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1.
听觉系统是接受、传输、分析、处理声音信息的特殊感觉系统。从20世纪70年代至今对听觉系统的研究进展迅速。耳蜗足听觉感受器所在之处,其结构复杂,但中学生物学教材中对耳蜗结构阐述很简单,一些中学教师对耳蜗的结构了解较少,冈此本文就耳蜗的解剖结构及生理功能作一介绍、  相似文献   

2.
目的:了解链霉素对鸟听觉毒性的作用。方法:选33只健康成年虎皮鹦鹉,不同剂量的链霉素肌肉注射15日,脑干听觉诱发电位测试外周的听觉敏度和听觉通路中神经的传导和传递能力。结果:链霉素对鸟听觉有毒性作用。结论:用链霉素处理鸟可以制作聋鸟模型。  相似文献   

3.
本文用辣根过氧化物酶注入鸣禽鸟蜡嘴雀和锡嘴雀,耳蜗内顺行追踪方法,均在不同侧延脑的NM和NA获标记纤维。结果表明蜡嘴和锡嘴雀听觉低级中枢由NM和NA两部分组成。  相似文献   

4.
视网膜母细胞瘤蛋白虽然是一种抑癌蛋白,但其在听觉系统发育过程中起到重要调控作用。与前庭毛细胞相比,视网膜母细胞瘤蛋白可能在耳蜗毛细胞的发育过程中扮演更加重要的角色。本文主要就视网膜母细胞瘤蛋白在内耳感觉祖细胞的细胞周期退出、细胞命运决定和分化以及毛细胞成熟、存活等各个阶段的作用进行综述,并分析了它在毛细胞再生研究中的重要价值。暂时阻断视网膜母细胞瘤蛋白表达可能为毛细胞再生提供有效途径,开辟听力损伤修复的新方向。  相似文献   

5.
目的:电子耳蜗是一个帮助聋人恢复听觉的装置。它根据人耳的仿生学原理,用有限个电极刺激神经以恢复聋人听觉。目前实际应用的电子耳蜗技术已经能够在安静环境下帮助聋人恢复一定的听觉。本文在使用GIS方案的基础上,采取了频谱增强的方法,以提高电子耳蜗的在噪声环境下的性能。另外采用计算机仿真及声音合成的方法,以评估耳蜗植入者听到的声音。本实验获得了比较好的试听效果。其中提出的方法对耳子耳蜗的研究和工程现实具有一定的意义。  相似文献   

6.
对近年来听觉反馈在鸣禽鸣唱学习可塑性方面的研究进行综述.鸣禽的鸣曲学习与人类的语言学习都是一种依赖于听觉反馈的模仿学习.在鸣曲学习过程中,幼鸟根据听觉反馈的信息对鸣曲进行比较和修正,使其不断完善;在鸣曲维持过程中,成鸟通过听觉反馈实时监测自己鸣曲的完整性与准确性,使鸣曲保持稳定.鸣曲的输出与听觉反馈信息在鸟脑中得到整合,并指导下一次鸣唱做出适当的调整.近年来,这种感觉与运动信息在鸣禽发声核团中的整合机制逐渐引起了国内外研究者的兴趣.其中,新纹状体巨细胞核外侧部(LMAN)神经元对自鸣曲(BOS)高度选择性的听觉应答在鸣曲去稳定化过程中的作用,以及高级发声中枢(HVC)中镜像神经元的发现,为今后的研究提供了重要的线索.  相似文献   

7.
Yu L  Tang H 《生理科学进展》2008,39(1):53-56
近几年的研究发现,在耳蜗基底膜的外毛细胞膜上有一种新奇的蛋白质:prestin(马达蛋白),它能感受细胞膜电位的变化,进而发生构象改变,引发外毛细胞的形状和表面积的改变.Prestin作为一种独特的马达蛋白,能驱动耳蜗外毛细胞的电能动性(electromotility),产生耳蜗的放大器作用,因而使哺乳动物的听觉具有高度的敏感性,广阔的听觉域,敏锐的频率选择性.这种蛋白质的缺失或基因的突变会导致听觉功能严重受损,对于prestin的深入细致的研究,也许可以使人们进一步认识和理解哺乳动物的听觉调谐机制,通过对这种蛋白质基因的表达的调控,是否能够防治一些与之相关的疾病?这或许将是今后听觉研究领域的一个重要课题.  相似文献   

8.
睫状神经营养因子对听觉损伤的保护作用   总被引:3,自引:1,他引:2  
本研究以耳廓反射、听觉脑干诱发电位、耳蜗生物电和耳蜗铺片组织学检测为指标,观察重组人睫状神经营养因子对豚鼠庆大霉素耳毒性的防治作用。实验结果表明,睫状神经营养因子能减轻庆大霉素对耳蜗及听神经的损害,具有保护听觉功能的作用。  相似文献   

9.
本文将辣根过氧化物酶(HRP)注入鹌鹑耳蜗内,应用HRP在行标记方法对耳蜗核进行了研究,结果在同侧的角核和前庭外侧核发现有密集的标记终未,结果表明延髓的角核和前庭外侧是组成延髓听觉中枢--耳蜗核的两个亚核,耳蜗核是听觉上行通路中在脑内的第一级神经元的换元站。  相似文献   

10.
猫耳蜗电图中N_2波起源的分析   总被引:4,自引:0,他引:4  
魏保龄  康健  曲非 《生理学报》1986,38(5):535-538
在35只猫进行了耳蜗电图、听觉脑干电反应及耳蜗核局部电位的同时描记,将普鲁卡因或海人酸微量注入耳蜗核内,观察电位的变化,以分析耳蜗电图中N_2 波的起源。实验结果表明:猫的 N_2 波来源于外周第一级神经元冲动的成分和耳蜗核电活动的成分。  相似文献   

11.
12.
The cochlea of the mammalian inner ear contains three rows of outer hair cells and a single row of inner hair cells. These hair cell receptors reside in the organ of Corti and function to transduce mechanical stimuli into electrical signals that mediate hearing. To date, the molecular mechanisms underlying the maintenance of these delicate sensory hair cells are unknown. We report that targeted disruption of Barhl1, a mouse homolog of the Drosophila BarH homeobox genes, results in severe to profound hearing loss, providing a unique model for the study of age-related human deafness disorders. Barhl1 is expressed in all sensory hair cells during inner ear development, 2 days after the onset of hair cell generation. Loss of Barhl1 function in mice results in age-related progressive degeneration of both outer and inner hair cells in the organ of Corti, following two reciprocal longitudinal gradients. Our data together indicate an essential role for Barhl1 in the long-term maintenance of cochlear hair cells, but not in the determination or differentiation of these cells.  相似文献   

13.
Cochlear microphonics (CMs), which represent the electrical activity of hair cells, and compound action potentials (CAPs), which represent the activity of the auditory nerve, were recorded from the round window of the inner ear, in owlets aged between 5 and 97 days posthatching, i.e., from soon after hatching to beyond fledgling. At the earliest ages examined, animals showed very insensitive CM and virtually no CAP responses. Thus, hearing in barn owls develops entirely posthatching and the birds appear to be profoundly deaf well into the second week. Thresholds improved gradually after that and CMs reached their adult sensitivity at 5 weeks posthatching at all frequencies. Compound action potential responses appeared progressively later with increasing frequency. Adult neural sensitivity was achieved about 1 week later than for the CM responses at most frequencies, but took until 9–10 weeks posthatching at the highest frequencies (8–10 kHz). This indicates an apex-to-base maturation sequence of neural sensitivity within the cochlea, with a disproportionately long period to maturity for the most basal regions. Compound action potential amplitudes matured even later, at about 3 months posthatching, at all frequencies. This suggests a prolonged immaturity in the temporal synchrony of spiking in the auditory nerve.  相似文献   

14.
甲状腺激素对豚鼠卡那霉素中毒性耳聋的预防作用   总被引:6,自引:0,他引:6  
卡那霉素、庆大霉素等抗生素常引起耳聋,目前尚无较好的防治方法。卡那霉素对内耳的毒性作用,主要先影响有关的酶功能,继而破坏毛细胞而致聋。甲状腺激素具有促进蛋白质合成、增强细胞生物氧化的功能。因此可能具有减轻卡那霉素耳毒性的作用。本实验以耳廓反射、内耳生物电及耳蜗铺片为指标,观察甲状腺激素对卡那霉素耳中毒的预防。实验豚鼠分两组,各13只,对照组每天注射卡那霉素300mg/kg,共10天;甲状腺素组先隔天服甲状腺片20mg共四次,以后给予与对照组相同剂量卡那霉素,同时仍隔天服甲状腺片20mg直至停药后16天,前后总共服17次。结果:(1)耳廓反射阈变化,对8、4、2KHz三个频率听力均下降的耳,对照组为11只耳,甲状腺素组为3只耳,两者差异显著。听力下降的频率范围及程度,对照组比甲状腺素组更大。对照组听力下降开始出现的时间明显早于甲状腺素组;(2)内耳生物电,0~80dβ不同程度短声引起的耳蜗微音器电位与听神经动作电位幅值甲状腺素组动物均高于对照组;(8)耳蜗铺片,对照组大部分动物耳蜗各回的毛细胞严重变性缺损,甲状腺素组耳蜗病变仅局限在底回。以上结果表明甲状腺激素能减轻卡那霉素的耳毒性,为耳毒性抗生素致聋的防治提供了一条新的研究途径。  相似文献   

15.
ATP-gated non-selective cation channels assembled from P2X3 receptor subunits contribute to transduction and neurotransmitter signaling in peripheral sensory systems and also feature prominently in the development of the central nervous system. In this study, P2X3 receptor expression was characterized in the mouse cochlea from embryonic day 18 (E18) using confocal immunofluorescence. From E18 to P6, spiral ganglion neuron cell bodies and peripheral neurites projecting to the inner and outer hair cells were labeled. The inner spiral plexus associated with the inner hair cell synapses had a stronger fluorescence signal than outer spiral bundle fibers which provide the afferent innervation to the outer hair cells. Labeling in the cell bodies and peripheral neurites diminished around P6, and was no longer detected after the onset of hearing (P11, P17, adult). In opposition to the axiom that P2X3 expression is neuron-specific, inner and outer sensory hair cells were labeled in the base and mid turn region at E18, but at P3 only the outer hair cells in the most apical region of the cochlea continued to express the protein. These data suggest a role for P2X3 receptor-mediated purinergic signaling in cochlear synaptic reorganization, and establishment of neurotransmission, which occurs just prior to the onset of hearing function.  相似文献   

16.
17.
Osseous inner ear structures and hearing in early marsupials and placentals   总被引:2,自引:0,他引:2  
Based on the internal anatomy of petrosal bones as shown in radiographs and scanning electron microscopy, the inner ear structures of Late Cretaceous marsupials and placentals (about 65 Myr ago) from the Bug Creek Anthills locality of Montana, USA, are described. The inner ears of Late Cretaceous marsupials and placentals are similar to each other in having the following tribosphenic therian synapomorphies: a fully coiled cochlea, primary and secondary osseous spiral laminae, the perilymphatic recess merging with the scala tympani of the cochlea, an aqueductus cochleae, a true fenestra cochleae, a radial pattern of the cochlear nerve and an elongate basilar membrane extending to the region between the fenestra vestibuli and fenestra cochleae. The inner ear structures of living therians differ from those of their Late Cretaceous relatives mainly in having a greater number of spiral turns of the cochlea and a longer basilar membrane. Functionally, a coiled cochlea not only permits the development of an elongate basilar membrane within a restricted space in the skull but also allows a centralized nerve system to innervate the elongate basilar membrane. Qualitative and quantitative analyses show that, with a typical therian inner ear, Late Cretaceous marsupials and placentals were probably capable of high-frequency hearing.  相似文献   

18.
The physical characteristics of vocalization were examined in budgerigars (Melopsittacus undulatus) deafened at the age of about 28 days. Autocorrelation was used in the analysis, with 2 parameters: 1) inter-element intervals and 2) amplitudes of all sound elements of the vocalization. The deafened birds developed the temporal pattern specific to normal warble song in autocorrelograms. However, abnormalities were found in the frequency spectrum of elements. The temporal pattern of warble song might be an innate character, because auditory feedback is unnecessary for its development.  相似文献   

19.
The vertebrate-restricted carcinoembryonic antigen gene family evolves extremely rapidly. Among their widely expressed members, the mammal-specific, secreted CEACAM16 is exceptionally well conserved and specifically expressed in the inner ear. To elucidate a potential auditory function, we inactivated murine Ceacam16 by homologous recombination. In young Ceacam16(-/-) mice the hearing threshold for frequencies below 10 kHz and above 22 kHz was raised. This hearing impairment progressed with age. A similar phenotype is observed in hearing-impaired members of Family 1070 with non-syndromic autosomal dominant hearing loss (DFNA4) who carry a missense mutation in CEACAM16. CEACAM16 was found in interdental and Deiters cells and was deposited in the tectorial membrane of the cochlea between postnatal days 12 and 15, when hearing starts in mice. In cochlear sections of Ceacam16(-/-) mice tectorial membranes were significantly more often stretched out as compared with wild-type mice where they were mostly contracted and detached from the outer hair cells. Homotypic cell sorting observed after ectopic cell surface expression of the carboxyl-terminal immunoglobulin variable-like N2 domain of CEACAM16 indicated that CEACAM16 can interact in trans. Furthermore, Western blot analyses of CEACAM16 under reducing and non-reducing conditions demonstrated oligomerization via unpaired cysteines. Taken together, CEACAM16 can probably form higher order structures with other tectorial membrane proteins such as α-tectorin and β-tectorin and influences the physical properties of the tectorial membrane. Evolution of CEACAM16 might have been an important step for the specialization of the mammalian cochlea, allowing hearing over an extended frequency range.  相似文献   

20.
Mice that lack caspase-3, which functions in apoptosis, were generated by gene targeting and shown to undergo hearing loss. The ABR threshold of the caspase-3(-/-) mice was significantly elevated compared to that of caspase-3(+/+) mice at 15 days of age and was progressively elevated further by 30 days. Distortion product otoacoustic emissions were not detectable in caspase-3(-/-) mice at 15 days of age. Caspase-3(-/-) mice exhibited marked degeneration of spiral ganglion neurons and a loss of inner and outer hair cells in the cochlea at 30 days of age, although no such changes were apparent at 15 days. The degenerating neurons manifested features, including cytoplasmic vacuolization, distinct from those characteristic of apoptosis. Spiral ganglion neurons and cochlear hair cells thus appear to require caspase-3 for survival but not for initial development. The mapping of both the human caspase-3 gene and the locus responsible for an autosomal dominant, nonsyndromic form of hearing loss (DFNA24) to chromosome 4q35 suggests that the caspase-3(-/-) mice may represent a model of this human condition.  相似文献   

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