mutants Black swiss mice optogenetic stimulation sensorineural hearing loss development inner hair cell Biologie (PPN619462639)
158	Avaliação do recesso do nervo facial e cóclea no osso temporal de cadáveres de recém nascidos natimortos com vistas ao implante coclear percutâneo / Evaluation of the facial nerve recess and cochlea on the temporal bones of cadaveric newborns and its applicability in the percutaneous cochlear implant technique Gabriela Pereira Bom Braga 23 January 2017 (has links) INTRODUÇÃO: A literatura evidencia as diferenças anatômicas do osso temporal em crianças quando comparadas à adultos. Mais e mais a literatura enfatiza a importância de que as crianças com surdez congênita devem ser implantadas cada vez mais precocemente. Estudos anátomo-radiológicos são importantes para o desenvolvimento de técnicas cirúrgicas que possibilitem implantar crianças recém natas. Técnicas de implante coclear percutâneo (através de robótica) tem sido desenvolvidas na Universidade de Vanderbilt. Criamos então nossa principal pergunta \"Seria possível implantar crianças recém natas através de implante percutâneo?\" e procuraremos respondê-la no curso desse trabalho. OBJETIVO: Aferir as medidas do recesso do nervo facial e sua relação com a cóclea visando simular o trajeto da broca através desse recesso, para realização da cocleostomia, objetivando o implante coclear percutâneo. CASUÍSTICA E METODOLOGIA: Estudo experimental realizado com 9 espécimes de natimortos com idade gestacional entre 32 e 40 semanas, submetidos à tomografia computadorizada com individualização e reconstrução do nervo facial, cadeia ossicular, membrana timpânica, cóclea e labirinto, seguido da definição da trajetória da broca até a escala timpânica, utilizando o software Improvise. RESULTADOS: As medidas da trajetória da broca até o nervo facial, variaram de 0.58 a mais próxima e, 1.71 a mais distante; quando analisamos os resultados obtidos para cadeia ossicular, temos uma variação que vai de 0.38 até 1.49. A membrana timpânica se encontra entre 0.85 e 1.96 de distância da trajetória simulada da broca. A trajetória da cortical do osso temporal até a escala timpânica, variou de 5.92 a 12.65. CONCLUSÃO: As medidas da relação, entre a broca e as estruturas anatômicas da orelha média e, a simulação da trajetória, mostraram que é possível executar com segurança a técnica de implante coclear percutâneo em crianças a partir de 32 semanas de gestação / INTRODUCTION: Literature shows changes in the temporal bone anatomy in children when compared with adults. More and more literature emphasizes the importance of children with congenital deafness should be implanted increasingly early. Anatomical radiologic studies are important for the development of surgical techniques that allow implanting new born. Percutaneous cochlear implant technique (through robotics) was developed in Vanderbilt University. So we created our main question \" Is it possible to implant new born children using the percutaneous technique? \" and we\'ll try to answer it in the course of this work. PATIENTS AND METHODS: Experimental study done in 9 stillbirth specimens with 32 and 40 weeks of age, submitted to CT study followed by reconstruction of the facial nerve, ossicular chain, tympanic membrane, labyrinth and cochlea. The CT evaluation and reconstruction was done with Improvise software, also used for measurements of the distances and in the simulation of the drill\'s trajectory (mm). RESULTS: The drill trajectory measurements to the facial nerve, ranged from 0.58 the nearest and the farthest 1.71, when we analyzed the results for ossicular chain, we have a range that goes from 0.38 to 1.49. The tympanic membrane is between 0.85 and 1.96 away from the simulated drill path. Cortical trajectory of the temporal bone to the scala tympani, ranged from 5.92 to 12.65. CONCLUSION: The measures of the relationship between the drill and the anatomical structures of the middle ear and the simulated trajectory, showed that it is possible to use safely the percutaneous cochlear implant technique in children of 32 weeks/old Cóclea Estudos experimentais Implante coclear Osso temporal/anatomia Ouvido médio Perda auditiva neurossensorial Cochlea Cochlear implantation Ear middle Experimental studies Hearing loss sensorineural Temporal bone/anatomy
159	Development of an objective procedure allowing frequency selectivity measurements using the masking function of auditory steady state evoked potentials Markessis, Emily 10 June 2010 (has links) <u><b>Introduction</u></b><p><p align = "justify">Les surdités cochléaires induisent, outre une audibilité réduite, une série de distorsions de la représentation neurale des sons. Deux des mécanismes à la base de ces distorsions sont d’une part une atteinte de la sélectivité fréquentielle et d’autre part des zones neuro-épithéliales non fonctionnelles. Tant le premier que le second mécanisme apparaissent dans une proportion variable et non prédictible d’un sujet à un autre. Deux tests permettent le diagnostic de ces atteintes spécifiques: la Courbe d’Accord (Tuning Curve: TC) et le Threshold Equalising Noise (TEN) test. La TC, mesurée par une technique psychoacoustique chez un adulte collaborant (Psychophysical TC: PTC), consiste en la mesure du niveau de bruit (masqueur) nécessaire pour masquer un son pur (signal) de fréquence et d’intensité fixes. Le TEN test consiste en la mesure des seuils auditifs dans le silence et en présence d’un bruit égalisateur de seuil (TEN). Ces tests qui requièrent des capacités cognitives adultes normales, ne sont pas applicables aux populations pédiatriques prélinguales.<p>Ce travail de thèse avait pour but le développement d’un équivalent objectif et non invasif des TCs et du TEN test applicable aux populations pédiatriques. La méthode objective choisie fut les potentiels auditifs stationnaires ou ASSEPs (Auditory Steady State Evoked Potentials). Les ASSEPs sont une réponse électrophysiologique cérébrale évoquée par un stimulus acoustique de longue durée modulé en amplitude et/ou en fréquence.</p align = "justify"><p><u><b>Méthodes & Résultats</u></b><p><p>Etape 1<p><p align = "justify">Les développements méthodologiques ont été réalisés sur l’espèce canine et humaine adulte. Les ASSEPs n’ayant jamais été préalablement enregistrés chez le chien, une première étape à consister à définir chez cette espèce les paramètres d’enregistrement optimaux (modulation en amplitude optimale) dont on sait qu’ils interagissent avec l’état veille-sommeil, avec la fréquence testée et probablement avec l’espèce animale investiguée. <p>A cette fin, les seuils auditifs obtenus chez 32 chiens à l’aide des ASSEPs ont été validés à cinq fréquences audiométriques par comparaison aux seuils obtenus avec les potentiels auditifs du tronc cérébral évoqués aux bouffées tonales. <p>Les seuils obtenus aux ASSEPs avec les paramètres optimaux d’enregistrement (légèrement différents des paramètres optimaux humains) étaient similaires à ceux obtenus aux bouffées tonales. <p>Ces résultats ont été publiés dans Clinical Neurophysiology (Markessis et al. 2006; 117: 1760-1771).</p align = "justify"><p>Etape 2<p><p align = "justify">La possibilité de mesurer des TCs à l’aide des ASSEPs (ASSEP-TCs) a été évaluée sur 10 chiens. Les données canines ont été comparées à des données de la littérature, çàd aux TC enregistrées chez d’autres espèces et avec d’autres méthodes. Des ASSEP-TCs ont également été enregistrées chez 7 humains adultes et confrontées aux PTCs obtenues chez les mêmes sujets. Les PTCs sont typiquement energistrées avec un signal sinusoïdal alors que le stimulus utilisé pour évoquer un ASSEP est une sinusoïde modulée en amplitude. L’effet des sinusoïdes modulées en amplitude sur les paramètres qualitatifs et quantitatifs des TCs a donc été évalué en comparant les PTCs obtenues avec un son pur et avec un son pur modulé en amplitude chez 10 humains adultes. <p>Les résultats ont révélé que les ASSEP-TCs enregistrées chez le chien et l’humain présentaient des paramètres qualitatifs et quantitatifs similaires respectivement à ceux décrits dans la littérature et aux PTCs. Par ailleurs, auncun effet des stimuli modulés en amplitude sur les paramètres des PTCs n’a été démontré.<p>Ces données ont été publiées dans Ear & Hearing (Markessis et al. 2009, 30: 43-53).</p align = "justify"><p>Etape 3<p><p align = "justify">Les ASSEP-TCs ont été validées chez 10 chiens en comparant les données aux TC enregistrées par électrocochléographie (Compound Action Potential TC: CAP-TC). Le masqueur utilisé pour les CAP-TCs est typiquement une sinusoïde alors que le masqueur utilisé pour les ASSEP-TCs est un bruit à bande étroite. Dès lors, une comparaison du type de masqueur (sinusoïde vs bruit à bande étroite) sur les paramètres des CAP-TCs et ASSEP-TCs a été réalisée chez 10 chiens.<p>Les ASSEP-TCs chez le chien se sont révélées qualitativement et quantitativement similaires aux CAP-TCs quel que soit le type de masqueur. Elles presentaient par ailleurs l’avantage d’être moins variables, plus précises et non invasives par rapport aux CAP-TCs. <p>Ces données ont été publiées dans International Journal of Audiology (Markessis et al. 2010, 49 ;455-62).</p align = "justify"><p>Etape 4<p><p align = "justify">Afin d’étudier la validité de la procédure à mettre en évidence des changements de sélectivité fréquentielle dus à une atteinte cochléaire, des ASSEP-TCs ont été obtenues chez 10 chiens cochléo-lésés suite à un trauma acoustique. Les Produits de Distorsion Acoustiques, les potentiels évoqués auditifs du tronc cérébral évoqués par un clic et les ASSEPs à cinq fréquences audiométriques ont été enregisrés afin de délimiter l’étendue de la lésion.<p>Les ASSEP-TCs ont été fortement altérées, mais pas comme attendu ni suggéré par les mesures fonctionnelles indiquant que le trauma acoustique a créé une lésion différente de celle espérée. <p>Cette étude doit être poursuivie, des lésions moins importantes créées et une validation histopathologique réalisée.</p align = "justify"><p>Etape 5<p><p align = "justify">Le TEN test a été mesuré à l’aide des ASSEPs (ASSEP-TEN) chez 12 adultes et cinq enfants normo-entendants. Les données adultes ont été confrontées aux données comportementales. L’effet des stimuli ASSEP (son pur modulé en amplitude) sur les TEN test a également été investigué en comparant les données comportementales obtenues avec une sinusoïde et avec une sinusoïde modulée en amplitude chez 24 adultes. <p>Les seuils masqués enregistrés aux ASSEPs étaient supérieurs à ceux mesurés par une épreuve comportementale. L’élévation des seuils masqués pose un problème potentiel de dynamique.<p>La procédure doit être testée chez des patients présentant une surdité cochléaire attendu que la différence entre les seuils auditifs mesurés aux ASSEPs et par une épreuve comportementale est moindre dans cette population. Dans la mesure où le problème de dynamique résiduelle persiste chez les patients malentendants, d’autres stimuli ou algorithmes d’enregistrement doivent être utilisés.</p align = "justify"><p>Etape 6<p><p align = "justify">Le TEN est un stimulus large bande. Il peut dès lors se révéler intolérable chez des patients présentant une atteinte auditive restreinte à une region fréquentielle. L’effet du filtrage du TEN sur les seuils et la sonie du TEN a été étudié chez 24 sujets normo-entendants et 35 patients présentant une perte cochléaire dans les hautes fréquences.<p>Le filtrage passe-haut du TEN s’est avéré être une solution satisfaisante.<p>Ces données ont été publiées dans International Journal of Audiology (Markessis et al. 2006; 45: 91-98).</p align = "justify"><p>Etape 7<p><p align = "justify">L’effet de l’intensité du TEN sur le diagnostic des zones neuro-épithéliales non fonctionnelles a été investigué chez 24 patients en mesurant les seuils masqués à quatre intensités de TEN différentes. La fiabilité du TEN test a également été évaluée. <p>Le TEN est une procédure fiable. L’intensité du TEN a affecté le diagnostic chez cinq patients. Ce résultat est interprété en termes de degré de l’atteinte du complexe neurosensoriel.<p>Ces données ont été publiées dans International Journal of Audiology (Markessis et al. 2009; 48: 55-62).</p align = "justify"><p><u><b>Conclusion</u></b><p><p align = "justify">Un algorithme permettant la mesure de TC et du TEN test objective à l’aide des ASSEPs a été développé. L’implémentation clinique de l’algorithme appliqué à l’enregistrement des CA paraît envisageable. Une importante étape de la corrélation entre modifications anatomiques (à l’aide de l’histopathologie) et physiologiques (ASSEP-TC et CAP-TC) est maintenant celle qui s’impose. Les données préliminaires obtenues sur le TEN test électrophysiologique chez des sujets normo-entendants suggèrent que son implémentation clinique puisse se heurter à un problème de dynamique si ce dernier est confirmé en présence de surdités cochléaires. Plusieurs pistes potentielles de solutions ont été avancées.</p align = "justify"> / Doctorat en Sciences biomédicales et pharmaceutiques / info:eu-repo/semantics/nonPublished Disciplines biomédicales diverses Hearing disorders Cochlea -- Physiology Psychoacoustics Neurophysiology Audition, Troubles de l' Cochlée -- Physiologie Psychoacoustique Neurophysiologie diagnosis dogs neurophysiology hearing disorder psychoacoustics
160	Vglut3 : un rôle essentiel dans la cochlée et implication dans la surdité DFNA25. / Vglut3 : an essential role in cochlea and implication in deafness DFNA25. Bersot, Tiphaine 19 December 2011 (has links) Avant sa libération, le glutamate est accumulé dans des vésicules synaptiques par trois transporteurs vésiculaires (VGLUT1-3). Les cellules ciliées internes (CCI) de la cochlée n'expriment que VGLUT3. Pour étudier son rôle dans la physiologie cochléaire, nous avons utilisé une lignée de souris dont le gène Slc17a8, qui code pour VGLUT3, a été invalidé par recombinaison homologue. Les mutants ne présentaient pas de réponse nerveuse à une stimulation sonore. Les mécanismes d'exocytose des CCI étaient normaux et leurs synapses normales en microscopie électronique. Des immunoblots montraient que le transporteur membranaire du glutamate GLAST, ainsi que les sous-unités GLUR2 et NR1 des récepteurs AMPA et NMDA étaient toujours exprimées. Enfin, des potentiels auditifs du tronc cérébral étaient enregistrés après une stimulation électrique au niveau de la fenêtre ronde. Toutefois, nos résultats indiquent des diminutions de ~50% des synapses afférentes et de ~40% des neurones auditifs primaires ainsi qu'une réduction importante des terminaisons efférentes latérales sous les CCI.SLC17A8 est responsable de la surdité de perception non syndromique dominante DFNA25. Nous avons identifié une mutation dans l'exon 5 conduisant au remplacement de l'Alanine211 en Valine. Cette Alanine est conservée dans les VGLUT3 de différentes espèces ainsi que dans les VGLUT1-3 humains, suggérant un rôle fonctionnel important pour cet acide aminé. Nous avons caractérisé les propriétés biochimiques de la mutation A211V en culture de cellules. Le transporteur muté était correctement adressé aux boutons présynaptiques. Cependant, la mutation pA211V entraîne un défaut d'expression important en partie expliqué par le fait que le codon codant la valine est un codon rare. De plus, les études du transport de glutamate ont montré que la forme mutée est hyperactive par rapport à la forme native. L'ensemble de ces résultats montre que la mutation entraine un phénotype cellulaire complexe. / Before its release, glutamate is accumulated into synaptic vesicles by three vesicular glutamate transporters (VGLUT1-3). Only VGLUT3 is expressed in the inner hair cells (IHCs) of the cochlea. To study its role in the hearing physiology, we used a mouse in which the Slc17a8 gene, which encodes VGLUT3, has been null-mutated. In this VGLUT3-/- mouse, no auditory nerve response to acoustic stimuli could be recorded. All the others cochlear potentials were normal. The genetic deletion of Slc17a8 in mice resulted in a profound deafness, without altering the IHCs synapse morphology and the synaptic vesicles turnover. Using western blot, we then observed that the glutamate-aspartate transporter GLAST and the GLUR2 and NR1 subunits of AMPA and NMDA receptors were always expressed. Finally, auditory brainstem responses could be elicited by electrical stimuli on the round window. However, VGLUT3-/- IHCs presented a ~50% loss of IHCs synapses and a ~40% loss of primary auditory neurons. The number of lateral olivocochlear synapses with primary auditory neurons dendrites was strongly reduced.The SLC17A8 gene is responsible for DFNA25, an autosomal dominant progressive, high-frequency nonsyndromic deafness. We identified a heterozygous non-synonymous missense mutation in exon 5, leading to the amino acid change p.A211V. The A211 residue is conserved in VGLUT3 across species and in all the human VGLUT subtypes (VGLUT1-3), suggesting an important functional role. We characterized the biochemical properties of the A211V mutation in cell culture. Our results suggest that the mutated VGLUT3 was correctly addressed at the presynaptic boutons. However, the pA211V mutation induced an expression decrease because the valine codon is a rare codon. Moreover, the glutamate uptake is increased with the mutated VGLUT3. All these results shows that this mutation involves a complex cellular phenotype. Cochlée Transporteur vésiculaire du glutamate Neurotransmission glutamatergique Cellules ciliées internes Surdité génétique Audition Cochlea Vesicular glutamate transporter Glutamatergic neurotransmission Inner hair cells Genetic deafness Hearing

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