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Presynaptic mitochondria volumes and complexity of subsynaptic distribution increase during development at a high-fidelity synapse

Presynaptic mitochondria volumes and complexity of subsynaptic distribution increase during development at a high-fidelity synapse

来源:bioRxiv_logobioRxiv
英文摘要

Abstract The calyx of Held, a large glutamatergic presynaptic terminal in the auditory brainstem undergoes developmental changes to support the high action-potential firing rates required for auditory information encoding. In addition, calyx terminals are morphologically diverse which impacts vesicle release properties and synaptic plasticity. Mitochondria influence synaptic plasticity through calcium buffering and are crucial for providing the energy required for synaptic transmission. Therefore, it has been postulated that mitochondrial levels increase during development and contribute to the morphological-functional diversity in the mature calyx. However, the developmental profile of mitochondrial volumes and subsynaptic distribution at the calyx of Held remains unclear. To provide insight on this, we developed a helper-dependent adenoviral vector (HdAd) that expresses the genetically encoded peroxidase marker for mitochondria, mito-APEX2, at the mouse calyx of Held. We developed protocols to detect labeled mitochondria for use with serial block face scanning electron microscopy to carry out semi-automated segmentation of mitochondria, high-throughput whole terminal reconstruction and presynaptic ultrastructure in mice of either sex. Subsequently, we measured mitochondrial volumes and subsynaptic distributions at the immature postnatal day 7 (P7) and the mature (P21) calyx. We found an increase of mitochondria volumes in terminals and axons from P7 to P21 but did not observe differences between stalk and swelling subcompartments in the mature calyx. Based on these findings, we propose that mitochondrial volumes developmentally increase to support high firing rates but have limited contribution to morphological-functional diversity at the calyx. Significance StatementElucidating the developmental processes of auditory brainstem presynaptic terminals is critical to understanding auditory information encoding. Additionally, morphological-functional diversity at these terminals is proposed to enhance coding capacity. Mitochondria provide energy for synaptic transmission and can buffer calcium, impacting synaptic plasticity; however, their developmental profile to ultimately support the energetic demands of synapses following the onset of hearing remains unknown. Therefore, we created a helper-dependent adenoviral vector with the mitochondria-targeting peroxidase mito-APEX2 and expressed it at the mouse calyx of Held. Volumetric reconstructions of serial block face electron microscopy data of immature and mature labeled calyces reveal that mitochondrial volumes are increased to support high firing rates upon maturity and likely have little contribution to morphological-functional diversity at the calyx.

Keine Christian、Okayama Satoko、Guerrero-Given Debbie、Kamasawa Naomi、Young Samuel M. Jr.、Musgrove Morgan、Satterfield Rachel、Thomas Connon I.

Department of Anatomy and Cell Biology, Iowa Neuroscience Institute, University of IowaMolecular Mechanisms of Synaptic Function, Max Planck Florida InstituteElectron Microscopy Core Facility, Max Planck Florida InstituteElectron Microscopy Core Facility, Max Planck Florida InstituteDepartment of Anatomy and Cell Biology, Iowa Neuroscience Institute, University of Iowa||Department of Otolaryngology, University of IowaElectron Microscopy Core Facility, Max Planck Florida InstituteMolecular Mechanisms of Synaptic Function, Max Planck Florida InstituteElectron Microscopy Core Facility, Max Planck Florida Institute

10.1101/689653

细胞生物学生理学生物物理学

Keine Christian,Okayama Satoko,Guerrero-Given Debbie,Kamasawa Naomi,Young Samuel M. Jr.,Musgrove Morgan,Satterfield Rachel,Thomas Connon I..Presynaptic mitochondria volumes and complexity of subsynaptic distribution increase during development at a high-fidelity synapse[EB/OL].(2025-03-28)[2025-05-21].https://www.biorxiv.org/content/10.1101/689653.点此复制

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