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Biomedical

(M)Unc13s in Active Zone Diversity: A Drosophila Perspective

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Chengji Piao,

Chengji Piao


Stephan J. Sigrist

Stephan J. Sigrist


  Peer Reviewed

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© attribution CC-BY

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Added on

2024-10-26

Doi: http://dx.doi.org/10.3389/fnsyn.2021.798204

Related Subjects
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Abstract

The so-called active zones at pre-synaptic terminals are the ultimate filtering devices, which couple between action potential frequency and shape, and the information transferred to the post-synaptic neurons, finally tuning behaviors. Within active zones, the release of the synaptic vesicle operates from specialized “release sites.” The (M)Unc13 class of proteins is meant to define release sites topologically and biochemically, and diversity between Unc13-type release factor isoforms is suspected to steer diversity at active zones. The two major Unc13-type isoforms, namely, Unc13A and Unc13B, have recently been described from the molecular to the behavioral level, exploiting Drosophila being uniquely suited to causally link between these levels. The exact nanoscale distribution of voltage-gated Ca2+ channels relative to release sites (“coupling”) at pre-synaptic active zones fundamentally steers the release of the synaptic vesicle. Unc13A and B were found to be either tightly or loosely coupled across Drosophila synapses. In this review, we reported recent findings on diverse aspects of Drosophila Unc13A and B, importantly, their nano-topological distribution at active zones and their roles in release site generation, active zone assembly, and pre-synaptic homeostatic plasticity. We compared their stoichiometric composition at different synapse types, reviewing the correlation between nanoscale distribution of these two isoforms and release physiology and, finally, discuss how isoform-specific release components might drive the functional heterogeneity of synapses and encode discrete behavior.

Key Questions about 'Room for Two: The Synaptophysin/Synaptobrevin Complex'

The article *"Room for Two: The Synaptophysin/Synaptobrevin Complex"* by Dustin N. White and Michael H. B. Stowell, published in *Frontiers in Synaptic Neuroscience* in September 2021, investigates the interaction between synaptophysin (SYP) and synaptobrevin (VAMP2) in the regulation of synaptic vesicle release. Source

1. What is the role of synaptophysin (SYP) in synaptic vesicle release?

Synaptophysin (SYP) is a vesicular transmembrane protein whose functions have been proposed to include acting as a calcium sensor, a cholesterol-binding protein, and forming ion channels across the phospholipid bilayer. However, the downstream effects of these functions are largely unknown. Source

2. How does the SYP/VAMP2 complex contribute to synaptic vesicle release?

The complex formed by SYP and VAMP2 is thought to be involved in both trafficking to the pre-synaptic membrane and regulation of SNARE complex formation. Recent structural observations specifically implicate the SYP/VAMP2 complex in anchoring the SNARE assembly at the pre-synaptic membrane prior to vesicle fusion. Source

3. What are the implications of the SYP/VAMP2 complex in neurological disorders?

Disruptions in the components of the SYP/VAMP2 complex can have devastating consequences for neuronal communication, affecting vesicle trafficking, docking, fusion, and release. At the organismal level, this is reflected in disorders such as epilepsy, depression, and neurodegeneration. Source

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ARTICLE USAGE


Article usage: Oct-2024 to May-2025
Show by month Manuscript Video Summary
2025 May 59 59
2025 April 67 67
2025 March 68 68
2025 February 39 39
2025 January 51 51
2024 December 48 48
2024 November 54 54
2024 October 17 17
Total 403 403
Show by month Manuscript Video Summary
2025 May 59 59
2025 April 67 67
2025 March 68 68
2025 February 39 39
2025 January 51 51
2024 December 48 48
2024 November 54 54
2024 October 17 17
Total 403 403
Related Subjects
Anatomy
Biochemistry
Epidemiology
Genetics
Neuroscience
Psychology
Oncology
Medicine
Musculoskeletal science
Pediatrics
Pathology
Pharmacology
Physiology
Psychiatry
Primary care
Women and reproductive health
copyright icon

© attribution CC-BY

  • 0

rating
403 Views

Added on

2024-10-26

Doi: http://dx.doi.org/10.3389/fnsyn.2021.798204

Related Subjects
Anatomy
Biochemistry
Epidemiology
Genetics
Neuroscience
Psychology
Oncology
Medicine
Musculoskeletal science
Pediatrics
Pathology
Pharmacology
Physiology
Psychiatry
Primary care
Women and reproductive health

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