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2009年01月12日

【期刊论文】Subcellular Localization and Complements of GABAA and GABAC Receptors on Bullfrog Retinal Bipolar Cells

杨雄里, JIU-LIN DU AND XIONG-LI YANG

,-0001,():

-1年11月30日

摘要

Subcellular localization and complements of GABAA and GABAC receptors on bullfrog retinal bipolar cells. J Neurophysiol 84: 666-676, 2000. γ-Aminobutyric acid (GABA) receptors on retinal bipolar cells (BCs) are highly relevant to spatial and temporal integration of visual signals in the outer and inner retina. In the present work, subcellular localization and complements of GABAA and GABAC receptors on BCs were investigated by whole cell recordings and local drug application via multi-barreled puff pipettes in the bullfrog retinal slice preparation. Four types of the BCs (types 1-4) were identified morphologically by injection of Lucifer yellow. According to the ramification levels of the axon terminals and the responses of these cells to glutamate (or kainate) applied at their dendrites, types 1 and 2 of BCs were supposed to be OFF type, whereas types 3 and 4 of BCs might be ON type. Bicuculline (BIC), a GABAA receptor antagonist, and imidazole-4-acetic acid (I4AA), a GABAC receptor antagonist, were used to distinguish GABA receptor-mediated responses. In all BCs tested, not only the axon terminals but also the dendrites showed high GABA sensitivity mediated by both GABAA and GABAC receptors. Subcellular localization and complements of GABAA and GABAC receptors at the dendrites and axon terminals were highly related to the dichotomy of OFF and ON BCs. In the case of OFF BCs, GABAA receptors were rather evenly distributed at the dendrites and axon terminals, but GABAC receptors were predominantly expressed at the axon terminals. Moreover, the relative contribution of GABAC receptors to the axon terminals was prevalent over that of GABAA receptors, while the situation was reversed at the dendrites. In the case of ON BCs, GABAA and GABAC receptors both preferred to be expressed at the axon terminals; relative contributions of these two GABA receptor subtypes to both the sites were comparable, while GABAC receptors were much less expressed than GABAA receptors. GABAA, but not GABAC receptors, were expressed clusteringly at axons of a population of BCs. In a minority of BCs, I4AA suppressed the GABAC responses at the dendrites, but not at the axon terminal, implying that the GABAC receptors at these two sites may be heterogeneous. Taken together, these results suggest that GABAA and GABAC receptors may play different roles in the outer and inner retina and the differential complements of the two receptors on OFF and ON BCs may be closely related to physiological functions of these cells.

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2009年01月12日

【期刊论文】GLYCINERGIC SYNAPTIC TRANSMISSION TO BULLFROG RETINAL BIPOLAR CELLS IS INPUT-SPECIFIC

杨雄里, J. L. DUa, b* and X. L. YANGa, b

Neuroscience Vol. 113, No.4, pp. 779-784, 2002,-0001,():

-1年11月30日

摘要

Glycinergic inhibitory postsynaptic currents (IPSCs) focally elicited at the dendrites and axon terminals were recorded from bipolar cells in the bullfrog retinal slice, using the whole-cell clamp technique. IPSCs driven by input from interplexiform cells at bipolar cell dendrites (ipc-IPSCs) had a much slower decay time constant (25.29

retinal slice preparation,, whole-cell recording,, peak-scaled non-stationary noise analysis,, glycine receptor,, single-channel conductance.,

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2009年01月12日

【期刊论文】FUNCTIONAL GABAB RECEPTORS ARE EXPRESSED AT THE CONE PHOTORECEPTOR TERMINALS IN BULLFROG RETINA

杨雄里, J. LIU, a, b, J.-W. ZHAO, J.-LDUa, AND X.-L. YANGa*

Neuroscience 132(2005)103-113,-0001,():

-1年11月30日

摘要

GABAB receptors at the cone terminals in bullfrog retina were characterized by immunocytochemical and whole-cell patch clamp techniques in retinal slice preparations. Somata, axons and synaptic terminals (pedicles) of cones were both GABAB receptor (GABABR) 1 and GABABR2 immunoreactive. Physiologically, barium/calcium currents of cones to voltage steps were significantly reduced in size when GABA was puffed to cone terminals in the presence of picrotoxin that is supposed to block both GABAA and GABAC receptors. Similar reduction in barium currents was obtained with puff application of baclofen to cone terminals. These results suggest the presence of functional GABAB receptors at the bullfrog cone terminals. Suppression of barium currents of cones by baclofen was dose-dependent. Moreover, barium currents of cones were potentiated by background illumination, as compared with those recorded in the dark. 6,7-Dinitroquinoxaline-2,3-dione, an antagonist of non-NMDA receptors that hyperpolarizes horizontal cells and reduces GABA release from these cells, and saclofen, a GABAB receptor antagonist, both potentiated barium currents of cones in the dark, thereby mimicking the effects of background illumination. It is suggested that changes in calcium influx into the cone synaptic terminals due to activation of GABAB receptors may provide a negative feedback mechanism for regulating signal transmission between cones and secondorder neurons in the retina by modifying the amount of glutamate released from the cones.

GABA,, calcium channel,, barium current,, transmitter release,, horizontal cell.,

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2009年01月12日

【期刊论文】Glycine modulates the center response of ON type rod-dominant bipolar cells in carp retina

杨雄里, Yin Shen, Ling Chen, Yong Ping, Xiong-Li Yang*

Brain Research Bulletin 67(2005)492-497,-0001,():

-1年11月30日

摘要

pots, which was reversed by co-application of 10μM strychnine. It was further found that illumination of the receptive field surround did not affect the depolarizing center response of RBCs. The above result therefore suggests that glycine modulates the center response of RBCs. Focal application of glycine to either dendrites or axon terminals of RBCs failed to induce any currents in both isolated cell and retinal slice preparations. On the other hand, glycine of 4mM increased the amplitude of the scotopic electroretinographic PIIIcomponent, which reflects the activity of rod photoreceptors. It seems likely that modulation by glycine of the RBC center response may be in part ascribed to a consequence of the potentiation of rod responses by glycine.

Glycine, Bipolar cell, Carp retina, Receptive field

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2009年01月12日

【期刊论文】Modulation by melatonin of glutamatergic synaptic transmission in the carp retina

杨雄里, Hai Huang, , Shu-Chen Lee and Xiong-Li Yang

J Physiol 569.3 (2005) pp 857-871,-0001,():

-1年11月30日

摘要

Melatonin is involved in a variety of physiological functions through activating specific receptors coupled to GTP-binding protein.Melatonin and its receptors are abundant in the retina. Here we showfor the first time that melatoninmodulates glutamatergic synaptic transmission fromcones to horizontal cells (HCs) in carp retina. Immunocytochemical data revealed the expression of the MT1 receptoroncarpHCs.Whole-cell recordings further showedthat melatonin ofphysiological concentrationspotentiatedglutamate-inducedcurrents fromisolatedcone-drivenHCs(H1cells) in a dose-dependent manner, by increasing the efficacy and apparent affinity of the glutamate receptor. The effects of melatonin were reversed by luzindole, but not by K 185, indicating the involvement of the MT1 receptor. Like melatonin, methylene blue (MB), a guanylate cyclase inhibitor, also potentiated the glutamate currents, but internal infusion of cGMP suppressed them. The effects of melatonin were not observed in cGMP-filled and MB-incubated HCs. These results suggest that the melatonin effects may be mediated by decreasing the intracellular concentration of cGMP. Consistent with these observations, melatonin depolarized the membrane potential of H1 cells and reduced their light responses, which could also be blocked by luzindole. These effects of melatonin persisted in the presence of the antagonists of receptors for dopamine, GABA and glycine, indicating a direct action of melatonin on H1 cells. Such modulation by melatonin of glutamatergic transmission from cones to HCs is thought to be in part responsible for circadian changes in light responsiveness of cone HCs in teleost retina.

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    复旦大学,上海

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