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首页> 外文期刊>The Journal of Comparative Neurology >Circuitry and role of substance P-immunoreactive neurons in the primate retina.
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Circuitry and role of substance P-immunoreactive neurons in the primate retina.

机译:灵长类动物视网膜中P物质免疫反应性神经元的回路和作用。

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摘要

In this paper, we extend our previous light microscopic (LM) study of substance P (SP)-containing amacrine and ganglion cell types of the human retina (Cuenca et al. [1995] J. Comp. Neurol. 356:491-504) to an electron microscopic (EM) and confocal-imaging study in order to reveal synaptic circuitry and putative input and output neurons. SP-immunoreactive (-IR) amacrine cells in primate retina are typically wide-field cells with large cell bodies occurring in normal or displaced positions relative to the inner plexiform layer (IPL). Their main dendrites bear many spines and are monostratified in stratum 3 (S3) of the IPL. Axon-like processes arise from dendrites close to the cell body and run for hundreds of microns at the same level as the dendrites, thus forming a relatively dense plexus in S3 of the IPL. SP-IR axon processes also climb to S1 to surround some amacrine cell bodies, and others pass into the outer plexiform layer (OPL). Still other axons run down to the ganglion cell layer, where they encircle SP-IR ganglion cells and pass on to end in the nerve fiber layer. The SP-IR ganglion cell types have large cell bodies (20-22 microm diameter) and dendrites that costratify in S3 among the SP-IR amacrine cell processes. Double immunostaining and study by confocal microscopy reveals that SP-IR amacrine cells in the monkey colocalize gamma-aminobutyric acid (GABA). Their main plexus of dendrites in S3 of the IPL is skirted on the S2/S3 border by cone bipolar axons that stain for calbindin but intermingles primarily with glycinergic bipolar cell types of S3 and S3-S4. Strongly GABA-IR/weakly glycine-IR amacrine cell bodies, in addition to the SP-IR large-bodied ganglion cell type, are targets of encircling SP-IR axon processes. EM study of the human SP-IR amacrine cell indicates that input synapses to its dendrites are from bipolar cell axons of the S2/S3 border, S3, and the S3/S4 border of the IPL neuropil (33% of the synaptic input) and from amacrine cell processes (67% of the synaptic input). The input amacrine cells are of at least two distinct types based on cytological criteria. Synaptic output from the SP-IR amacrine cell dendrites is to bipolar cell axons as reciprocal synapses (31%), to amacrine cells (40%), and to ganglion cell profiles, primarily in S3 (29%) of the IPL. The SP-IR axons synapse upon SP-IR ganglion cell bodies and axons, upon normally placed and displaced amacrine cell bodies, and upon bipolar cell dendrites in the OPL. In addition, they appear to synapse among themselves. We shall discuss a wiring diagram and the possible role of SP-IR amacrine cells in the primate retina.
机译:在本文中,我们扩展了先前对人类视网膜中含有P(SP)物质的无长突神经节和神经节细胞类型的光学显微镜(LM)研究(Cuenca等人,[1995] J. Comp。Neurol。356:491-504 )进行电子显微镜(EM)和共聚焦成像研究,以揭示突触电路和推定的输入和输出神经元。灵长类动物视网膜中的SP免疫反应(-IR)无长春碱细胞通常是具有大细胞体的宽视野细胞,相对于内部丛状层(IPL)处于正常或移位位置。它们的主要树突带有许多刺,并在IPL的第3层(S3)中单层化。轴突样过程起因于靠近细胞体的树突,并在与树突相同的水平上延伸数百微米,从而在IPL的S3中形成相对致密的丛。 SP-IR轴突过程也爬到S1周围,包围了一些无长突细胞体,其他的则进入了外部丛状层(OPL)。还有其他轴突向下延伸到神经节细胞层,在那里它们包围SP-IR神经节细胞,并在神经纤维层中终止。 SP-IR神经节细胞类型具有较大的细胞体(直径为20-22微米),并且在SP-IR无长突细胞过程中在S3中共同树突化了树突。双重免疫染色和共聚焦显微镜研究表明,猴子中的SP-1R无长突细胞共定位γ-氨基丁酸(GABA)。它们在IPL S3中的主要树突丛在S2 / S3边界上被锥形双极轴突所包围,该轴突染色了钙结合蛋白,但主要与S3和S3-S4的甘氨酸双极细胞类型混合。除了SP-IR大神经节细胞类型之外,强烈的GABA-IR /弱甘氨酸-IR长春红素细胞体也是环绕SP-IR轴突过程的目标。对人SP-IR无长突细胞的EM研究表明,其树突的输入突触来自IPL Neuropil的S2 / S3边界,S3和S3 / S4边界的双极细胞轴突(占突触输入的33%)和来自无长突细胞过程(突触输入的67%)。根据细胞学标准,输入的无长分泌细胞是至少两种不同的类型。 SP-IR无长突细胞树突的突触输出主要是在IPL的S3(29%)中以双突触突向双极细胞轴突(31%),无长突细胞(40%)和神经节细胞分布。 SP-IR轴突突触到OP-L中的SP-IR神经节细胞体和轴突,正常放置和移位的无长突突细胞体以及双极细胞树突。另外,它们似乎在彼此之间具有突触。我们将讨论布线图以及SP-IR无长突细胞在灵长类动物视网膜中的可能作用。

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