Your search keyword '"auditory brainstem"' showing total 518 results

1. Loss of C1q alters the auditory brainstem response.

Author

Chokr, Sima M., Bui-Tran, Ashley, and Cramer, Karina S.

Abstract

Neural circuits in the auditory brainstem compute interaural time and intensity differences used to determine the locations of sound sources. These circuits display features that are specialized for these functions. The projection from the ventral cochlear nucleus (VCN) to the medial nucleus of the trapezoid (MNTB) body travels along highly myelinated fibers and terminates in the calyx of Held. This monoinnervating synapse emerges during development as multiple inputs are eliminated. We previously demonstrated that elimination of microglia with a colony stimulating factor-1 inhibitor results in impaired synaptic pruning so that multiple calyceal terminals reside on principal cells of MNTB. This inhibitor also resulted in impaired auditory brainstem responses (ABRs), with elevated thresholds and increased peak latencies. Loss of the microglial fractalkine receptor, CX3CR1, decreased peak latencies in the ABR. The mechanisms underlying these effects are not known. One prominent microglial signaling pathway involved in synaptic pruning and plasticity during development and aging is the C1q-initiated compliment cascade. Here we investigated the classical complement pathway initiator, C1q, in auditory brainstem maturation. We found that C1q expression is detected in the MNTB by the first postnatal week. C1q levels increased with age and were detected within microglia and surrounding the soma of MNTB principal neurons. Loss of C1q did not affect microglia-dependent calyceal pruning. Excitatory and inhibitory synaptic markers in the MNTB and LSO were not altered with C1q deletion. ABRs showed that C1q KO mice had normal hearing thresholds but shortened peak latencies. Altogether this study uncovers the developmental time frame of C1q expression in the sound localization pathway and shows a subtle functional consequence of C1q knockdown. [ABSTRACT FROM AUTHOR]

Published

2024

2. Anatomy of superior olivary complex and lateral lemniscus in Etruscan shrew

Author

Alina C. Zacher and Felix Felmy

Subjects

Auditory brainstem, Etruscan shrew, Inferior colliculus, Lateral lemniscus, Superior olivary complex, Medicine, Science

Abstract

Abstract Based on the auditory periphery and the small head size, Etruscan shrews (Suncus etruscus) approximate ancestral mammalian conditions. The auditory brainstem in this insectivore has not been investigated. Using labelling techniques, we assessed the structures of their superior olivary complex (SOC) and the nuclei of the lateral lemniscus (NLL). There, we identified the position of the major nuclei, their input pattern, transmitter content, expression of calcium binding proteins (CaBPs) and two voltage-gated ion channels. The most prominent SOC structures were the medial nucleus of the trapezoid body (MNTB), the lateral nucleus of the trapezoid body (LNTB), the lateral superior olive (LSO) and the superior paraolivary nucleus (SPN). In the NLL, the ventral (VNLL), a specific ventrolateral VNLL (VNLLvl) cell population, the intermediate (INLL) and dorsal (DNLL) nucleus, as well as the inferior colliculus’s central aspect were discerned. INLL and VNLL were clearly separated by the differential distribution of various marker proteins. Most labelled proteins showed expression patterns comparable to rodents. However, SPN neurons were glycinergic and not GABAergic and the overall CaBPs expression was low. Next to the characterisation of the Etruscan shrew’s auditory brainstem, our work identifies conserved nuclei and indicates variable structures in a species that approximates ancestral conditions.

Published

2024

3. Postnatal functional integrity of the brainstem auditory pathway in late preterm infants born of small-for-gestation age: how different from those born of appropriate-for-gestation.

Author

Jiang, Ze Dong, Wang, Cui, and Jiang, James K.

Subjects

*PREMATURE infants, *AUDITORY pathways, *BRAIN stem, *NEURAL conduction

Abstract

It is unclear whether there is any postnatal abnormality in brainstem auditory function in late preterm small-for-gestational-age (SGA) infants. We investigated the functional integrity of the brainstem auditory pathway at 4 months after term in late preterm SGA infants and defined differences from appropriate-for-gestational age (AGA) infants. The maximum length sequence brainstem evoked response (MLS BAER) was recorded and analyzed in 24 SGA (birthweight < 3rd centile) infants and 28 AGA infants (birthweight > 10th centile). All infants were born at 33–36-week gestation without major perinatal and postnatal problems. We found that I-V interval in SGA infants was shorter than in AGA infants at higher click rates and significantly shorter at the highest rate of 910/s. Of the two smaller intervals, I-III interval was significantly shorter in SGA infants than in AGA infants at higher click rates of 455 and 910/s clicks, whereas III-V interval was similar in the two groups. The III-V/I-III interval ratio in SGA infants tended to be greater than in AGA infants at all rates and was significantly greater at 455 and 910/s clicks. The slope of I-III interval-rate functions in SGA infants was moderately smaller than in AGA infants. Conclusions: The main and fundamental difference between late preterm SGA and AGA infants was a significant shortening in the MLS BAER I-III interval in SGA infants at higher click rates, suggesting moderately faster neural conduction in the caudal brainstem regions. Postnatal neural maturation in the caudal brainstem regions is moderately accelerated in late preterm SGA infants. What is Known: • At 40 weeks of postconceptional age, late preterm SGA infants manifested a mild delay in neural conduction in the auditory brainstem. What is New: • At 56 weeks of postconceptional age, late preterm SGA infants manifested moderately faster neural conduction in the caudal brainstem regions. • Postnatal neural maturation is moderately accelerated in the caudal brainstem regions of late preterm SGA infants. [ABSTRACT FROM AUTHOR]

Published

2024

4. Does age protect against loss of tonotopy after acute deafness in adulthood?

Author

Nicole Rosskothen-Kuhl, Sarah Green, and Till F. Jakob

Subjects

aging, adult hearing loss, auditory brainstem, tonotopy, cochlear implant, cochlear nucleus, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The mammalian auditory system develops a topographical representation of sound frequencies along its pathways, also called tonotopy. In contrast, sensory deprivation during early development results in no or only rudimentary tonotopic organization. This study addresses two questions: (1) How robust is the central tonotopy when hearing fails in adulthood? (2) What role does age play at time of deafness? To address these questions, we deafened young and old adult rats with previously normal hearing. One month after deafening, both groups were unilaterally supplied with cochlear implants and electrically stimulated for 2 h. The central auditory neurons, which were activated as a result of the local electrical intracochlear stimulation, were visualized using Fos staining. While the auditory system of young rats lost the tonotopic organization throughout the brainstem, the auditory system of the older rats mainly sustained its tonotopy. It can be proposed that plasticity prevails in the central auditory system of young adult rats, while network stability prevails in the brains of aging rats. Consequently, age may be an important factor in protecting a hearing-experienced adult auditory system from a rapid loss of tonotopy when suffering from acute hearing loss. Furthermore, the study provides compelling evidence that acute deafness in young adult patients should be diagnosed as early as possible to prevent maladaptation of the central auditory system and thus achieve the optimal hearing outcome with a hearing prosthesis.

Published

2024

5. Loss of C1q alters the auditory brainstem response

Author

Sima M. Chokr, Ashley Bui-Tran, and Karina S. Cramer

Subjects

auditory brainstem, microglia, medial nucleus of the trapezoid body (MNTB), neural development, complement, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Neural circuits in the auditory brainstem compute interaural time and intensity differences used to determine the locations of sound sources. These circuits display features that are specialized for these functions. The projection from the ventral cochlear nucleus (VCN) to the medial nucleus of the trapezoid (MNTB) body travels along highly myelinated fibers and terminates in the calyx of Held. This monoinnervating synapse emerges during development as multiple inputs are eliminated. We previously demonstrated that elimination of microglia with a colony stimulating factor-1 inhibitor results in impaired synaptic pruning so that multiple calyceal terminals reside on principal cells of MNTB. This inhibitor also resulted in impaired auditory brainstem responses (ABRs), with elevated thresholds and increased peak latencies. Loss of the microglial fractalkine receptor, CX3CR1, decreased peak latencies in the ABR. The mechanisms underlying these effects are not known. One prominent microglial signaling pathway involved in synaptic pruning and plasticity during development and aging is the C1q-initiated compliment cascade. Here we investigated the classical complement pathway initiator, C1q, in auditory brainstem maturation. We found that C1q expression is detected in the MNTB by the first postnatal week. C1q levels increased with age and were detected within microglia and surrounding the soma of MNTB principal neurons. Loss of C1q did not affect microglia-dependent calyceal pruning. Excitatory and inhibitory synaptic markers in the MNTB and LSO were not altered with C1q deletion. ABRs showed that C1q KO mice had normal hearing thresholds but shortened peak latencies. Altogether this study uncovers the developmental time frame of C1q expression in the sound localization pathway and shows a subtle functional consequence of C1q knockdown.

Published

2024

6. GABAB receptor‐mediated modulation in the developing dorsal nucleus of the lateral lemniscus.

Author

Javadova, Amina and Felmy, Felix

Subjects

*ACTION potentials, *MONGOLIAN gerbil, *GERBILS, *NEURAL transmission, *BRAIN stem, *NEURONS, *POTASSIUM channels, *CALCIUM-dependent potassium channels

Abstract

The dorsal nucleus of the lateral lemniscus (DNLL) is a GABAergic, reciprocally connected auditory brainstem structure that continues to develop postnatally in rodents. One key feature of the DNLL is the generation of a strong, prolonged, ionotropic, GABAA receptor‐mediated inhibition. Possible GABAB receptor‐mediated signalling is unexplored in the DNLL. Here, we used Mongolian gerbils of either sex to describe GABAB receptor‐mediated modulation of postsynaptic potassium currents and synaptic inputs in postnatal (P) animals of days 10/11 and 23–28. Throughout development, we observed the presence of a Baclofen‐activated GABAB receptor‐enhanced potassium outward conductance that is capable of suppressing action potential generation. In P10/11, old gerbils GABAB receptor activation enhances glutamatergic and suppresses ionotropic GABAergic synaptic transmission. During development, this differential modulation becomes less distinct, because in P22–28, old animals Baclofen‐activated GABAB receptors rather enhance ionotropic GABAergic synaptic transmission, whereas glutamatergic transmission is both enhanced and suppressed. Blocking GABAB receptors causes an increase in ionotropic GABAergic transmission in P10/11 old gerbils that was independent on stimulation frequency but depended on the type of short‐term plasticity. Together with the lack of Baclofen‐induced changes in the synaptic paired‐pulse ratio of either input type, we suggest that GABAB receptor‐mediated modulation is predominantly postsynaptic and activates different signalling cascades. Thus, we argue that in DNLL neurons, the GABAB receptor is a post‐synaptically located signalling hub that alters signalling cascades during development for distinct targets. [ABSTRACT FROM AUTHOR]

Published

2024

7. The click-evoked auditory brainstem response is not affected in auditory processing disorder: a meta-analysis systematic review

Author

Akshay R. Maggu, Ying Yu, and Tobias Overath

Subjects

click-evoked ABR, Auditory Processing Disorder (APD), APD diagnosis, electrophysiology, auditory brainstem, Medicine

Abstract

IntroductionAmong several controversies surrounding the field of Auditory Processing Disorder (APD), one of the central unresolved topics is the putative neural origin of APD. More specifically, it is debated whether basic sensory auditory neural processes are affected in individuals with APD. The objective of the current study was to understand whether or not basic sensory auditory neural processes at the level of the brainstem are affected in those with APD.MethodsWe approached this question by conducting a meta-analysis of studies that compared the Auditory Brainstem Response (ABR) to brief non-speech sounds in individuals with vs. without APD. The ultimate criterion for a study to be included in this meta-analysis was the presence of both APD and non-APD groups on whom ABR waves I, III, and V were collected in response to clicks. In order to extract these studies, a list of inclusion and exclusion criteria were employed during our search using Google Scholar and PubMed databases (accessed between March 2021 and July 2023), resulting in the inclusion of 8 studies. From these studies, we retrieved ABR waves I, III, and V peak amplitude and latency measures.ResultsOverall, we found no significant differences between those with and without APD on the ABR waves peak latency (wave I: effect size = −0.0365, C.I. = 0.0384; wave III: effect size = −0.0540, C.I. = 0.1417; wave V: effect size = −0.0577, C.I. = 0.1589) and peak amplitude measures (wave I: effect size = 0.0327, C.I. = 0.0473; wave III: effect size = 0.1415, C.I. = 0.1648; wave V: effect size = 0.1281, C.I. = 0.1346).ConclusionThese findings suggest that the click-evoked ABR does not seem to be implicated in those with APD.

Published

2024

8. Molecular mechanisms for activity-dependent control of neuronal excitability in the central auditory pathway

Author

Bondarenko, Kseniia

Subjects

molecular mechanisms, central auditory pathway, Kv3, neurons, Potassium channels, auditory system, Kv3.1, Kv3.3, auditory brainstem, MNTB neurons, Medial Nuclei of Trapezoid Body, neuronal activity, neuroscience, hearing system, superior olivary complex, cognition, nerve cells, neuronal firing, Auditory neuroscience, Thesis

Abstract

Voltage-gated potassium channels of the Kv3 subfamily mediate fast repolarisation of action potentials, allowing neurons to fire at high frequencies. High-frequency firing is especially important in the auditory system, where fast and precise information transmission is crucial for the flawless perception of sound. Previous experiments from the laboratory have shown that only two (Kv3.1 and Kv3.3) out of four Kv3 subunits are expressed in the Medial Nuclei of Trapezoid Body (MNTB) in the auditory brainstem. Tetraethylammonium (TEA) is known to block all Kv3 channels, but a key unknown is whether Kv3.1 or Kv3.3 subunits confer any unique properties on the Kv3 channels formed from these subunits. Since there are no subunit-specific antagonists, my project aimed to combine transgenic manipulation with light-activated pharmacology to investigate the roles of these subunits. This technology involved tethering a light-activated TEA moiety to the pore vestibule of Kv3.3 or Kv3.1; where the respective subunit had been mutated to possess a highly reactive cysteine substitution at the appropriate site. The hypothesis was that by blocking one specific subunit in a Kv3 channel, we could selectively suppress those Kv3 channels mediated by either Kv3.1 or Kv3.3 subunits, which should reveal any subunit-specific physiological functions. This project investigated the action of light-activated pharmacology based on the photochromic tethered ligand MAQ. Electrophysiology was performed ex vivo on brainstem slices from CRISPR/Cas9-edited mice with the single amino acid substitution (for MAQ anchoring) in either Kv3.1 (E380C in mouse kcnc1) or Kv3.3 (N483C in mouse kcnc3) subunit. MAQ, tethered to either Kv3.1E380C or Kv3.3N483C, introduced a reversible light activated block of the Kv3 channel pore, studied in the principal MNTB neurons of transgenic lines. However, the portion of light-controlled potassium current was too small to answer scientific questions (8.6% of total potassium current at +40 mV). Therefore much of the experimental work revolved around testing the materials and assumptions of the original hypothesis. Several conditions were tested to determine the reason for the partial light-induced block by MAQ. The quality of the MAQ was verified using the NMR analysis of the synthesized compound. Homology modelling of the Kv3.3N483C channel with docked MAQ ligand confirmed its binding ability when tethered to the channel pore. The tests with the non-specific photochromic ligand AAQ had shown that azobenzene moiety, a key part of both AAQ and MAQ, successfully undergoes a conformational change when switched between 380 nm and 500 nm using the current optical setup and thus, the set light intensity is enough to convert trans-MAQ molecule to its cis form. I also confirmed that the experimental conditions provide maximum achievable block and that the quality of the brain slice preparation did not undermine the effect achieved using the photo-activated pharmacology. However, the immunofluorescent studies showed that large portions of edited Kv3.1 were retained in the cytosol in the Kv3.1E380C mouse, while edited Kv3.3 and non-edited Kv3.1 in Kv3.3N483C mouse were almost absent, suggesting that Kv3.3 subunits are essential to achieve trafficking of Kv3 channels to the presynaptic terminal. Together, these alterations in Kv3 channel expression in CRISPR/Cas9-edited strains caused reduced photo-controlled portions of Kv3.1-specific and Kv3.3-specific potassium currents. In addition, MAQ showed strong neuronal toxicity that was not reported before. Further immunofluorescent work revealed for the first time that the Kv3.3 subunit is present in the axon initial segments and the nodes of Ranvier. I also deployed the expansion microscopy technique to bypass the resolution limit of confocal microscopes combined with the superresolution post-acquisition algorithms to establish the role of the Kv3.1 and Kv3.3 subunit through their location in the subcellular structures of MNTB neurons. I found that Kv3.1 is mostly present in somatic Kv3 channels (post-synaptic MNTB cell membrane), while Kv3.3 is present in both somatic and presynaptic Kv3s. My findings support the hypothesis that Kv3.3 has a presynaptic function in regulating action potential duration at the synapse in addition to its postsynaptic role in regulating somatic action potentials. It also supported the electrophysiological evidence obtained previously in the lab.

Published

2022

9. Anatomy of superior olivary complex and lateral lemniscus in Etruscan shrew

Author

Zacher, Alina C. and Felmy, Felix

Published

2024

10. Prognostic Value of Auditory Brainstem Evoked Response in Patients with Idiopathic Sudden Sensorineural hearing loss.

Author

Koura, Rabab Ahmed, Fawaz, Mohamed Sayed, Mahmoud, Marwa Mamdouh, and Basiouny, Iman Mostafa

Subjects

SENSORINEURAL hearing loss, PROGNOSIS, BRAIN stem, AUDIOMETRY, HEARING disorders

Abstract

Background: A hearing loss of at least 30 decibels over three successive frequencies in less than 72 hours is referred to as idiopathic sudden sensorineural hearing loss (ISSNHL). Auditory brainstem response may serve as a potential prognostic indication in patients with ISSNHL, according to several studies. Low serum thyroid hormone levels can contribute to hearing loss since they are strongly tied to the cochlea's proper functioning. Aim: To investigate the prognostic value of ABR and the association between its results and the thyroid hormone serum levels in ISSNHL patients. Methods: Observational prospective study was conducted on thirty patients with ISSNHL that occurred within the last 72 h with 30 dB hearing loss at three sequential frequencies. Pure tone audiometry, word discrimination scores, immittencemetry and auditory brain stem response were performed on the day of admission then again on the third day after admission and one month later. Thyroid hormone serum level were assessed after admission. Result: Hearing recovery was observed in 21 patients (70%). The absolute latencies of waves I, III, and V latencies were statistically significantly delayed in the affected ears compared with the unaffected ears. There was a statistically significant correlation between hearing outcome and wave I latency. Wave V latency was statistically significantly negatively correlated with free T4. Conclusion: Auditory brainstem response is an important prognostic factor in ISSNHL but caution should be considered when adopting ABR testing without assessing thyroid hormone levels. [ABSTRACT FROM AUTHOR]

Published

2023

11. CX3CR1 mutation alters synaptic and astrocytic protein expression, topographic gradients, and response latencies in the auditory brainstem

Author

Milinkeviciute, Giedre, Chokr, Sima M, Castro, Emily M, and Cramer, Karina S

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Neurosciences, Clinical Sciences, Neurological, Animals, Astrocytes, Auditory Pathways, Brain Stem, CX3C Chemokine Receptor 1, Evoked Potentials, Auditory, Brain Stem, Female, Gene Expression, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Mutation, Neuronal Plasticity, Reaction Time, Synapses, ABR, astrocytes, auditory brainstem, fractalkine, inhibition, microglia, MNTB, neurotactin, pruning, tonotopy, Zoology, Medical Physiology, Neurology & Neurosurgery

Abstract

The precise and specialized circuitry in the auditory brainstem develops through adaptations of cellular and molecular signaling. We previously showed that elimination of microglia during development impairs synaptic pruning that leads to maturation of the calyx of Held, a large encapsulating synapse that terminates on neurons of the medial nucleus of the trapezoid body (MNTB). Microglia depletion also led to a decrease in glial fibrillary acidic protein (GFAP), a marker for mature astrocytes. Here, we investigated the role of signaling through the fractalkine receptor (CX3CR1), which is expressed by microglia and mediates communication with neurons. CX3CR1-/- and wild-type mice were studied before and after hearing onset and at 9 weeks of age. Levels of GFAP were significantly increased in the MNTB in mutants at 9 weeks. Pruning was unaffected at the calyx of Held, but we found an increase in expression of glycinergic synaptic marker in mutant mice at P14, suggesting an effect on maturation of inhibitory inputs. We observed disrupted tonotopic gradients of neuron and calyx size in MNTB in mutant mice. Auditory brainstem recording (ABR) revealed that CX3CR1-/- mice had normal thresholds and amplitudes but decreased latencies and interpeak latencies, particularly for the highest frequencies. These results demonstrate that disruption of fractalkine signaling has a significant effect on auditory brainstem development. Our findings highlight the importance of neuron-microglia-astrocyte communication in pruning of inhibitory synapses and establishment of tonotopic gradients early in postnatal development.

Published

2021

12. Distinct Cellular Profiles of Hif1a and Vegf mRNA Localization in Microglia, Astrocytes and Neurons during a Period of Vascular Maturation in the Auditory Brainstem of Neonate Rats.

Author

Chang, Daphne, Brown, Quetanya, Tsui, Grace, He, Ye, Liu, Jia, Shi, Lingyan, and Rodríguez-Contreras, Adrián

Subjects

Hif1a, Vegfa, auditory brainstem, hypoxia, microglia, Neurosciences, Psychology, Cognitive Sciences

Abstract

Defining the relationship between vascular development and the expression of hypoxia-inducible factors (Hifs) and vascular endothelial growth factor (Vegf) in the auditory brainstem is important to understand how tissue hypoxia caused by oxygen shortage contributes to sensory deficits in neonates. In this study, we used histology, molecular labeling, confocal microscopy and 3D image processing methods to test the hypothesis that significant maturation of the vascular bed in the medial nucleus of the trapezoid body (MNTB) occurs during the postnatal period that precedes hearing onset. Isolectin-B4 histochemistry experiments suggested that the MNTB vasculature becomes more elaborate between P5 and P10. When combined with a cell proliferation marker and immunohistochemistry, we found that vascular growth coincides with a switch in the localization of proliferating cells to perivascular locations, and an increase in the density of microglia within the MNTB. Furthermore, microglia were identified as perivascular cells with proliferative activity during the period of vascular maturation. Lastly, combined in situ hybridization and immunohistochemistry experiments showed distinct profiles of Hif1a and Vegf mRNA localization in microglia, astrocytes and MNTB principal neurons. These results suggest that different cells of the neuro-glio-vascular unit are likely targets of hypoxic insult in the auditory brainstem of neonate rats.

Published

2021

13. Auditory Brainstem Deficits from Early Treatment with a CSF1R Inhibitor Largely Recover with Microglial Repopulation.

Author

Milinkeviciute, Giedre, Chokr, Sima M, and Cramer, Karina S

Subjects

GFAP, MNTB, auditory brainstem, calyx of Held, depletion, microglia, Neurosciences

Abstract

Signaling between neurons and glia is necessary for the formation of functional neural circuits. A role for microglia in the maturation of connections in the medial nucleus of the trapezoid body (MNTB) was previously demonstrated by postnatal microglial elimination using a colony stimulating factor 1 receptor (CSF1R). Defective pruning of calyces of Held and significant reduction of the mature astrocyte marker glial fibrillary acidic protein (GFAP) were observed after hearing onset. Here, we investigated the time course required for microglia to populate the mouse MNTB after cessation of CSF1R inhibitor treatment. We then examined whether defects seen after microglial depletion were rectified by microglial repopulation. We found that microglia returned to control levels at four weeks of age (18 d postcessation of treatment). Calyceal innervation of MNTB neurons was comparable to control levels at four weeks and GFAP expression recovered by seven weeks. We further investigated the effects of microglia elimination and repopulation on auditory function using auditory brainstem recordings (ABRs). Temporary microglial depletion significantly elevated auditory thresholds in response to 4. 8, and 12 kHz at four weeks. Treatment significantly affected latencies, interpeak latencies, and amplitudes of all the ABR peaks in response to many of the frequencies tested. These effects largely recovered by seven weeks. These findings highlight the functions of microglia in the formation of auditory neural circuits early in development. Further, the results suggest that microglia retain their developmental functions beyond the period of circuit refinement.

Published

2021

14. Hearing Damage Through Blast

Author

Reichenbach, Tobias, Bull, Anthony M. J., editor, Clasper, Jon, editor, Mahoney, Peter F., editor, McGregor, Alison H, Section Editor, Masouros, Spyros D, Section Editor, and Ramasamy, Arul, Section Editor

Published

2022

15. Graded optogenetic activation of the auditory pathway for hearing restoration.

Author

Mittring, Artur, Moser, Tobias, and Huet, Antoine Tarquin

Abstract

Optogenetic control of neural activity enables innovative approaches to improve functional restoration of diseased sensory and motor systems. For clinical translation to succeed, optogenetic stimulation needs to closely match the coding properties of the targeted neuronal population and employ optimally operating emitters. This requires the customization of channelrhodopsins, emitters and coding strategies. Here, we provide a framework to parametrize optogenetic neural control and apply it to the auditory pathway that requires high temporal fidelity of stimulation. We used a viral gene transfer of ultrafast targeting-optimized Chronos into spiral ganglion neurons (SGNs) of the cochlea of mice. We characterized the light-evoked response by in vivo recordings from individual SGNs and neurons of the anteroventral cochlear nucleus (AVCN) that detect coincident SGN inputs. Our recordings from single SGNs demonstrated that their spike probability can be graded by adjusting the duration of light pulses at constant intensity, which optimally serves efficient laser diode operation. We identified an effective pulse width of 1.6 ms to maximize encoding in SGNs at the maximal light intensity employed here (∼35 mW). Alternatively, SGNs were activated at lower energy thresholds using short light pulses (<1 ms). An upper boundary of optical stimulation rates was identified at 316 Hz, inducing a robust spike rate adaptation that required a few tens of milliseconds to recover. We developed a semi-stochastic stimulation paradigm to rapidly (within minutes) estimate the input/output function from light to SGN firing and approximate the time constant of neuronal integration in the AVCN. By that, our data pave the way to design the sound coding strategies of future optical cochlear implants. • We demonstrate that spike probability of the spiral ganglion neurons (SGN) and anteroventral cochlear nucleus neurons can be gradually "dialed" by adjusting the width of light pulses like what can be achieved with acoustic clicks of different sound pressure levels. Varying duration rather than light intensity is an important objective as laser diodes operate most efficiently with large driver currents and short pulses. • Under our experimental condition (light intensity ∼35 mW), we identified an optimal pulse width of 1.6 ms for maximizing information coding in SGNs. • The lowest energy requirement to activate SGNs was achieved using short light pulses (<1 ms). • We identified a spike failure induced during high rate optical stimulation (>300 Hz) that likely was due to depolarization block and required a few tens of milliseconds to recover. This is another important constraint that future optogenetic coding strategies need to consider. • Our data reveal that the timing of optogenetically evoked SGN spikes varied little across iterations for a given neuron but substantially within an SGN population, reminiscent of what is observed acoustically. This insight indicates that optogenetic cochlear implants will likely overcome the problem of overly synchronized activity in the auditory nerve faced by current state of the art electrical cochlear implants. • We established a new framework to rapidly determine the input/output function from light to firing of the spiral ganglion neurons using a semi-stochastic stimulus. This stimulus allowed us to approximate the time constant of neuronal integration in the neurons of the anteroventral cochlear nucleus, which recode the firing transmitted from the spiral ganglion neurons. [ABSTRACT FROM AUTHOR]

Published

2023

16. Microglia Regulate Pruning of Specialized Synapses in the Auditory Brainstem

Author

Milinkeviciute, Giedre, Henningfield, Caden M, Muniak, Michael A, Chokr, Sima M, Green, Kim N, and Cramer, Karina S

Subjects

Biomedical and Clinical Sciences, Neurosciences, Clinical Sciences, 1.1 Normal biological development and functioning, Neurological, Animals, Brain Stem, Female, Male, Mice, Mice, Inbred C57BL, Microglia, Random Allocation, Synapses, microglia, calyx of Held, MNTB, pruning, auditory brainstem, CSF1R inhibitors, depletion, Biological psychology

Abstract

The assembly of uniquely organized sound localization circuits in the brainstem requires precise developmental mechanisms. Glial cells have been shown to shape synaptic connections in the retinogeniculate system during development, but their contributions to specialized auditory synapses have not been identified. Here we investigated the role of microglia in auditory brainstem circuit assembly, focusing on the formation and pruning of the calyx of Held in the medial nucleus of the trapezoid body (MNTB). Microglia were pharmacologically depleted in mice early in development using subcutaneous injections of an inhibitor of colony stimulating factor 1 receptor, which is essential for microglia survival. Brainstems were examined prior to and just after hearing onset, at postnatal days (P) 8 and P13, respectively. We found that at P13 there were significantly more polyinnervated MNTB neurons when microglia were depleted, consistent with a defect in pruning. Expression of glial fibrillary acidic protein (GFAP), a mature astrocyte marker that normally appears in the MNTB late in development, was significantly decreased in microglia-depleted mice at P13, suggesting a delay in astrocyte maturation. Our results demonstrate that monoinnervation of MNTB neurons by the calyx of Held is significantly disrupted or delayed in the absence of microglia. This finding may reflect a direct role for microglia in synaptic pruning. A secondary role for microglia may be in the maturation of astrocytes in MNTB. These findings highlight the significant function of glia in pruning during calyx of Held development.

Published

2019

17. Eph and ephrin signaling in the development of the central auditory system.

Author

Krasewicz, Jakub and Yu, Wei‐Ming

Subjects

AUDITORY pathways, ACOUSTIC nerve, NEURAL circuitry, EPHRINS, EPHRIN receptors

Abstract

Acoustic communication relies crucially on accurate interpretation of information about the intensity, frequency, timing, and location of diverse sound stimuli in the environment. To meet this demand, neurons along different levels of the auditory system form precisely organized neural circuits. The assembly of these precise circuits requires tight regulation and coordination of multiple developmental processes. Several groups of axon guidance molecules have proven critical in controlling these processes. Among them, the family of Eph receptors and their ephrin ligands emerge as one group of key players. They mediate diverse functions at multiple levels of the auditory pathway, including axon guidance and targeting, topographic map formation, as well as cell migration and tissue pattern formation. Here, we review our current knowledge of how Eph and ephrin molecules regulate different processes in the development and maturation of central auditory circuits. Key Findings: Eph/ephrin signaling regulates the segregation and patterning of eighth cranial nerve central projections and tonotopic map precision of the CN.Eph/ephrin signaling regulates the assembly of the sound localization circuit in the auditory brainstem.Eph/ephrin signaling regulates the formation of tonotopic projections in the inferior colliculus.Eph/ephrin signaling regulates frequency tuning and axon targeting in the medial geniculate body and auditory cortex. [ABSTRACT FROM AUTHOR]

Published

2023

18. The Effects of Middle-ear Stiffness on the Auditory Brainstem Neural Encoding of Phase.

Author

Racca, Jordan M., Delgado, Rafael E., Gifford, René H., Ramachandran, Ramnarayan, and Hood, Linda J.

Subjects

PHASE coding, AUDITORY evoked response, BRAIN stem, NEURAL pathways, DIRECTIONAL hearing

Abstract

The middle-ear system relies on a balance of mass and stiffness characteristics for transmitting sound from the external environment to the cochlea and auditory neural pathway. Phase is one aspect of sound that, when transmitted and encoded by both ears, contributes to binaural cue sensitivity and spatial hearing. The study aims were (i) to investigate the effects of middle-ear stiffness on the auditory brainstem neural encoding of phase in human adults with normal pure-tone thresholds and (ii) to investigate the relationships between middle-ear stiffness-induced changes in wideband acoustic immittance and neural encoding of phase. The auditory brainstem neural encoding of phase was measured using the auditory steady-state response (ASSR) with and without middle-ear stiffness elicited via contralateral activation of the middle-ear muscle reflex (MEMR). Middle-ear stiffness was quantified using a wideband acoustic immittance assay of acoustic absorbance. Statistical analyses demonstrated decreased ASSR phase lag and decreased acoustic absorbance with contralateral activation of the MEMR, consistent with increased middle-ear stiffness changing the auditory brainstem neural encoding of phase. There were no statistically significant correlations between stiffness-induced changes in wideband acoustic absorbance and ASSR phase. The findings of this study may have important implications for understanding binaural cue sensitivity and horizontal plane sound localization in audiologic and otologic clinical populations that demonstrate changes in middle-ear stiffness, including cochlear implant recipients who use combined electric and binaural acoustic hearing and otosclerosis patients. [ABSTRACT FROM AUTHOR]

Published

2022

19. Computational Models of Binaural Processing

Author

Dietz, Mathias, Ashida, Go, Fay, Richard R., Series Editor, Popper, Arthur N., Series Editor, Avraham, Karen, Editorial Board Member, Bass, Andrew, Editorial Board Member, Cunningham, Lisa, Editorial Board Member, Fritzsch, Bernd, Editorial Board Member, Groves, Andrew, Editorial Board Member, Hertzano, Ronna, Editorial Board Member, Le Prell, Colleen, Editorial Board Member, Litovsky, Ruth, Editorial Board Member, Manis, Paul, Editorial Board Member, Manley, Geoffrey, Editorial Board Member, Moore, Brian, Editorial Board Member, Simmons, Andrea, Editorial Board Member, Yost, William, Editorial Board Member, Litovsky, Ruth Y., editor, and Goupell, Matthew J., editor

Published

2021

20. MicroRNAs in the auditory system: tiny molecules with big impact.

Author

Ebbers, Lena, Altaf, Faiza, and Nothwang, Hans Gerd

Subjects

*AUDITORY pathways, *MICRORNA, *NON-coding RNA, *INNER ear, *NEURAL transmission

Abstract

"Blindness separates from things; deafness separates from people." This quote attributed to the deaf-blind author and activist Helen Keller (1880–1968) indicates the importance of proper hearing for social interaction in our society which is largely driven by acoustic communication. A major cause for auditory dysfunction lies in our genome with currently more than 100 genes linked to hearing loss. One example is the microRNA gene Mir-96 of the microRNA-183 family. MicroRNAs are small regulatory RNAs involved in the finetuning of gene expression. Analyses of transgenic mouse models established this microRNA family as a major regulator for the function of the inner ear as well as synaptic transmission in the auditory brainstem. The microRNA-183 family might therefore play an important role in coordinating the development of the peripheral and central auditory system and their specializations. [ABSTRACT FROM AUTHOR]

Published

2022

21. Structural arrangement of auditory brainstem nuclei in the bats Phyllostomus discolor and Carollia perspicillata.

Author

Pätz, Christina, Console‐Meyer, Laura, and Felmy, Felix

Abstract

The structure of the mammalian auditory brainstem is evolutionarily highly plastic, and distinct nuclei arrange in a species‐dependent manner. Such anatomical variability is present in the superior olivary complex (SOC) and the nuclei of the lateral lemniscus (LL). Due to the structure–function relationship in the auditory brainstem, the identification of individual nuclei supports the understanding of sound processing. Here, we comparatively describe the nucleus arrangement and the expression of functional markers in the auditory brainstem of the two bat species Phyllostomus discolor and Carollia perspicillata. Using immunofluorescent labeling, we describe the arrangement and identity of the SOC and LL nuclei based on the expression of synaptic markers (vesicular glutamate transporter 1 and glycine transporter 2), calcium‐binding proteins, as well as the voltage‐gated ion channel subunits Kv1.1 and HCN1. The distribution of excitatory and inhibitory synaptic labeling appears similar between both species and matches with that of other mammals. The detection of calcium‐binding proteins indicates species‐dependent differences and deviations from other mammals. Kv1.1 and HCN1 show largely the same expression pattern in both species, which diverges from other mammals, indicating functional adaptations in the cellular physiology of bat neurons. [ABSTRACT FROM AUTHOR]

Published

2022

22. Presynaptic Rac1 controls synaptic strength through the regulation of synaptic vesicle priming

Author

Christian Keine, Mohammed Al-Yaari, Tamara Radulovic, Connon I Thomas, Paula Valino Ramos, Debbie Guerrero-Given, Mrinalini Ranjan, Holger Taschenberger, Naomi Kamasawa, and Samuel M Young Jr

Subjects

rac1, actin cytoskeleton, auditory brainstem, synaptic plasticity, synaptic transmission, synaptic vesicle replenishment, Medicine, Science, Biology (General), QH301-705.5

Abstract

Synapses contain a limited number of synaptic vesicles (SVs) that are released in response to action potentials (APs). Therefore, sustaining synaptic transmission over a wide range of AP firing rates and timescales depends on SV release and replenishment. Although actin dynamics impact synaptic transmission, how presynaptic regulators of actin signaling cascades control SV release and replenishment remains unresolved. Rac1, a Rho GTPase, regulates actin signaling cascades that control synaptogenesis, neuronal development, and postsynaptic function. However, the presynaptic role of Rac1 in regulating synaptic transmission is unclear. To unravel Rac1’s roles in controlling transmitter release, we performed selective presynaptic ablation of Rac1 at the mature mouse calyx of Held synapse. Loss of Rac1 increased synaptic strength, accelerated EPSC recovery after conditioning stimulus trains, and augmented spontaneous SV release with no change in presynaptic morphology or AZ ultrastructure. Analyses with constrained short-term plasticity models revealed faster SV priming kinetics and, depending on model assumptions, elevated SV release probability or higher abundance of tightly docked fusion-competent SVs in Rac1-deficient synapses. We conclude that presynaptic Rac1 is a key regulator of synaptic transmission and plasticity mainly by regulating the dynamics of SV priming and potentially SV release probability.

Published

2022

23. The neural response at the fundamental frequency of speech is modulated by word-level acoustic and linguistic information.

Author

Kegler, Mikolaj, Weissbart, Hugo, and Reichenbach, Tobias

Subjects

SPEECH, WORD frequency, NEUROLINGUISTICS, VOWELS, AUDITORY pathways, ORAL communication, CEREBRAL cortex

Abstract

Spoken language comprehension requires rapid and continuous integration of information, from lower-level acoustic to higher-level linguistic features. Much of this processing occurs in the cerebral cortex. Its neural activity exhibits, for instance, correlates of predictive processing, emerging at delays of a few hundred milliseconds. However, the auditory pathways are also characterized by extensive feedback loops from higher-level cortical areas to lower-level ones as well as to subcortical structures. Early neural activity can therefore be influenced by higher-level cognitive processes, but it remains unclear whether such feedback contributes to linguistic processing. Here, we investigated early speech-evoked neural activity that emerges at the fundamental frequency. We analyzed EEG recordings obtained when subjects listened to a story read by a single speaker. We identified a response tracking the speaker's fundamental frequency that occurred at a delay of 11 ms, while another response elicited by the high-frequency modulation of the envelope of higher harmonics exhibited a larger magnitude and longer latency of about 18 ms. Subsequently, we determined the magnitude of these early neural responses for each individual word in the story. We then quantified the context-independent frequency of each word and used a language model to compute context-dependent word surprisal and precision. The word surprisal represented how predictable a word is, given the previous context, and the word precision reflected the confidence about predicting the next word from the past context. We found that the word-level neural responses at the fundamental frequency were predominantly influenced by the acoustic features: the average fundamental frequency and its variability. Amongst the linguistic features, only context-independent word frequency showed a weak but significant modulation of the neural response to the high-frequency envelope modulation. Our results show that the early neural response at the fundamental frequency is already influenced by acoustic as well as linguistic information, suggesting top-down modulation of this neural response. [ABSTRACT FROM AUTHOR]

Published

2022

24. The neural response at the fundamental frequency of speech is modulated by word-level acoustic and linguistic information

Author

Mikolaj Kegler, Hugo Weissbart, and Tobias Reichenbach

Subjects

spoken language processing, fundamental frequency, auditory brainstem, language, EEG, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Spoken language comprehension requires rapid and continuous integration of information, from lower-level acoustic to higher-level linguistic features. Much of this processing occurs in the cerebral cortex. Its neural activity exhibits, for instance, correlates of predictive processing, emerging at delays of a few 100 ms. However, the auditory pathways are also characterized by extensive feedback loops from higher-level cortical areas to lower-level ones as well as to subcortical structures. Early neural activity can therefore be influenced by higher-level cognitive processes, but it remains unclear whether such feedback contributes to linguistic processing. Here, we investigated early speech-evoked neural activity that emerges at the fundamental frequency. We analyzed EEG recordings obtained when subjects listened to a story read by a single speaker. We identified a response tracking the speaker's fundamental frequency that occurred at a delay of 11 ms, while another response elicited by the high-frequency modulation of the envelope of higher harmonics exhibited a larger magnitude and longer latency of about 18 ms with an additional significant component at around 40 ms. Notably, while the earlier components of the response likely originate from the subcortical structures, the latter presumably involves contributions from cortical regions. Subsequently, we determined the magnitude of these early neural responses for each individual word in the story. We then quantified the context-independent frequency of each word and used a language model to compute context-dependent word surprisal and precision. The word surprisal represented how predictable a word is, given the previous context, and the word precision reflected the confidence about predicting the next word from the past context. We found that the word-level neural responses at the fundamental frequency were predominantly influenced by the acoustic features: the average fundamental frequency and its variability. Amongst the linguistic features, only context-independent word frequency showed a weak but significant modulation of the neural response to the high-frequency envelope modulation. Our results show that the early neural response at the fundamental frequency is already influenced by acoustic as well as linguistic information, suggesting top-down modulation of this neural response.

Published

2022

25. Predicting the Influence of Axon Myelination on Sound Localization Precision Using a Spiking Neural Network Model of Auditory Brainstem.

Author

Li, Ben-Zheng, Pun, Sio Hang, Vai, Mang I., Lei, Tim C., and Klug, Achim

Subjects

DIRECTIONAL hearing, ACOUSTIC localization, ARTIFICIAL neural networks, MYELINATION, NEURAL circuitry

Abstract

Spatial hearing allows animals to rapidly detect and localize auditory events in the surrounding environment. The auditory brainstem plays a central role in processing and extracting binaural spatial cues through microsecond-precise binaural integration, especially for detecting interaural time differences (ITDs) of low-frequency sounds at the medial superior olive (MSO). A series of mechanisms exist in the underlying neural circuits for preserving accurate action potential timing across multiple fibers, synapses and nuclei along this pathway. One of these is the myelination of afferent fibers that ensures reliable and temporally precise action potential propagation in the axon. There are several reports of fine-tuned myelination patterns in the MSO circuit, but how specifically myelination influences the precision of sound localization remains incompletely understood. Here we present a spiking neural network (SNN) model of the Mongolian gerbil auditory brainstem with myelinated axons to investigate whether different axon myelination thicknesses alter the sound localization process. Our model demonstrates that axon myelin thickness along the contralateral pathways can substantially modulate ITD detection. Furthermore, optimal ITD sensitivity is reached when the MSO receives contralateral inhibition via thicker myelinated axons compared to contralateral excitation, a result that is consistent with previously reported experimental observations. Our results suggest specific roles of axon myelination for extracting temporal dynamics in ITD decoding, especially in the pathway of the contralateral inhibition. [ABSTRACT FROM AUTHOR]

Published

2022

26. Non-Apoptotic Caspase Activity Preferentially Targets a Novel Consensus Sequence Associated With Cytoskeletal Proteins in the Developing Auditory Brainstem

Author

Forrest Weghorst, Yeva Mirzakhanyan, Kiersten L. Hernandez, Paul D. Gershon, and Karina S. Cramer

Subjects

auditory brainstem, neural development, caspase, non-apoptotic, proteomics, cytoskeleton, Biology (General), QH301-705.5

Abstract

The auditory brainstem relies on precise circuitry to facilitate sound source localization. In the chick, the development of this specialized circuitry requires non-apoptotic activity of caspase-3, for which we previously identified several hundred proteolytic substrates. Here we tested whether the sequence of the caspase cleavage site differentially encodes proteolytic preference in apoptotic and non-apoptotic contexts. We constructed a consensus sequence for caspase activity in the non-apoptotic chick auditory brainstem comprising the four residues N-terminal to the cleavage site: IX(G/R)D↓ where X represents no significant enrichment and ↓ represents the cleavage site. We identified GO terms significantly enriched among caspase substrates containing motifs found in the above consensus sequence. (G/R)D↓ was associated with the term “Structural Constituent of Cytoskeleton” (SCoC), suggesting that SCoC proteins may be specifically targeted by caspase activity during non-apoptotic developmental processes. To ascertain whether this consensus sequence was specific to the non-apoptotic auditory brainstem at embryonic day (E) 10, we used protein mass spectrometry of brainstems harvested at a time when auditory brainstem neurons undergo apoptotic cell death (E13). The apoptotic motif VD was significantly enriched among E13 cleavage sites, indicating that motif preference at the P2 subsite had shifted toward the canonical caspase consensus sequence. Additionally, Monte Carlo simulations revealed that only the GD motif was associated with SCoC substrates in the apoptotic auditory brainstem, indicating that GD encodes specificity for SCoC proteins in both non-apoptotic and apoptotic contexts, despite not being preferred in the latter. Finally, to identify candidate human non-apoptotic consensus sequences, we used Monte Carlo analyses to determine motifs and motif pairs associated with SCoC caspase substrates in the Degrabase, a database of cleavage sites in human apoptotic cell lines. We found 11 motifs significantly associated with SCoC proteolysis, including IXXD and GD. We employed a stepwise method to select motif pairs that optimized SCoC specificity for a given coverage of SCoC cleavage events, yielding 11 motif pairs likely to be preferred in SCoC-directed human non-apoptotic caspase consensus sequences. GD + IXXD was among these motif pairs, suggesting a conservation of non-apoptotic consensus sites among vertebrates.

Published

2022

27. Predicting the Influence of Axon Myelination on Sound Localization Precision Using a Spiking Neural Network Model of Auditory Brainstem

Author

Ben-Zheng Li, Sio Hang Pun, Mang I. Vai, Tim C. Lei, and Achim Klug

Subjects

sound localization, auditory brainstem, medial superior olive, myelin alteration, interaural time difference, spiking neural network, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Spatial hearing allows animals to rapidly detect and localize auditory events in the surrounding environment. The auditory brainstem plays a central role in processing and extracting binaural spatial cues through microsecond-precise binaural integration, especially for detecting interaural time differences (ITDs) of low-frequency sounds at the medial superior olive (MSO). A series of mechanisms exist in the underlying neural circuits for preserving accurate action potential timing across multiple fibers, synapses and nuclei along this pathway. One of these is the myelination of afferent fibers that ensures reliable and temporally precise action potential propagation in the axon. There are several reports of fine-tuned myelination patterns in the MSO circuit, but how specifically myelination influences the precision of sound localization remains incompletely understood. Here we present a spiking neural network (SNN) model of the Mongolian gerbil auditory brainstem with myelinated axons to investigate whether different axon myelination thicknesses alter the sound localization process. Our model demonstrates that axon myelin thickness along the contralateral pathways can substantially modulate ITD detection. Furthermore, optimal ITD sensitivity is reached when the MSO receives contralateral inhibition via thicker myelinated axons compared to contralateral excitation, a result that is consistent with previously reported experimental observations. Our results suggest specific roles of axon myelination for extracting temporal dynamics in ITD decoding, especially in the pathway of the contralateral inhibition.

Published

2022

28. Brain-Derived Neurotrophic Factor Is Involved in Activity-Dependent Tonotopic Refinement of MNTB Neurons.

Author

Wollet, Mackenna and Kim, Jun Hee

Subjects

BRAIN-derived neurotrophic factor, AUDITORY neurons, NEURONS, NEURONAL differentiation, NEURON development, BRAIN stem

Abstract

In the mammalian brain, auditory brainstem nuclei are arranged topographically according to acoustic frequency responsiveness. During postnatal development, the axon initial segment (AIS) of principal neurons undergoes structural refinement depending on location along the tonotopic axis within the medial nucleus of the trapezoid body (MNTB). However, the molecular mechanisms underlying the structural refinement of the AIS along the tonotopic axis in the auditory brainstem have not been explored. We tested the hypothesis that brain-derived neurotrophic factor (BDNF) is a molecular mediator of the structural development of the MNTB in an activity-dependent manner. Using BDNF heterozygous mutant (BDNF+/–) mice, we examined the impact of global BDNF reduction on structural and functional development of MNTB neurons by assessing AIS structure and associated intrinsic neuronal properties. BDNF reduction inhibits the structural and functional differentiation of principal neurons along the tonotopic axis in the MNTB. Augmented sound input during the critical period of development has been shown to enhance the structural refinement of the AIS of MNTB neurons. However, in BDNF +/– mice, MNTB neurons did not show this activity-dependent structural modification of the AIS following repeated sound stimulation. In addition, BDNF+/– mice lacked a defined isofrequency band of neuronal activity following exposure to 16 kHz sound, suggesting degradation of tonotopy. Taken together, structural development and functional refinement of auditory brainstem neurons require physiological levels of BDNF to establish proper tonotopic gradients. [ABSTRACT FROM AUTHOR]

Published

2022

29. Theoretical Relationship Between Two Measures of Spike Synchrony: Correlation Index and Vector Strength.

Author

Kessler, Dominik, Carr, Catherine E., Kretzberg, Jutta, and Ashida, Go

Subjects

INFORMATION storage & retrieval systems, AUDITORY pathways, ACOUSTIC nerve, SYNCHRONIC order, ACTION potentials

Abstract

Information processing in the nervous system critically relies on temporally precise spiking activity. In the auditory system, various degrees of phase-locking can be observed from the auditory nerve to cortical neurons. The classical metric for quantifying phase-locking is the vector strength (VS), which captures the periodicity in neuronal spiking. More recently, another metric, called the correlation index (CI), was proposed to quantify the temporally reproducible response characteristics of a neuron. The CI is defined as the peak value of a normalized shuffled autocorrelogram (SAC). Both VS and CI have been used to investigate how temporal information is processed and propagated along the auditory pathways. While previous analyses of physiological data in cats suggested covariation of these two metrics, general characterization of their connection has never been performed. In the present study, we derive a rigorous relationship between VS and CI. To model phase-locking, we assume Poissonian spike trains with a temporally changing intensity function following a von Mises distribution. We demonstrate that VS and CI are mutually related via the so-called concentration parameter that determines the degree of phase-locking. We confirm that these theoretical results are largely consistent with physiological data recorded in the auditory brainstem of various animals. In addition, we generate artificial phase-locked spike sequences, for which recording and analysis parameters can be systematically manipulated. Our analysis results suggest that mismatches between empirical data and the theoretical prediction can often be explained with deviations from the von Mises distribution, including skewed or multimodal period histograms. Furthermore, temporal relations of spike trains across trials can contribute to higher CI values than predicted mathematically based on the VS. We find that, for most applications, a SAC bin width of 50 ms seems to be a favorable choice, leading to an estimated error below 2.5% for physiologically plausible conditions. Overall, our results provide general relations between the two measures of phase-locking and will aid future analyses of different physiological datasets that are characterized with these metrics. [ABSTRACT FROM AUTHOR]

Published

2021

30. Brain-Derived Neurotrophic Factor Is Involved in Activity-Dependent Tonotopic Refinement of MNTB Neurons

Author

Mackenna Wollet and Jun Hee Kim

Subjects

BDNF, auditory brainstem, MNTB, tonotopy, axon initial segment, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

In the mammalian brain, auditory brainstem nuclei are arranged topographically according to acoustic frequency responsiveness. During postnatal development, the axon initial segment (AIS) of principal neurons undergoes structural refinement depending on location along the tonotopic axis within the medial nucleus of the trapezoid body (MNTB). However, the molecular mechanisms underlying the structural refinement of the AIS along the tonotopic axis in the auditory brainstem have not been explored. We tested the hypothesis that brain-derived neurotrophic factor (BDNF) is a molecular mediator of the structural development of the MNTB in an activity-dependent manner. Using BDNF heterozygous mutant (BDNF+/–) mice, we examined the impact of global BDNF reduction on structural and functional development of MNTB neurons by assessing AIS structure and associated intrinsic neuronal properties. BDNF reduction inhibits the structural and functional differentiation of principal neurons along the tonotopic axis in the MNTB. Augmented sound input during the critical period of development has been shown to enhance the structural refinement of the AIS of MNTB neurons. However, in BDNF +/– mice, MNTB neurons did not show this activity-dependent structural modification of the AIS following repeated sound stimulation. In addition, BDNF+/– mice lacked a defined isofrequency band of neuronal activity following exposure to 16 kHz sound, suggesting degradation of tonotopy. Taken together, structural development and functional refinement of auditory brainstem neurons require physiological levels of BDNF to establish proper tonotopic gradients.

Published

2022

31. Theoretical Relationship Between Two Measures of Spike Synchrony: Correlation Index and Vector Strength

Author

Dominik Kessler, Catherine E. Carr, Jutta Kretzberg, and Go Ashida

Subjects

phase-locking, circular statistics, temporal coding, auditory brainstem, autocorrelogram, spike train analysis, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Information processing in the nervous system critically relies on temporally precise spiking activity. In the auditory system, various degrees of phase-locking can be observed from the auditory nerve to cortical neurons. The classical metric for quantifying phase-locking is the vector strength (VS), which captures the periodicity in neuronal spiking. More recently, another metric, called the correlation index (CI), was proposed to quantify the temporally reproducible response characteristics of a neuron. The CI is defined as the peak value of a normalized shuffled autocorrelogram (SAC). Both VS and CI have been used to investigate how temporal information is processed and propagated along the auditory pathways. While previous analyses of physiological data in cats suggested covariation of these two metrics, general characterization of their connection has never been performed. In the present study, we derive a rigorous relationship between VS and CI. To model phase-locking, we assume Poissonian spike trains with a temporally changing intensity function following a von Mises distribution. We demonstrate that VS and CI are mutually related via the so-called concentration parameter that determines the degree of phase-locking. We confirm that these theoretical results are largely consistent with physiological data recorded in the auditory brainstem of various animals. In addition, we generate artificial phase-locked spike sequences, for which recording and analysis parameters can be systematically manipulated. Our analysis results suggest that mismatches between empirical data and the theoretical prediction can often be explained with deviations from the von Mises distribution, including skewed or multimodal period histograms. Furthermore, temporal relations of spike trains across trials can contribute to higher CI values than predicted mathematically based on the VS. We find that, for most applications, a SAC bin width of 50 ms seems to be a favorable choice, leading to an estimated error below 2.5% for physiologically plausible conditions. Overall, our results provide general relations between the two measures of phase-locking and will aid future analyses of different physiological datasets that are characterized with these metrics.

Published

2021

32. Sex-specific loss of mitochondrial membrane integrity in the auditory brainstem of a mouse model of Fragile X syndrome.

Author

Caron C, McCullagh EA, and Bertolin G

Abstract

Sound sensitivity is one of the most common sensory complaints for people with autism spectrum disorders (ASDs). How and why sounds are perceived as overwhelming by affected people is unknown. To process sound information properly, the brain requires high activity and fast processing, as seen in areas like the medial nucleus of the trapezoid body (MNTB) of the auditory brainstem. Recent work has shown dysfunction in mitochondria, which are the primary source of energy in cells, in a genetic model of ASD, Fragile X syndrome (FXS). Whether mitochondrial functions are also altered in sound-processing neurons, has not been characterized yet. To address this question, we imaged the MNTB in a mouse model of FXS. We stained MNTB brain slices from wild-type and FXS mice with two mitochondrial markers, TOMM20 and PMPCB, located on the Outer Mitochondrial Membrane and in the matrix, respectively. These markers allow exploration of mitochondrial subcompartments. Our integrated imaging pipeline reveals significant sex-specific differences between genotypes. Colocalization analyses between TOMM20 and PMPCB reveal that the integrity of mitochondrial subcompartments is most disrupted in female FXS mice compared to female wildtype mice. We highlight a quantitative fluorescence microscopy pipeline to monitor mitochondrial functions in the MNTB from control or FXS mice and provide four complementary readouts. Our approach paves the way to understanding how cellular mechanisms important to sound encoding are altered in ASDs., Competing Interests: Declaration of Interests The authors declare no conflicts of interest

Published

2024

33. Mechanisms of non-apoptotic roles for apoptotic proteins in development of the chick auditory brainstem

Author

Weghorst, Forrest

Subjects

Molecular biology, Developmental biology, Neurosciences, Auditory brainstem, Caspase, Cytoskeleton, Development, Extracellular vesicles, RNA-binding proteins

Abstract

The auditory brainstem is specialized to localize sounds with extreme temporal precision, which requires highly accurate development of the circuit that facilitates this function. In the embryonic chicken, this circuit is comprised of the axonal projection from the cochlear nucleus (nucleus magnocellularis; NM) to the monolayer coincidence detector nucleus laminaris (NL). Our lab has previously shown that formation of this circuit requires non-apoptotic activity of the apoptotic protease caspase-3. Pharmacological inhibition of caspase-3 activity in NM axons results in dual aberrant phenotypes: NM axons that overshoot NL, and NL cells that do not form a monolayer. How does caspase activity mediate auditory brainstem development? We characterized the proteome of auditory brainstems that had been treated with caspase-3 inhibitor or vehicle, screening for peptides that bore the biochemical signature of caspase proteolysis and that were present in control brainstems but absent in caspase-inhibited brainstems. The 288 proteins with at least one such peptide (i.e. likely caspase-3 substrates) were disproportionately proteins associated with extracellular vesicles (EVs; membrane-bound nanoparticles that carry cargo and information between cells). We purified EVs from chick auditory brainstems and found that their contents were enriched for caspase substrates. We next sought to determine how caspase activity occurs in the auditory brainstem without inducing apoptosis. One possibility was that caspases cleave proteins at different sites than during apoptosis. We analyzed the cleavage sites of auditory brainstem caspase substrates and found that they were cleaved at a novel cleavage site: IX(G/R)D instead of DEVD. The proteins with (G/R)D cleavage sites were enriched for proteins associated with the cytoskeleton. The human apoptotic proteomic database Degrabase also showed evidence that specific motifs are associated with cytoskeletal proteins, suggesting that non-apoptotic caspase activity may cleave substrates at sites enriched in cytoskeletal proteins to change cell morphology without killing the cell. Finally, based on the preponderance of EV proteins and RNA-binding proteins (RBPs) in caspase substrates, as well as the established enrichment of RBPs in EVs, we hypothesized that caspase activity controls the loading of RBPs (and therefore RNAs) into EVs. We sequenced the RNA of EVs derived from brainstems treated with caspase inhibitor or vehicle solution. We found that a highly abundant, long intergenic non-coding RNA (CREVASSE; Caspase-Regulated, Extracellular-Vesicle-Associated, Single-Stranded Effector) was more abundant in EVs from caspase-inhibited brainstems than EVs from control brainstems. We corrected some inconsistencies between the Ensembl annotation for this lncRNA and the annotation indicated by our sequencing data, and we predicted RNA binding partners for the resulting transcripts. Gene Set Enrichment Analysis of the ranked RNA binding partners showed that CREVASSE binds RNAs involved in development and differentiation, especially in the nervous system, auditory system, and brainstem. Together, these data suggest that auditory brainstem caspase activity regulates axon guidance by targeting cytoskeletal proteins, and it facilitates timely intercellular communication leading to neuronal differentiation (likely of NL cells) once caspase activity subsides.

Published

2022

34. Myelination Deficits in the Auditory Brainstem of a Mouse Model of Fragile X Syndrome.

Author

Lucas, Alexandra, Poleg, Shani, Klug, Achim, and McCullagh, Elizabeth A.

Subjects

FRAGILE X syndrome, INTELLECTUAL disabilities, LABORATORY mice, RAMAN spectroscopy, MYELINATION, BRAIN stem

Abstract

Auditory symptoms are one of the most frequent sensory issues described in people with Fragile X Syndrome (FXS), the most common genetic form of intellectual disability. However, the mechanisms that lead to these symptoms are under explored. In this study, we examined whether there are defects in myelination in the auditory brainstem circuitry. Specifically, we studied myelinated fibers that terminate in the Calyx of Held, which encode temporally precise sound arrival time, and are some of the most heavily myelinated axons in the brain. We measured anatomical myelination characteristics using coherent anti-stokes Raman spectroscopy (CARS) and electron microscopy (EM) in a FXS mouse model in the medial nucleus of the trapezoid body (MNTB) where the Calyx of Held synapses. We measured number of mature oligodendrocytes (OL) and oligodendrocyte precursor cells (OPCs) to determine if changes in myelination were due to changes in the number of myelinating or immature glial cells. The two microscopy techniques (EM and CARS) showed a decrease in fiber diameter in FXS mice. Additionally, EM results indicated reductions in myelin thickness and axon diameter, and an increase in g-ratio, a measure of structural and functional myelination. Lastly, we showed an increase in both OL and OPCs in MNTB sections of FXS mice suggesting that the myelination phenotype is not due to an overall decrease in number of myelinating OLs. This is the first study to show that a myelination defects in the auditory brainstem that may underly auditory phenotypes in FXS. [ABSTRACT FROM AUTHOR]

Published

2021

35. Sparsely Distributed, Pre-synaptic Kv3 K+ Channels Control Spontaneous Firing and Cross-Unit Synchrony via the Regulation of Synaptic Noise in an Auditory Brainstem Circuit.

Author

OIsen, Timothy, Capurro, Alberto, Švent, Maša, Pilati, Nadia, Large, Charles, Hartell, Nick, and Hamann, Martine

Subjects

BRAIN stem, CENTRAL nervous system, SYNCHRONIC order, NOISE, AUDITORY pathways, COCHLEAR nucleus, NEURAL transmission

Abstract

Spontaneous subthreshold activity in the central nervous system is fundamental to information processing and transmission, as it amplifies and optimizes sub-threshold signals, thereby improving action potential initiation and maintaining reliable firing. This form of spontaneous activity, which is frequently considered noise, is particularly important at auditory synapses where acoustic information is encoded by rapid and temporally precise firing rates. In contrast, when present in excess, this form of noise becomes detrimental to acoustic information as it contributes to the generation and maintenance of auditory disorders such as tinnitus. The most prominent contribution to subthreshold noise is spontaneous synaptic transmission (synaptic noise). Although numerous studies have examined the role of synaptic noise on single cell excitability, little is known about its pre-synaptic modulation owing in part to the difficulties of combining noise modulation with monitoring synaptic release. Here we study synaptic noise in the auditory brainstem dorsal cochlear nucleus (DCN) of mice and show that pharmacological potentiation of Kv3 K+ currents reduces the level of synaptic bombardment onto DCN principal fusiform cells. Using a transgenic mouse line (SyG37) expressing SyGCaMP2-mCherry, a calcium sensor that targets pre-synaptic terminals, we show that positive Kv3 K+ current modulation decreases calcium influx in a fifth of pre-synaptic boutons. Furthermore, while maintaining rapid and precise spike timing, positive Kv3 K+ current modulation increases the synchronization of local circuit neurons by reducing spontaneous activity. In conclusion, our study identifies a unique pre-synaptic mechanism which reduces synaptic noise at auditory synapses and contributes to the coherent activation of neurons in a local auditory brainstem circuit. This form of modulation highlights a new therapeutic target, namely the pre-synaptic bouton, for ameliorating the effects of hearing disorders which are dependent on aberrant spontaneous activity within the central auditory system. [ABSTRACT FROM AUTHOR]

Published

2021

36. Myelination Deficits in the Auditory Brainstem of a Mouse Model of Fragile X Syndrome

Author

Alexandra Lucas, Shani Poleg, Achim Klug, and Elizabeth A. McCullagh

Subjects

myelination, auditory brainstem, Fragile X Syndrome, coherent anti-stokes Raman scattering, medial nucleus of the trapezoid body, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Auditory symptoms are one of the most frequent sensory issues described in people with Fragile X Syndrome (FXS), the most common genetic form of intellectual disability. However, the mechanisms that lead to these symptoms are under explored. In this study, we examined whether there are defects in myelination in the auditory brainstem circuitry. Specifically, we studied myelinated fibers that terminate in the Calyx of Held, which encode temporally precise sound arrival time, and are some of the most heavily myelinated axons in the brain. We measured anatomical myelination characteristics using coherent anti-stokes Raman spectroscopy (CARS) and electron microscopy (EM) in a FXS mouse model in the medial nucleus of the trapezoid body (MNTB) where the Calyx of Held synapses. We measured number of mature oligodendrocytes (OL) and oligodendrocyte precursor cells (OPCs) to determine if changes in myelination were due to changes in the number of myelinating or immature glial cells. The two microscopy techniques (EM and CARS) showed a decrease in fiber diameter in FXS mice. Additionally, EM results indicated reductions in myelin thickness and axon diameter, and an increase in g-ratio, a measure of structural and functional myelination. Lastly, we showed an increase in both OL and OPCs in MNTB sections of FXS mice suggesting that the myelination phenotype is not due to an overall decrease in number of myelinating OLs. This is the first study to show that a myelination defects in the auditory brainstem that may underly auditory phenotypes in FXS.

Published

2021

37. Sparsely Distributed, Pre-synaptic Kv3 K+ Channels Control Spontaneous Firing and Cross-Unit Synchrony via the Regulation of Synaptic Noise in an Auditory Brainstem Circuit

Author

Timothy OIsen, Alberto Capurro, Maša Švent, Nadia Pilati, Charles Large, Nick Hartell, and Martine Hamann

Subjects

Kv3 K+ currents, synaptic release, excitability, auditory brainstem, pre-synaptic, synchrony, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Spontaneous subthreshold activity in the central nervous system is fundamental to information processing and transmission, as it amplifies and optimizes sub-threshold signals, thereby improving action potential initiation and maintaining reliable firing. This form of spontaneous activity, which is frequently considered noise, is particularly important at auditory synapses where acoustic information is encoded by rapid and temporally precise firing rates. In contrast, when present in excess, this form of noise becomes detrimental to acoustic information as it contributes to the generation and maintenance of auditory disorders such as tinnitus. The most prominent contribution to subthreshold noise is spontaneous synaptic transmission (synaptic noise). Although numerous studies have examined the role of synaptic noise on single cell excitability, little is known about its pre-synaptic modulation owing in part to the difficulties of combining noise modulation with monitoring synaptic release. Here we study synaptic noise in the auditory brainstem dorsal cochlear nucleus (DCN) of mice and show that pharmacological potentiation of Kv3 K+ currents reduces the level of synaptic bombardment onto DCN principal fusiform cells. Using a transgenic mouse line (SyG37) expressing SyGCaMP2-mCherry, a calcium sensor that targets pre-synaptic terminals, we show that positive Kv3 K+ current modulation decreases calcium influx in a fifth of pre-synaptic boutons. Furthermore, while maintaining rapid and precise spike timing, positive Kv3 K+ current modulation increases the synchronization of local circuit neurons by reducing spontaneous activity. In conclusion, our study identifies a unique pre-synaptic mechanism which reduces synaptic noise at auditory synapses and contributes to the coherent activation of neurons in a local auditory brainstem circuit. This form of modulation highlights a new therapeutic target, namely the pre-synaptic bouton, for ameliorating the effects of hearing disorders which are dependent on aberrant spontaneous activity within the central auditory system.

Published

2021

38. Coincidence Detection and Absolute Threshold in the Auditory Brainstem

Author

Meddis, Ray, Wang, Rubin, Series Editor, Delgado-García, José M., editor, Pan, Xiaochuan, editor, and Sánchez-Campusano, Raudel, editor

Published

2018

39. A phenomenological spiking model for octopus cells in the posterior–ventral cochlear nucleus.

Author

Rebhan, Michael and Leibold, Christian

Subjects

*COCHLEAR nucleus, *COCHLEA physiology, *OCTOPUSES, *SOUND pressure, *AMPLITUDE modulation, *SOUND waves, *CELL populations

Abstract

Octopus cells in the posteroventral cochlear nucleus exhibit characteristic onset responses to broad band transients but are little investigated in response to more complex sound stimuli. In this paper, we propose a phenomenological, but biophysically motivated, modeling approach that allows to simulate responses of large populations of octopus cells to arbitrary sound pressure waves. The model depends on only few parameters and reproduces basic physiological characteristics like onset firing and phase locking to amplitude modulations. Simulated responses to speech stimuli suggest that octopus cells are particularly sensitive to high-frequency transients in natural sounds and their sustained firing to phonemes provides a population code for sound level. [ABSTRACT FROM AUTHOR]

Published

2021

40. Structural Refinement of the Auditory Brainstem Neurons in Baboons During Perinatal Development

Author

Eun Jung Kim, Kaila Nip, Cynthia Blanco, and Jun Hee Kim

Subjects

non-human primate, auditory brainstem, MSO, fetal development, NICU, structural plasticity, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Children born prematurely suffer from learning disabilities and exhibit reading, speech, and cognitive difficulties, which are associated with an auditory processing disorder. However, it is unknown whether gestational age at delivery and the unnatural auditory environment in neonatal intensive care units (NICU) collectively affect proper auditory development and neuronal circuitry in premature newborns. We morphologically characterized fetal development of the medial superior olivary nucleus (MSO), an area important for binaural hearing and sound localization, in the auditory brainstem of baboon neonates at different gestational ages. Axonal and synaptic structures and the tonotopic differentiation of ion channels in the MSO underwent profound refinements after hearing onset in the uterus. These developmental refinements of the MSO were significantly altered in preterm baboon neonates in the NICU. Thus, the maternal environment in uterus is critical for auditory nervous system development during the last trimester of pregnancy and critically affects the anatomic and functional formation of synapses and neural circuitry in the preterm newborn brain.

Published

2021

41. Individual Differences in Temporal Perception and Their Implications for Everyday Listening

Author

Shinn-Cunningham, Barbara, Varghese, Leonard, Wang, Le, Bharadwaj, Hari, Fay, Richard R., Series editor, Popper, Arthur N., Series editor, Kraus, Nina, editor, Anderson, Samira, editor, and White-Schwoch, Travis, editor

Published

2017

42. Shaping Brainstem Representation of Pitch-Relevant Information by Language Experience

Author

Krishnan, Ananthanarayan, Gandour, Jackson T., Fay, Richard R., Series editor, Popper, Arthur N., Series editor, Kraus, Nina, editor, Anderson, Samira, editor, and White-Schwoch, Travis, editor

Published

2017

43. Auditory System Development: A Tribute to Edwin W Rubel

Author

Cramer, Karina S., Coffin, Allison B., Fay, Richard R., Series editor, Popper, Arthur N., Series editor, Cramer, Karina S., editor, and Coffin, Allison B., editor

Published

2017

44. Trigeminal Microvascular Decompression

Author

Koht, Antoun, Koht, Antoun, editor, Sloan, Tod B., editor, and Toleikis, J. Richard, editor

Published

2017

45. Structural Refinement of the Auditory Brainstem Neurons in Baboons During Perinatal Development.

Author

Kim, Eun Jung, Nip, Kaila, Blanco, Cynthia, and Kim, Jun Hee

Subjects

BABOONS, NEURAL circuitry, AUDITORY processing disorder, NERVOUS system, DIRECTIONAL hearing, BRAIN stem, AUDITORY neurons

Abstract

Children born prematurely suffer from learning disabilities and exhibit reading, speech, and cognitive difficulties, which are associated with an auditory processing disorder. However, it is unknown whether gestational age at delivery and the unnatural auditory environment in neonatal intensive care units (NICU) collectively affect proper auditory development and neuronal circuitry in premature newborns. We morphologically characterized fetal development of the medial superior olivary nucleus (MSO), an area important for binaural hearing and sound localization, in the auditory brainstem of baboon neonates at different gestational ages. Axonal and synaptic structures and the tonotopic differentiation of ion channels in the MSO underwent profound refinements after hearing onset in the uterus. These developmental refinements of the MSO were significantly altered in preterm baboon neonates in the NICU. Thus, the maternal environment in uterus is critical for auditory nervous system development during the last trimester of pregnancy and critically affects the anatomic and functional formation of synapses and neural circuitry in the preterm newborn brain. [ABSTRACT FROM AUTHOR]

Published

2021

46. Transient Delivery of a KCNQ2/3-Specific Channel Activator 1 Week After Noise Trauma Mitigates Noise-Induced Tinnitus.

Author

Marinos, Laura, Kouvaros, Stylianos, Bizup, Brandon, Hambach, Bryce, Wipf, Peter, and Tzounopoulos, Thanos

Abstract

Exposure to loud noise can cause hearing loss and tinnitus in mice and humans. In mice, one major underlying mechanism of noise-induced tinnitus is hyperactivity of auditory brainstem neurons, due at least in part, to decreased Kv7.2/3 (KCNQ2/3) potassium channel activity. In our previous studies, we used a reflex-based mouse model of tinnitus and showed that administration of a non-specific KCNQ channel activator, immediately after noise trauma, prevented the development of noise-induced tinnitus, assessed 1 week after trauma. Subsequently, we developed RL-81, a very potent and highly specific activator of KCNQ2/3 channels. Here, to test the timing window within which RL-81 prevents tinnitus in mice, we modified and employed an operant animal model of tinnitus, where mice are trained to move in response to sound but not move in silence. Mice with behavioral evidence of tinnitus are expected to move in silence. We validated this mouse model by testing the effect of salicylate, which is known to induce tinnitus. We found that transient administration of RL-81 1 week after noise exposure did not affect hearing loss but reduced significantly the percentage of mice with behavioral evidence of tinnitus, assessed 2 weeks after noise exposure. Our results indicate that RL-81 is a promising drug candidate for further development for the treatment of noise-induced tinnitus. [ABSTRACT FROM AUTHOR]

Published

2021

47. Small dendritic synapses enhance temporal coding in a model of cochlear nucleus bushy cells.

Author

Koert, Elisabeth and Kuenzel, Thomas

Abstract

Spherical bushy cells (SBCs) in the anteroventral cochlear nucleus receive a single or very few powerful axosomatic inputs from the auditory nerve. However, SBCs are also contacted by small regular bouton synapses of the auditory nerve, located in their dendritic tree. The function of these small inputs is unknown. It was speculated that the interaction of axosomatic inputs with small dendritic inputs improved temporal precision, but direct evidence for this is missing. In a compartment model of spherical bushy cells with a stylized or realistic three-dimensional (3-D) representation of the bushy dendrite, we explored this hypothesis. Phase-locked dendritic inputs caused both tonic depolarization and a modulation of the model SBC membrane potential at the frequency of the stimulus. For plausible model parameters, dendritic inputs were subthreshold. Instead, the tonic depolarization increased the excitability of the SBC model and the modulation of the membrane potential caused a phase-dependent increase in the efficacy of the main axosomatic input. This improved response rate and entrainment for low-input frequencies and temporal precision of output at and above the characteristic frequency. A careful exploration of morphological and biophysical parameters of the bushy dendrite suggested a functional explanation for the peculiar shape of the bushy dendrite. Our model for the first time directly implied a role for the small excitatory dendritic inputs in auditory processing: they modulate the efficacy of the main input and are thus a plausible mechanism for the improvement of temporal precision and fidelity in these central auditory neurons. NEW & NOTEWORTHY We modeled dendritic inputs from the auditory nerve that spherical bushy cells of the cochlear nucleus receive. Dendritic inputs caused both tonic depolarization and modulation of the membrane potential at the input frequency. This improved the rate, entrainment, and temporal precision of output action potentials. Our simulations suggest a role for small dendritic inputs in auditory processing: they modulate the efficacy of the main input supporting temporal precision and fidelity in these central auditory neurons. [ABSTRACT FROM AUTHOR]

Published

2021

48. GABA B receptor-mediated modulation in the developing dorsal nucleus of the lateral lemniscus.

Author

Javadova A and Felmy F

Subjects

Animals, Gerbillinae, Synaptic Transmission physiology, Receptors, GABA-A, Potassium, Receptors, GABA-B, Baclofen pharmacology

Abstract

The dorsal nucleus of the lateral lemniscus (DNLL) is a GABAergic, reciprocally connected auditory brainstem structure that continues to develop postnatally in rodents. One key feature of the DNLL is the generation of a strong, prolonged, ionotropic, GABA A receptor-mediated inhibition. Possible GABA B receptor-mediated signalling is unexplored in the DNLL. Here, we used Mongolian gerbils of either sex to describe GABA B receptor-mediated modulation of postsynaptic potassium currents and synaptic inputs in postnatal (P) animals of days 10/11 and 23-28. Throughout development, we observed the presence of a Baclofen-activated GABA B receptor-enhanced potassium outward conductance that is capable of suppressing action potential generation. In P10/11, old gerbils GABA B receptor activation enhances glutamatergic and suppresses ionotropic GABAergic synaptic transmission. During development, this differential modulation becomes less distinct, because in P22-28, old animals Baclofen-activated GABA B receptors rather enhance ionotropic GABAergic synaptic transmission, whereas glutamatergic transmission is both enhanced and suppressed. Blocking GABA B receptors causes an increase in ionotropic GABAergic transmission in P10/11 old gerbils that was independent on stimulation frequency but depended on the type of short-term plasticity. Together with the lack of Baclofen-induced changes in the synaptic paired-pulse ratio of either input type, we suggest that GABA B receptor-mediated modulation is predominantly postsynaptic and activates different signalling cascades. Thus, we argue that in DNLL neurons, the GABA B receptor is a post-synaptically located signalling hub that alters signalling cascades during development for distinct targets., (© 2024 The Authors. European Journal of Neuroscience published by Federation of European Neuroscience Societies and John Wiley & Sons Ltd.)

Published

2024

49. Minimal Number of Required Inputs for Temporally Precise Action Potential Generation in Auditory Brainstem Nuclei

Author

Nikolaos Kladisios, Linda Fischer, and Felix Felmy

Subjects

auditory brainstem, postnatal development, action potential generation, synaptic transmission, superior olive, lateral lemniscus, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The auditory system relies on temporal precise information transfer, requiring an interplay of synchronously activated inputs and rapid postsynaptic integration. During late postnatal development synaptic, biophysical, and morphological features change to enable mature auditory neurons to perform their appropriate function. How the number of minimal required input fibers and the relevant EPSC time course integrated for action potential generation changes during late postnatal development is unclear. To answer these questions, we used in vitro electrophysiology in auditory brainstem structures from pre-hearing onset and mature Mongolian gerbils of either sex. Synaptic and biophysical parameters changed distinctively during development in the medial nucleus of the trapezoid body (MNTB), the medial superior olive (MSO), and the ventral and dorsal nucleus of the lateral lemniscus (VNLL and DNLL). Despite a reduction in input resistance in most cell types, all required fewer inputs in the mature stage to drive action potentials. Moreover, the EPSC decay time constant is a good predictor of the EPSC time used for action potential generation in all nuclei but the VNLL. Only in MSO neurons, the full EPSC time course is integrated by the neuron’s resistive element, while otherwise, the relevant EPSC time matches only 5–10% of the membrane time constant, indicating membrane charging as a dominant role for output generation. We conclude, that distinct developmental programs lead to a general increase in temporal precision and integration accuracy matched to the information relaying properties of the investigated nuclei.

Published

2020

50. Caspase-3 Cleaves Extracellular Vesicle Proteins During Auditory Brainstem Development

Author

Forrest Weghorst, Yeva Mirzakhanyan, Kian Samimi, Mehron Dhillon, Melanie Barzik, Lisa L. Cunningham, Paul D. Gershon, and Karina S. Cramer

Subjects

auditory brainstem, neural development, caspase-3, non-apoptotic, extracellular vesicles, proteomics, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Sound localization requires extremely precise development of auditory brainstem circuits, the molecular mechanisms of which are largely unknown. We previously demonstrated a novel requirement for non-apoptotic activity of the protease caspase-3 in chick auditory brainstem development. Here, we used mass spectrometry to identify proteolytic substrates of caspase-3 during chick auditory brainstem development. These auditory brainstem caspase-3 substrates were enriched for proteins previously shown to be cleaved by caspase-3, especially in non-apoptotic contexts. Functional annotation analysis revealed that our caspase-3 substrates were also enriched for proteins associated with several protein categories, including proteins found in extracellular vesicles (EVs), membrane-bound nanoparticles that function in intercellular communication. The proteome of EVs isolated from the auditory brainstem was highly enriched for our caspase-3 substrates. Additionally, we identified two caspase-3 substrates with known functions in axon guidance, namely Neural Cell Adhesion Molecule (NCAM) and Neuronal-glial Cell Adhesion Molecule (Ng-CAM), that were found in auditory brainstem EVs and expressed in the auditory pathway alongside cleaved caspase-3. Taken together, these data suggest a novel developmental mechanism whereby caspase-3 influences auditory brainstem circuit formation through the proteolytic cleavage of extracellular vesicle (EV) proteins.

Published

2020