The Human Spiral Ganglion

Anniko, Matti; Arnold, W.; Stigbrand, Torgny; Strom, Alexander

doi:10.1159/000276714

Cited by 26 publications

(14 citation statements)

References 45 publications

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“…The specific staining of type-2 cells for mAb NF-H is attributable to the abundant, highly phosphorylated NF-H, which seems to be necessary for the imme diate assembly of NFs in order to stabilize the cytoskeleton [10], The specificity of mAb NF-M for type-1 cells can ORL 1997;59:258-262be explained by its larger axon diameter with more NFs as observed in the dorsal root ganglion [21,22] and vestibu lar ganglion [9], though its functional implication needs to be clarified. mAb NF-H has been noted to stain type-2 spiral gan glion cells specifically [2, 6-8, 10, 12-15], which can pos sibly be attributed to the more abundant NFs in type-2 cells than in type-1 cells as identified ultrastructurally [23,24], Our findings on the distribution of NF-M are consis tent with those of Anniko et al [2] and Berglund and Ryugo [10] in human specimens, where all the spiral ganglion cells seemed to be stained. In contrast, other studies claim that NF-M and NF-L occur in type-2 spiral ganglion cells in rodents and the human embryo [7,8,[13][14][15], Whether or not this discrepancy is due to differences in mAbs or in species needs to be clarified.…”

Section: Image Analysis Of Nfs In Human Spiral Ganglionsupporting

confidence: 85%

“…The immunomorphology of the human inner ear has been studied extensively but mainly qualitatively during the past decade [1,2], Recent developments in computerassisted morphological techniques have focused on image analysis, which is intended to analyse and compare immunostained specimens providing quantitative and ob jective information.…”

Section: Introductionmentioning

confidence: 99%

“…Neurofilaments (NFs), which belong to the group of intermediate filaments, have been found in both the cen tral and the peripheral nervous system [3][4][5] including the stato-acoustic ganglion [1,2,[6][7][8][9][10][11][12][13][14][15]. Their functions are mechanical support and intracellular transport of sub stances and organelles along the axons.…”

Section: Introductionmentioning

confidence: 99%

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Image Analysis of Neurofilament Immunoreactivity in Human Spiral Ganglion

Hsu

Anniko²,

Kubo³

et al. 1997

ORL

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Computer-assisted image analysis was used to study the immunoreactivity to NF-L, NF-M and NF-H in human spiral ganglion cells. The concentrations, represented by the relative mean grey of NF-L, NF-M and NF-H, were calculated and compared. The cell-area mean-grey correlations for NF-L, NF-M and NF-H were analysed and calculated, showing that NF-M is more specific to the larger cells (type 1?) and NF-H is more specific for the smaller cells (type 2?), while NF-L is non-specific for cell size. These findings confirm several previous assumptions by providing a quantitative basis. We conclude that image analysis is a useful – even essential – tool for the analysis of immunostained temporal bone sections.

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Section: Image Analysis Of Nfs In Human Spiral Ganglionsupporting

confidence: 85%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Image Analysis of Neurofilament Immunoreactivity in Human Spiral Ganglion

Hsu

Anniko²,

Kubo³

et al. 1997

ORL

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“…Synaptophysin is a well known marker for synaptic vesicles and is present in auditory nerve terminals in the organ of Corti. It can also act as a calcium-binding protein and is expressed in SGNs of the mammalian cochlea (Anniko et al, 1995;Rask-Andersen et al, 2000;Khalifa et al, 2003).…”

Section: Discussionmentioning

confidence: 99%

Nuclear Factor κB Deficiency Is Associated with Auditory Nerve Degeneration and Increased Noise-Induced Hearing Loss

Lang¹,

Schulte²,

Zhou³

et al. 2006

J. Neurosci.

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Degeneration of the spiral ganglion neurons (SGNs) of the auditory nerve occurs with age and in response to acoustic injury. Histopathological observations suggest that the neural degeneration often begins with an excitotoxic process affecting the afferent dendrites under the inner hair cells (IHCs), however, little is known about the sequence of cellular or molecular events mediating this excitotoxicity. Nuclear factor B (NFB) is a transcription factor involved in regulating inflammatory responses and apoptosis in many cell types. NFB is also associated with intracellular calcium regulation, an important factor in neuronal excitotoxicity. Here, we provide evidence that NFB can play a central role in the degeneration of SGNs. Mice lacking the p50 subunit of NFB (p50 Ϫ/Ϫ mice) showed an accelerated hearing loss with age that was highly associated with an exacerbated excitotoxic-like damage in afferent dendrites under IHCs and an accelerated loss of SGNs. Also, as evidenced by immunostaining intensity, calcium-buffering proteins were significantly elevated in SGNs of the p50 Ϫ/Ϫ mice. Finally, the knock-out mice exhibited an increased sensitivity to low-level noise exposure. The accelerated hearing loss and neural degeneration with age in the p50 Ϫ/Ϫ mice occurred in the absence of concomitant hair cell loss and decline of the endocochlear potential. These results indicate that NFB activity plays an important role in protecting the primary auditory neurons from excitotoxic damage and age-related degeneration. A possible mechanism underlying this protection is that the NFB activity may help to maintain calcium homeostasis in SGNs.

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“…Electrophysiological (Mo and Davis, 1997a,b) and immunohistochemical (Romand et al, 1990;Lopez et al, 1995;Anniko et al, 1995;Salih et al, 1999;Adamson et al, 1999) studies have revealed an unexpected heterogeneity in the firing features and voltage-dependent ionic currents of spiral ganglion neurons that appear to vary as a function of position in the cochlea (Adamson et al, 1999;Davis et al, 2001). To determine whether these electrophysiological features are subject to extrinsic regulation, we evaluated the effects of neurotrophins on neuronal firing patterns and on ion channel distribution of postnatal spiral ganglion neurons placed in tissue culture.…”

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confidence: 99%

Opposite Actions of Brain-Derived Neurotrophic Factor and Neurotrophin-3 on Firing Features and Ion Channel Composition of Murine Spiral Ganglion Neurons

2002

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It is now well established that sensory neurons and receptors display characteristic morphological and electrophysiological properties tailored to their functions. This is especially evident in the auditory system, where cells are arranged tonotopically and are highly specialized for precise coding of frequency-and timing-dependent auditory information. Less well understood, however, are the mechanisms that give rise to these biophysical properties. We have provided insight into this issue by using whole-cell current-clamp recordings and immunocytochemistry to show that BDNF and NT-3, neurotrophins found normally in the cochlea, have profound effects on the firing properties and ion channel distribution of spiral ganglion neurons in the murine cochlea. Exposure of neurons to BDNF caused all neurons, regardless of their original cochlear position, to display characteristics of the basal neurons. Conversely, NT-3 caused cells to show the properties of apical neurons. These results are consistent with oppositely oriented gradients of these two neurotrophins and/or their high-affinity receptors along the tonotopic map, and they suggest that a combination of neurotrophins are necessary to establish the characteristic firing features of postnatal spiral ganglion neurons.

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The Human Spiral Ganglion

Cited by 26 publications

References 45 publications

Image Analysis of Neurofilament Immunoreactivity in Human Spiral Ganglion

Image Analysis of Neurofilament Immunoreactivity in Human Spiral Ganglion

Nuclear Factor κB Deficiency Is Associated with Auditory Nerve Degeneration and Increased Noise-Induced Hearing Loss

Opposite Actions of Brain-Derived Neurotrophic Factor and Neurotrophin-3 on Firing Features and Ion Channel Composition of Murine Spiral Ganglion Neurons

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