Organization of the outer synaptic layer in the retina of the larval tiger Salamander

1973 ◽  
Vol 265 (872) ◽  
pp. 471-489 ◽  
Keyword(s):  
Bipolar Cell ◽  
Photoreceptor Cell ◽  
Horizontal Cell ◽  
Bipolar Cells ◽  
Horizontal Cells ◽  
Tiger Salamander ◽  
Serial Sections ◽  
Rods And Cones ◽  
Cell Processes ◽  
Rod Cell

The organization of the outer synaptic layer in the salamander retina was studied electronmicroscopically in serial sections of tissue prepared by conventional techniques or stained by the method of Golgi. Rod cell pedicles make ribbon junctions on cone cell processes, and rod cell processes invaginate cone pedicles without otherwise making any specialized contact with them. Horizontal cells make ribbon and distal junctions with the photoreceptor cell pedicles; a single horizontal cell may contact both rods and cones. Bipolar cells were observed to make either ribbon or basal junctions with the photoreceptor cell pedicles; in addition, certain processes believed to belong to bipolar cells make both ribbon and basal junctions with the same or different pedicles. A single bipolar cell may make contact with both rods and cones. Horizontal cells synapse on bipolar cell dendrites and on certain unidentified processes which in turn are also presynaptic to bipolar cells. Ascending branches of these processes invaginate deeply the rod and cone pedicles without otherwise engaging them in any junction. Horizontal cell processes are linked by two kinds of junctions: close membrane appositions, and contacts analogous to the distal junctions between horizontal cells and rod pedicles.

Synapse formation and modification between distal retinal neurons in larval and juvenile Xenopus

1981 ◽  
Vol 211 (1184) ◽  
pp. 373-389 ◽  
Keyword(s):  
Bipolar Cell ◽  
Synapse Formation ◽  
Developmental Stages ◽  
Horizontal Cell ◽  
Bipolar Cells ◽  
Horizontal Cells ◽  
Cell Junction ◽  
Ribbon Synapses ◽  
Cell Processes ◽  
Chemical Synapses

A serial section analysis of photoreceptor synaptic bases was undertaken in the clawed frog Xenopus laevis . The developmental period from tadpole stage 48 through metamorphosis was studied. Horizontal cells contacted rod and cone photoreceptors at ribbon synapses; the number of such contacts per receptor base was constant for rods, but increased for cones as a function-of developmental stage. In pre-metamorphic animals bipolar cells contacted receptors only through basal junctions; their number in cone bases increased dramatically during development but was unchanged in rod bases. A densitometric estimation of the cleft width of basal junctions showed that it ranged from 10 to 18 nm, but the junctions could not be divided reliably into the ‘wide’ and ‘narrow’ categories reported for other vertebrate species. Near metamorphic climax a new type of ribbon-related bipolar cell junction appeared. Gap junctions between horizontal cells and conventional chemical synapses of horizontal cell onto bipolar cell processes were first seen in mid-larval developmental stages.

Receptive field of the retinal bipolar cell: a pharmacological study in the tiger salamander

1996 ◽  
Vol 76 (3) ◽  
pp. 2005-2019 ◽  
Author(s):  
W. A. Hare ◽  
W. G. Owen
Keyword(s):  
Receptive Field ◽  
Gaba Receptors ◽  
Bipolar Cell ◽  
Horizontal Cell ◽  
Pharmacological Study ◽  
Bipolar Cells ◽  
Horizontal Cells ◽  
Gaba Uptake ◽  
Gamma Aminobutyric Acid ◽  
Gabaergic Synapse

1. It is widely believed that signals contributing to the receptive field surrounds of retinal bipolar cells pass from horizontal cells to bipolar cells via GABAergic synapses. To test this notion, we applied gamma-aminobutyric acid (GABA) agonists and antagonists to isolated, perfused retinas of the salamander Ambystoma tigrinum while recording intracellularly from bipolar cells, horizontal cells, and photoreceptors. 2. As we previously reported, administration of the GABA analogue D-aminovaleric acid in concert with picrotoxin did not block horizontal cell responses or the center responses of bipolar cells but blocked the surround responses of both on-center and off-center bipolar cells. 3. Surround responses were not blocked by the GABA, antagonists picrotoxin or bicuculline, the GABAB agonist baclofen or the GABAB antagonist phaclofen, and the GABAC antagonists picrotoxin or cis-4-aminocrotonic acid. Combinations of these drugs were similarly ineffective. 4. GABA itself activated a powerful GABA uptake mechanism in horizontal cells for which nipecotic acid is a competitive agonist. It also activated, both in horizontal cells and bipolar cells, large GABAA conductances that shunted light responses but that could be blocked by picrotoxin or bicuculline. 5. GABA, administered together with picrotoxin to block the shunting effect of GABAA activation, did not eliminate bipolar cell surround responses at concentrations sufficient to saturate the known types of GABA receptors. 6. Surround responses were not blocked by glycine or its antagonist strychnine, or by combinations of drugs designed to eliminate GABAergic and glycinergic pathways simultaneously. 7. Although we cannot fully discount the involvement of a novel GABAergic synapse, the simplest explanation of our findings is that the primary pathway mediating the bipolar cell's surround is neither GABAergic nor glycinergic.

Different types of synapses with different spectral types of cones underlie color opponency in a bipolar cell of the turtle retina

1999 ◽  
Vol 16 (5) ◽  
pp. 801-809 ◽  
Author(s):  
SILKE HAVERKAMP ◽  
WOLFGANG MÖCKEL ◽  
JOSEF AMMERMÜLLER
Keyword(s):  
Bipolar Cell ◽  
Metabotropic Glutamate Receptors ◽  
Horizontal Cell ◽  
Bipolar Cells ◽  
Horizontal Cells ◽  
Color Processing ◽  
Ionotropic Receptors ◽  
Metabotropic Glutamate ◽  
Different Types ◽  
Color Opponency

Electrophysiologically, color-opponent retinal bipolar cells respond with opposite polarities to stimulation with different wavelengths of light. The origin of these different polarities in the same bipolar cell has always been a mystery. Here we show that an intracellularly recorded and HRP-injected, red-ON, blue/green-OFF bipolar cell of the turtle retina made invaginating (ribbon associated) synapses exclusively with L-cones. Non-invaginating synapses resembling wide-cleft basal junctions were made exclusively with M-cones. Input from S-cones was not seen. From these results we suggest sign-inverting transmission from L-cones at invaginating synapses via metabotropic glutamate receptors, and sign-conserving transmission from M-cones at wide-cleft basal junctions via ionotropic receptors. To explain the pronounced blue sensitivity of the bipolar cell, computer simulations were performed using a sign-conserving input from a yellow/blue chromaticity-type (H3) horizontal cell. The response properties of the red-ON, blue/green-OFF bipolar cell could be quantitatively reproduced by this means. The simulation also explained the asymmetry in L- and M-cone inputs to the bipolar cell as found in the ultrastructural analysis and assigned a putative role to H3 horizontal cells in color processing in the turtle retina.

Contribution of rod, on-bipolar, and horizontal cell light responses to the ERG of dogfish retina

1999 ◽  
Vol 16 (3) ◽  
pp. 503-511 ◽  
Author(s):  
R.A. SHIELLS ◽  
G. FALK
Keyword(s):  
Bipolar Cell ◽  
Time Course ◽  
Horizontal Cell ◽  
Full Range ◽  
Bipolar Cells ◽  
Horizontal Cells ◽  
Negative Wave ◽  
Low Light ◽  
Cell Responses ◽  
Light Intensities

Simultaneous extracellular ERG and intracellular recordings from horizontal and ON-bipolar cells were obtained from the dark-adapted retina of the dogfish. The light intensity–peak response relation (IR) and time course of on-bipolar cell responses closely resembled that of the ERG b-wave, but only at low light intensities [<10 rhodopsin molecules bleached per rod (Rh*)]. Block of on-bipolar cell responses with 50 μM 2-amino-4-phosphonobutyrate (APB) abolished the b-wave and unmasked a vitreal-negative wave. Subtraction from the control ERG resulted in the isolation of a vitreal-positive ERG with an IR which matched that of on-bipolar cells over the full range of light intensities. The D.C. component of the ERG arises as a result of sustained depolarization of on-bipolar cells in response to long (>0.5 s) dim light stimuli, or following bright light flashes. The IR of horizontal cells and the vitreal-negative wave unmasked by APB could be matched by scaling at low light intensities (<5 Rh*). However, horizontal cell responses saturated at about 30 Rh*, while the vitreal-negative wave continued to increase in amplitude. The time course of horizontal cell membrane current with dim flashes could be matched to the rising phase of the vitreal-negative wave, assuming that the delay in generating the voltage response in horizontal cells is due to their long (100 ms) membrane time constant. Blocking post-photoreceptor activity resulted in a much smaller vitreal-negative wave than that unmasked by APB alone. We conclude that the b-wave arises from on-bipolar cell depolarization, while the leading edge of the a-wave is a composite of the change in extracellular voltage drop across the rod layer and a component (proximal PIII) reflecting a decrease in extracellular K+ as horizontal cell synaptic channels close with light.

scholarly journals Analyses of bipolar cell responses elicited by polarization of horizontal cells.

1982 ◽  
Vol 79 (1) ◽  
pp. 131-145 ◽  
Author(s):  
J Toyoda ◽  
T Kujiraoka
Keyword(s):  
Bipolar Cell ◽  
Horizontal Cell ◽  
Bipolar Cells ◽  
Horizontal Cells ◽  
Na Channels ◽  
Cell Responses ◽  
Ionic Mechanisms ◽  
Cl Channels ◽  
Hyperpolarizing Response ◽  
Conductance Changes

Simultaneous intracellular recordings were made from a bipolar cell and a horizontal cell in the carp retina. The properties of the bipolar cell were studied while injecting current into the horizontal cell. Hyperpolarization of horizontal cells, irrespective of their type, elicited a hyperpolarizing response in on-center bipolar cells and a depolarizing response in off-center bipolar cells. Analyses of the ionic mechanisms of bipolar cell responses revealed that depolarization of horizontal cells simulated and hyperpolarization opposed the effect of central illumination. The effect of polarization was exerted in such a manner that each type of horizontal cells modified the transmission from those photoreceptors from which they receive main inputs. In on-center bipolar cells, for example, the L-type horizontal cells receiving inputs mainly from red cones modified the cone-bipolar transmission accompanied by a conductance change of K+ and/or Cl- channels, and the intermediate horizontal cells receiving inputs from rods modified the rod-bipolar transmission accompanied by a conductance change of Na+ channels. In off-center bipolar cells, the effect of polarization of any type of horizontal cells was mediated mainly by conductance changes of Na+ channels. Feedback mechanisms from horizontal cells to photoreceptors could explain these results reasonably well.

Synaptic organization of cone cells in the turtle retina

1971 ◽  
Vol 262 (844) ◽  
pp. 365-381 ◽  
Keyword(s):  
Horizontal Cell ◽  
Plexiform Layer ◽  
Intercellular Junctions ◽  
Bipolar Cells ◽  
Outer Plexiform Layer ◽  
Horizontal Cells ◽  
Synaptic Organization ◽  
Basal Surface ◽  
Cone Cells ◽  
Cell Processes

The intercellular junctions of cone pedicles in the turtle retina were studied electronmicroscopically in tissue prepared by conventional techniques or impregnated by the method of Golgi. Dendritic branchlets of bipolar cells make specialized contacts with the basal surface of the pedicles. Processes ending laterally to wedge-shaped projections (synaptic ridges) of the pedicles probably belong always to horizontal cells, and make proximal and distal (to the synaptic ridges) junctions with the pedicles. Processes ending opposite the apex of the synaptic ridges are engaged also in two kinds of specialized contacts, termed apical and distal junctions. Basal processes of the cone pedicles make specialized contacts with adjacent pedicles, and with unidentified processes at the outer plexiform layer; their endings abut upon horizontal cell processes lodged within the pedicles of other cone cells.

scholarly journals The Nature of Surround-Induced Depolarizing Responses in Goldfish Cones

1999 ◽  
Vol 115 (1) ◽  
pp. 3-16 ◽  
Author(s):  
D.A. Kraaij ◽  
H. Spekreijse ◽  
M. Kamermans
Keyword(s):  
Membrane Potential ◽  
Neurotransmitter Release ◽  
Calcium Current ◽  
Calcium Influx ◽  
Horizontal Cell ◽  
Activation Function ◽  
Bipolar Cells ◽  
Horizontal Cells ◽  
Calcium Dependent ◽  
Postsynaptic Cell

Cones in the vertebrate retina project to horizontal and bipolar cells and the horizontal cells feedback negatively to cones. This organization forms the basis for the center/surround organization of the bipolar cells, a fundamental step in the visual signal processing. Although the surround responses of bipolar cells have been recorded on many occasions, surprisingly, the underlying surround-induced responses in cones are not easily detected. In this paper, the nature of the surround-induced responses in cones is studied. Horizontal cells feed back to cones by shifting the activation function of the calcium current in cones to more negative potentials. This shift increases the calcium influx, which increases the neurotransmitter release of the cone. In this paper, we will show that under certain conditions, in addition to this increase of neurotransmitter release, a calcium-dependent chloride current will be activated, which polarizes the cone membrane potential. The question is, whether the modulation of the calcium current or the polarization of the cone membrane potential is the major determinant for feedback-mediated responses in second-order neurons. Depolarizing light responses of biphasic horizontal cells are generated by feedback from monophasic horizontal cells to cones. It was found that niflumic acid blocks the feedback-induced depolarizing responses in cones, while the shift of the calcium current activation function and the depolarizing biphasic horizontal cell responses remain intact. This shows that horizontal cells can feed back to cones, without inducing major changes in the cone membrane potential. This makes the feedback synapse from horizontal cells to cones a unique synapse. Polarization of the presynaptic (horizontal) cell leads to calcium influx in the postsynaptic cell (cone), but due to the combined activity of the calcium current and the calcium-dependent chloride current, the membrane potential of the postsynaptic cell will be hardly modulated, whereas the output of the postsynaptic cell will be strongly modulated. Since no polarization of the postsynaptic cell is needed for these feedback-mediated responses, this mechanism of synaptic transmission can modulate the neurotransmitter release in single synaptic terminals without affecting the membrane potential of the entire cell.

scholarly journals Histological Studies on the Retina of the Falcon "S Eye Ball (Circus Cyaneus C.) Under Light and Electron Microscopy

2012 ◽  
Vol 36 (2) ◽  
pp. 83-92
Author(s):  
Samawal Jassim Mohamed Al-Robaae
Keyword(s):  
Histological Study ◽  
Light And Electron Microscopy ◽  
Plexiform Layer ◽  
Internal Limiting Membrane ◽  
Bipolar Cells ◽  
Horizontal Cells ◽  
Histological Studies ◽  
Rods And Cones ◽  
Pigmented Epithelium ◽  
Circus Cyaneus

The histological study showed that the retina of falcon"s eyeball was thin at the peripheryand ranges between 0.6-0.8 μ but it was thick at center 1.68-2.64 μ. The retina consists fromten layers: pigmented epithelium, rods and cons layer, external nuclear layer, externalplexiform layer, internal nuclear layer, internal plexiform layer, Gangilionic cells layer,neurofibres layer and internal limiting membrane layer. The ultra-structural study stated thatthe rods and cons layers contained single rods with single and double cons. The retinacharacterized by lacking of the oil droplets in the internal segments of rods with narrowexternal plexiform layer in order to form network connecting rods and cones, horizontal cells,bipolar cells and Muller's cells.

scholarly journals Prion-induced photoreceptor degeneration begins with misfolded prion protein accumulation in cones at two distinct sites: cilia and ribbon synapses

2021 ◽  
Vol 9 (1) ◽  
Author(s):  
James F. Striebel ◽  
Brent Race ◽  
Jacqueline M. Leung ◽  
Cindi Schwartz ◽  
Bruce Chesebro
Keyword(s):  
Retinitis Pigmentosa ◽  
Prion Protein ◽  
Bipolar Cell ◽  
Brain Diseases ◽  
Protein Accumulation ◽  
Post Inoculation ◽  
Rods And Cones ◽  
Ribbon Synapses ◽  
Cell Processes ◽  
Prpsc Deposition

AbstractAccumulation of misfolded host proteins is central to neuropathogenesis of numerous human brain diseases including prion and prion-like diseases. Neurons of retina are also affected by these diseases. Previously, our group and others found that prion-induced retinal damage to photoreceptor cells in mice and humans resembled pathology of human retinitis pigmentosa caused by mutations in retinal proteins. Here, using confocal, epifluorescent and electron microscopy we followed deposition of disease-associated prion protein (PrPSc) and its association with damage to critical retinal structures following intracerebral prion inoculation. The earliest time and place of retinal PrPSc deposition was 67 days post-inoculation (dpi) on the inner segment (IS) of cone photoreceptors. At 104 and 118 dpi, PrPSc was associated with the base of cilia and swollen cone inner segments, suggesting ciliopathy as a pathogenic mechanism. By 118 dpi, PrPSc was deposited in both rods and cones which showed rootlet damage in the IS, and photoreceptor cell death was indicated by thinning of the outer nuclear layer. In the outer plexiform layer (OPL) in uninfected mice, normal host PrP (PrPC) was mainly associated with cone bipolar cell processes, but in infected mice, at 118 dpi, PrPSc was detected on cone and rod bipolar cell dendrites extending into ribbon synapses. Loss of ribbon synapses in cone pedicles and rod spherules in the OPL was observed to precede destruction of most rods and cones over the next 2–3 weeks. However, bipolar cells and horizontal cells were less damaged, indicating high selectivity among neurons for injury by prions. PrPSc deposition in cone and rod inner segments and on the bipolar cell processes participating in ribbon synapses appear to be critical early events leading to damage and death of photoreceptors after prion infection. These mechanisms may also occur in human retinitis pigmentosa and prion-like diseases, such as AD.

Morphological and functional identifications of catfish retinal neurons. I. Classical morphology

1975 ◽  
Vol 38 (1) ◽  
pp. 53-71 ◽  
Author(s):  
K. Naka ◽  
N. R. Garraway
Keyword(s):  
Ganglion Cells ◽  
Horizontal Cell ◽  
Dendritic Tree ◽  
Amacrine Cells ◽  
Cell Types ◽  
Bipolar Cells ◽  
Inner Nuclear Layer ◽  
Horizontal Cells ◽  
Specific Cell ◽  
Definition Of

The morphology of the catfish horizontal cells is comparable to that in other fish retinas. The external horizontal cells contact cone receptors and are stellate in shape; the intermediate horizontal cells are even more so and contact rod receptors. The internal horizontal cells constitute the most proximal layer of the inner nuclear layer and may possibly be, in reality, extended processes from the other two horizontal cell types. Bipolar cells resemble those in other teleost retinas: the size and shape of their dendritic tree encompass a continuous spectrum ranging from what is known as the small to the large bipolar cells. The accepted definition of amacrine cells is sufficiently vague to justify our originating a more descriptive and less inferential name for the (axonless) neurons in the inner nuclear layer which radiate processes throughout the inner synaptic layer. These starbust and spaghetti cells vary considerably in the character and extent of their dendritic spread, but correlates exist in other vertebrate retinas. Ganglion cells are found not only in the classical ganglion layer but displaced into the inner nuclear layer as well. Several types can be distinguished on the basis of cell geometry and by the properties of their dendritic tree. Not all of the categorization corresponds with previous descriptions; our findings suggest that some reorganization may be necessary in the accepted classification of cells in the proximal areas of the vertebrate retina. A subtle yet remarkable pattern underlies the entire structure of the catfish retina; there exists a definite gradient of size within a particular class of cells, and of configuration among the subclasses of a specific cell type. It remains to be seen if these morphological spectra bear any functional consequences. The fact that the structure of the catfish retina most closely resembles those of other phylogenetically ancient animals, such as the skate and the dogfish shark, testifies to its primitive organization; morphological and functional mechanisms discernible in this simple system may, therefore, be applicable to the retinas of higher ordered vertebrates.

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