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      Voltage-sensitive dye imaging during functional development of the embryonic nervous system: a brief review with special thanks to Professor Larry Cohen

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          Abstract.

          Investigating the developmental organization of the embryonic nervous system is one of the major challenges in the field of neuroscience. Despite their significance, functional studies on the vertebrate embryonic central nervous system (CNS) have been hampered by the technical limitations associated with conventional electrophysiological methods. The advent of optical techniques using voltage-sensitive dyes, which were developed by Dr. Cohen and his colleagues, has enabled electrical activity in living cells to be monitored noninvasively and also facilitated the simultaneous recording of neural responses from multiple regions. Using optical recording techniques, it is now possible to follow the functional organization of the embryonic CNS and image the spatiotemporal dynamics involved in the formation of this neural network. We herein briefly reviewed optical studies on the embryonic CNS with a special emphasis on methodological considerations and the study of neuronal circuit formation, which demonstrates the utility of fast voltage-sensitive dye imaging as a powerful tool for elucidating the functional organization of the embryonic CNS.

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          Most cited references18

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          Sensory receptors—design principles revisited

          This research topic was aimed toward collecting the present knowledge of structure and function of sensory receptors in animal kingdom as well as the mechanisms of signal transduction and amplification. To translate external signals such as light, sound, smell, etc., into an appropriate intracellular signal, sensory receptors use either a fast, direct or a slow, indirect way. These qualitatively different signal transduction pathways are now usually called ionotopic or metabotropic. Historically, the term metabotropic receptor has been introduced to distinguish a subtype of glutamate receptors that triggers chemical reactions (cell metabolism) in the postsynaptic cell from other glutamate receptors that pass an ion current (ionotropic) (Eccles and McGeer, 1979). Metabotropic glutamate receptors were found to be linked to inositol phospholipid metabolism (Sugiyama et al., 1987), and were subsequently identified as G-protein-coupled receptors (GPCRs) (Masu et al., 1991). The terminology ionotropic/metabotropic has been extended to other neurotransmitter receptors, such as for nicotinic/muscarinergic acetyl choline or GABAA/GABAB receptors. All metabotropic neurotransmitter receptors are GPCRs. There are, however, a large number of non-GPCRs that also fulfill the original definition for a metabotropic receptor, namely “that the transmitter acts indirectly, by triggering a chemical reaction or a series of reactions” (Eccles and McGeer, 1979). Accordingly, it has been used to extent the term metabotropic receptor to receptor kinases, receptor cyclases, etc., as well. Sensory receptors are often part of complex signal transduction cascades. An ion current through an ionotropic receptor may initiate metabotropic signaling, as well as a metabotropic receptor may downstream affect the function of ion channels. An example for protein–protein interaction in chemosensation is given in the original article by Liu et al. (2012). The authors identified so far unknown binding partners of Gγ13, a G-protein subunit expressed in mammalian taste and olfactory receptor cells. These binding partners are PDZ-domain containing proteins assumed to target Gγ13 to specific subcellular locations or represent parts of the chemosensory signal transduction cascade. The evolution of chemoreceptors shows that—from bacteria to mammals—both, ionotropic as well as metabotropic mechanisms were conserved. Functional aspects of chemoreceptors, including the interaction of electrical and chemical signaling, and the amplification of sensory information are discussed in the perspective article (Wicher, 2012). Intriguingly, insect chemoreceptors operate as ionotropic receptors, namely odorant receptors (ORs), ionotropic glutamate-like receptors (IRs), and gustatory receptors (GRs). Getahun et al. (2012) investigate the temporal response dynamics of insect chemoreceptors and demonstrate that olfactory sensory neurons (OSNs) expressing ORs, GRs, or IRs differ in their response kinetics to brief stimuli. OR-expressing neurons respond faster and with higher sensitivity, while IR-expressing neurons do not adapt to long stimulations. Although ORs primarily operate as ionotropic receptors, metabotropic signaling was seen to modulate the ionotropic odor response (Olsson et al., 2011; Sargsyan et al., 2011). Stimulation of cAMP production enhanced the response to a given odor concentration, corresponding to an increased sensitivity. This type of modulation may constitute the mechanistic basis for the higher sensitivity of ORs compared with IRs. Chemical information released from different sources may interfere during processing in the nervous system and affect the response of an organism. Odor mixtures can act in synergistic or in an inhibitory way. On the level of the chemoreceptors the existence of a huge number of different chemical signal molecules leads to the intriguing question of receptor specificity and whether a given chemical signal is perceived independent of the background. The interaction of odorant and pheromone detection in moths is reported by Pregitzer et al. (2012) and commented by Anton and Renou (2012). Certain plant odors are known to inhibit the activation of pheromone receptors. The reported investigations provide evidence that the odorant-pheromone interaction already takes place at the receptor level. Since the first editorial to this topic was written in 2010 recent progress shed new light on structure and function of certain receptors. Channelrhodopsins, for example, are photoreceptors in green algae which conduct a current upon illumination. They are seven transmembrane (7-TM)-spanning proteins as typical for GPCRs but do not couple to a heterotrimeric G-protein. With the given 7-TM topology it was as yet not clear how the channelrhodopsin proteins have to arrange to form an ion channel. Recently, the non-selective cation channel, channelrhodopsin-2 from Chlamydomonas reinhardtii has been successfully crystallized (Müller et al., 2011; Kato et al., 2012). The channelrhodopsin-2 proteins were found to stably dimerize in such an arrangement that the third and the fourth TM helix of each protein align to a tetramer thereby lining the cation-permeable pore. Another example for ion channel-forming 7-TM proteins are the above mentioned insect ORs. In contrast to homodimeric channelrhodopsin channels they are heterodimers, composed of variable, odorant-binding protein OrX, and an ubiquitous co-receptor OrCo. There is growing evidence that both OR proteins contribute to channel pore formation and determine their properties such as the ion permeability and pharmacological properties (Nichols et al., 2011; Pask et al., 2011; Nakagawa et al., 2012). It remains to be established whether OrCo form homomeric channels in the receptor neurons as seen in the heterologous expression system and whether they represent the metabotropic pathway used to tune the sensitivity of the ionotropic receptor (Olsson et al., 2011; Sargsyan et al., 2011). The role of stimulatory G-proteins in olfactory signaling has been demonstrated (Deng et al., 2011), and also downstream signaling such as cAMP production were seen to affect the odor response of receptor neurons (Olsson et al., 2011). These recent findings on insect OR function modify the view to classify them. While in the first editorial they have been considered as combined metabotropic and ionotropic receptors, they might now be more appropriately characterized as metabotropically regulated ionotropic receptors. This change of view illustrates the highly dynamic development in the field.
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            Changes in neuron structure during action potential propagation and synaptic transmission.

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              Optical imaging of neuronal activity.

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                Author and article information

                Journal
                Neurophotonics
                Neurophotonics
                NEUROW
                NPh
                Neurophotonics
                Society of Photo-Optical Instrumentation Engineers
                2329-423X
                2329-4248
                3 February 2015
                April 2015
                : 2
                : 2
                : 021009
                Affiliations
                [a ]Kanto Gakuin University , College of Human and Environmental Studies, Department of Health and Nutrition, 1-50-1 Mutsuura-higashi, Kanazawa-ku, Yokohama 236-8503, Japan
                [b ]Komazawa Women’s University Faculty of Human Health , Department of Health and Nutrition Sciences, 238 Sakahama, Inagi-shi, Tokyo 206-8511, Japan
                Author notes
                [* ]Address all correspondence to: Katsushige Sato, E-mail: katsu-satoh@ 123456komajo.ac.jp
                Article
                NPH-14078VSSR 14078VSSR
                10.1117/1.NPh.2.2.021009
                4478868
                26157999
                e9c0a480-f01f-406e-b3d7-388fb9035b12
                © The Authors. Published by SPIE under a Creative Commons Attribution 3.0 Unported License. Distribution or reproduction of this work in whole or in part requires full attribution of the original publication, including its DOI.
                History
                : 2 December 2014
                : 31 December 2014
                Page count
                Figures: 3, Tables: 0, References: 18, Pages: 5
                Categories
                Special Section Papers
                Paper
                Pioneers in Neurophotonics: Special Section Honoring Professor Lawrence B. Cohen
                Custom metadata
                Momose-Sato and Sato: Voltage-sensitive dye imaging during functional development of the embryonic nervous system…

                optical recording,voltage-sensitive dye,embryonic central nervous system,functiogenesis

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