Gap junctions and chemical synapses

Anne Warner

doi:10.1038/273410a0

Electrical synaptic transmission requires a postsynaptic scaffolding protein

10.1101/2020.12.03.410696 ◽

2020 ◽

Author(s):

Abagael M. Lasseigne ◽

Fabio A. Echeverry ◽

Sundas Ijaz ◽

Jennifer Carlisle Michel ◽

E. Anne Martin ◽

...

Keyword(s):

Synaptic Transmission ◽

Gap Junctions ◽

Functional Organization ◽

Scaffolding Protein ◽

Scaffolding Proteins ◽

Electrical Transmission ◽

Critical Function ◽

Electrical Synapses ◽

Intercellular Channels ◽

Chemical Synapses

SUMMARYElectrical synaptic transmission relies on neuronal gap junctions containing channels constructed by Connexins. While at chemical synapses neurotransmitter-gated ion channels are critically supported by scaffolding proteins, it is unknown if channels at electrical synapses require similar scaffold support. Here we investigated the functional relationship between neuronal Connexins and Zonula Occludens 1 (ZO1), an intracellular scaffolding protein localized to electrical synapses. Using model electrical synapses in zebrafish Mauthner cells, we demonstrated that ZO1 is required for robust synaptic Connexin localization, but Connexins are dispensable for ZO1 localization. Disrupting this hierarchical ZO1/Connexin relationship abolishes electrical transmission and disrupts Mauthner-cell-initiated escape responses. We found that ZO1 is asymmetrically localized exclusively postsynaptically at neuronal contacts where it functions to assemble intercellular channels. Thus, forming functional neuronal gap junctions requires a postsynaptic scaffolding protein. The critical function of a scaffolding molecule reveals an unanticipated complexity of molecular and functional organization at electrical synapses.

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Electron microscopy of Golgi-impregnated photoreceptors reveals connections between red and green cones in the turtle retina

Journal of Neurophysiology ◽

10.1152/jn.1985.54.2.304 ◽

1985 ◽

Vol 54 (2) ◽

pp. 304-317 ◽

Cited By ~ 34

Author(s):

H. Kolb ◽

J. Jones

Keyword(s):

Electron Microscopy ◽

Light Microscopy ◽

Gap Junctions ◽

Plexiform Layer ◽

Thin Sections ◽

Turtle Species ◽

Ribbon Synapses ◽

Central Elements ◽

Spectral Identity ◽

Chemical Synapses

Red and green cones of two turtle species (Pseudemys scripta elegans and Chelydra serpentina) retina have been stained with Golgi procedures and examined by light microscopy of whole-mount tissue and by electron microscopy of serial thin sections. By light microscopy, red and green single cones appear indistinguishable, but double cones can be readily identified. All Golgi-stained photoreceptors in turtle retina have a spray of telodendria radiating from their synaptic pedicles. The telodendria of single cones are 10-20 micron long and end in clusters of terminals, whereas double cones have 30- to 50-micron long telodendria in addition to a very short bush of telodendria arising from one side of the pedicle. Electron microscopy of the Golgi-stained cones allows them to be distinguished into red or green spectral types by the appearance of their oil droplets. Furthermore, the spectral identity of cones contacted by the telodendria of identified Golgi-stained cones can similarly be determined. Red single cones make telodendrial contacts with other red singles, both members of the double cones, and with green single cones. Green single cones likewise connect to many surrounding red cones, both single and double types, and a few other green singles. Both members of the double cone connect to neighboring red and green singles and occasionally to double cones. The telodendria of stained cones end on spectrally homologous or heterologous cone types at basal junctions, central elements of ribbon synapses or, sometimes, as lateral elements of ribbon synapses. However, all these synaptic contacts appear to be of the same type, i.e., narrow-cleft basal junctions. Small gap junctions occur between neighboring cone pedicles, regardless of spectral type, in the visual streak area of the retina. Large gap junctions occur between unidentified cone telodendria in the neuropil of the outer plexiform layer. The telodendrial connections between red and green cones in the turtle retina have the appearance of chemical synapses and suggest an anatomical pathway responsible for the mixing of red and green signals in red or green cones of the turtle retina as reported in the accompanying physiological paper by Normann, Perlman, and Daly (27).

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Ultrastructural analysis of chemical synapses and gap junctions betweenDrosophila brain neurons in culture

Developmental Neurobiology ◽

10.1002/dneu.20575 ◽

2008 ◽

Vol 68 (3) ◽

pp. 281-294 ◽

Cited By ~ 10

Author(s):

Hyun-Woo Oh ◽

Jorge M. Campusano ◽

Lutz G.W. Hilgenberg ◽

Xicui Sun ◽

Martin A. Smith ◽

...

Keyword(s):

Gap Junctions ◽

Ultrastructural Analysis ◽

Brain Neurons ◽

Chemical Synapses

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The neuron doctrine is an insult to neurons

Behavioral and Brain Sciences ◽

10.1017/s0140525x9931219x ◽

1999 ◽

Vol 22 (5) ◽

pp. 838-839 ◽

Cited By ~ 3

Author(s):

Stuart Hameroff

Keyword(s):

Information Processing ◽

Gap Junctions ◽

Quantum Computation ◽

Switching Circuit ◽

Dendritic Processing ◽

Living State ◽

Bath Water ◽

Chemical Synapses ◽

Neuronal Functions

As presently implemented, the neuron doctrine (ND) portrays the brain's neurons and chemical synapses as fundamental components in a computer-like switching circuit, supporting a view of brain = mind = computer. However, close examination reveals individual neurons to be far more complex than simple switches, with enormous capacity for intracellular information processing (e.g., in the internal cytoskeleton). Other poorly appreciated factors (gap junctions, apparent randomness, dendritic-dendritic processing, possible quantum computation, the living state) also suggest that the ND grossly oversimplifies neuronal functions. In the quest to understand consciousness, the presently implemented ND may throw out the baby with the bath water.

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Antidromic-rectifying gap junctions amplify chemical transmission at functionally mixed electrical-chemical synapses

Nature Communications ◽

10.1038/ncomms14818 ◽

2017 ◽

Vol 8 (1) ◽

Cited By ~ 41

Author(s):

Ping Liu ◽

Bojun Chen ◽

Roger Mailler ◽

Zhao-Wen Wang

Keyword(s):

Gap Junctions ◽

Chemical Synapses ◽

Chemical Transmission

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Electrical synaptic transmission in developing zebrafish: properties and molecular composition of gap junctions at a central auditory synapse

Journal of Neurophysiology ◽

10.1152/jn.00397.2014 ◽

2014 ◽

Vol 112 (9) ◽

pp. 2102-2113 ◽

Cited By ~ 19

Author(s):

Cong Yao ◽

Kimberly G. Vanderpool ◽

Matthew Delfiner ◽

Vanessa Eddy ◽

Alexander G. Lucaci ◽

...

Keyword(s):

Synaptic Transmission ◽

Gap Junctions ◽

Developmental Stages ◽

Neural Function ◽

Electrical Transmission ◽

Electrical Synapses ◽

Connexin 36 ◽

Auditory Responses ◽

Electrophysiological Recordings ◽

Chemical Synapses

In contrast to the knowledge of chemical synapses, little is known regarding the properties of gap junction-mediated electrical synapses in developing zebrafish, which provide a valuable model to study neural function at the systems level. Identifiable “mixed” (electrical and chemical) auditory synaptic contacts known as “club endings” on Mauthner cells (2 large reticulospinal neurons involved in tail-flip escape responses) allow exploration of electrical transmission in fish. Here, we show that paralleling the development of auditory responses, electrical synapses at these contacts become anatomically identifiable at day 3 postfertilization, reaching a number of ∼6 between days 4 and 9. Furthermore, each terminal contains ∼18 gap junctions, representing between 2,000 and 3,000 connexon channels formed by the teleost homologs of mammalian connexin 36. Electrophysiological recordings revealed that gap junctions at each of these contacts are functional and that synaptic transmission has properties that are comparable with those of adult fish. Thus a surprisingly small number of mixed synapses are responsible for the acquisition of auditory responses by the Mauthner cells, and these are likely sufficient to support escape behaviors at early developmental stages.

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Intraglomerular dendritic link connected by gap junctions and chemical synapses in the mouse main olfactory bulb: Electron microscopic serial section analyses

Neuroscience ◽

10.1016/j.neuroscience.2004.11.050 ◽

2005 ◽

Vol 131 (3) ◽

pp. 611-625 ◽

Cited By ~ 30

Author(s):

T. Kosaka ◽

K. Kosaka

Keyword(s):

Olfactory Bulb ◽

Gap Junctions ◽

Serial Section ◽

Main Olfactory Bulb ◽

Electron Microscopic ◽

Chemical Synapses

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Effects of gap junction misexpression on synapses between auditory sensory neurons and the giant fiber of Drosophila melanogaster

10.1101/331074 ◽

2018 ◽

Author(s):

Sami H. Jezzini ◽

Amelia Merced ◽

Jonathan M. Blagburn

Keyword(s):

Transcription Factor ◽

Drosophila Melanogaster ◽

Gap Junctions ◽

Sensory Neurons ◽

De Novo ◽

Dye Coupling ◽

Giant Fiber ◽

Mixed Synapses ◽

Chemical Synapses ◽

Gap Junctional

AbstractThe synapse between auditory Johnston’s Organ neurons (JONs) and the giant fiber (GF) of Drosophila is structurally mixed, being composed of cholinergic chemical synapses and Neurobiotin-(NB) permeable gap junctions, which consist of the innexin Shaking-B (ShakB). Misexpression of one ShakB isoform, ShakB(N+16), in a subset of JONs that do not normally form gap junctions, results in their de novo dye coupling to the GF. This is similar to the effect of misexpression of the transcription factor Engrailed (En) in these same neurons, which also causes the formation of additional chemical synapses. In order to test the hypothesis that ShakB misexpression would similarly affect the distribution of chemical synapses, fluorescently-labeled presynaptic active zone protein (Brp) was expressed in JONs and the changes in its distribution were assayed with confocal microscopy. Both ShakB(N+16) and En increased the dye-coupling of JONs with the GF, indicating the formation of ectopic gap junctions. Conversely, expression of the ‘incorrect’ isoform, ShakB(N) abolishes dye coupling. However, while En misexpression increased the chemical contacts with the GF and the amount of GF medial branching, ShakB misexpression did not. ShakB immunocytochemistry showed that misexpression of ShakB(N+16) increases gap junctional plaques in JON axons but ShakB(N) does not. We conclude that both subsets of JON form chemical synapses onto the GF dendrites but only one population forms gap junctions, comprised of ShakB(N+16). Misexpression of this isoform in all JONs does not result in the formation of new mixed synapses but in the insertion of gap junctions, presumably at the sites of existing chemical synaptic contacts with the GF.

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Idealized model of the developing visual cortex

10.1101/2020.04.29.067942 ◽

2020 ◽

Author(s):

Jennifer Crodelle ◽

David W. McLaughlin

Keyword(s):

Synaptic Plasticity ◽

Visual Cortex ◽

Gap Junctions ◽

Gap Junction ◽

Pyramidal Cells ◽

Orientation Preference ◽

Coupled Cells ◽

Junction Coupling ◽

Chemical Synapses ◽

Cortical Map

AbstractRecent experiments in the developing mammalian visual cortex have revealed that gap junctions couple excitatory cells and potentially influence the formation of chemical synapses. Though gap junctions between inhibitory cells are ubiquitous in the adult cortex, and their presence has been shown to promote synchronous network firing, their function among excitatory, pyramidal cells remains poorly understood. During development, pyramidal cells that were derived from the same progenitor cell, called sister cells, are preferentially connected by a gap junction during the first postnatal week, while chemical synapses are still being formed. Additionally, these sister cells tend to share an orientation preference and a chemical synapse in the adult cortex, a property that is diminished when gap junctions are blocked. In this work, we construct an idealized model of the mouse visual cortex during the first two postnatal weeks of development to analyze the response properties of gap-junction-coupled cells and their effect on synaptic plasticity. Further, as an application of this model, we investigate the interplay of gap-junction coupling and synaptic plasticity on the order, or organization, of the resulting cortical map of orientation preference.Author summaryGap junctions, or sites of direct electrical connections between neurons, have a significant presence in the cortex, both during development and in adulthood. Their primary function during either of these periods, however, is still poorly understood. In the adult cortex, gap junctions between local, inhibitory neurons have been shown to promote synchronous firing, a network characteristic thought to be important for learning, attention, and memory. During development, gap junctions between excitatory, pyramidal cells, have been conjectured to play a role in synaptic plasticity and the formation of cortical circuits. In the visual cortex, where neurons exhibit tuned responses to properties of visual input such as orientation and direction, recent experiments show that excitatory cells are coupled by gap junctions during the first postnatal week and are replaced by chemical synapses during the second week. In this work, we explore the possible contribution of gap-junction coupling during development to the formation of chemical synapses both into the visual cortex from the thalamus and within the visual cortex between cortical cells. Specifically, within a mathematical model of the visual cortex during development, we identify the response properties of gap-junction-coupled cells and their influence on the formation of the cortical map of orientation preference.

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Behavioral control by depolarized and hyperpolarized states of an integrating neuron

eLife ◽

10.7554/elife.67723 ◽

2021 ◽

Vol 10 ◽

Author(s):

Aylesse Sordillo ◽

Cornelia I Bargmann

Keyword(s):

Caenorhabditis Elegans ◽

Gap Junctions ◽

Behavioral Control ◽

Spontaneous Behavior ◽

Chemical Synapses ◽

Insight Into

Coordinated transitions between mutually exclusive motor states are central to behavioral decisions. During locomotion, the nematode Caenorhabditis elegans spontaneously cycles between forward runs, reversals, and turns with complex but predictable dynamics. Here, we provide insight into these dynamics by demonstrating how RIM interneurons, which are active during reversals, act in two modes to stabilize both forward runs and reversals. By systematically quantifying the roles of RIM outputs during spontaneous behavior, we show that RIM lengthens reversals when depolarized through glutamate and tyramine neurotransmitters and lengthens forward runs when hyperpolarized through its gap junctions. RIM is not merely silent upon hyperpolarization: RIM gap junctions actively reinforce a hyperpolarized state of the reversal circuit. Additionally, the combined outputs of chemical synapses and gap junctions from RIM regulate forward-to-reversal transitions. Our results indicate that multiple classes of RIM synapses create behavioral inertia during spontaneous locomotion.

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