4.7 Article

Microcircuitry for two types of achromatic ganglion cell in primate fovea

期刊

JOURNAL OF NEUROSCIENCE
卷 27, 期 10, 页码 2646-2653

出版社

SOC NEUROSCIENCE
DOI: 10.1523/JNEUROSCI.4739-06.2007

关键词

primate retina; ganglion cell; bipolar cell; microcircuitry; ribbon synapse; parallel pathways

资金

  1. NEI NIH HHS [R01 EY008124, EY12480, EY08124] Funding Source: Medline

向作者/读者索取更多资源

Synaptic circuits in primate fovea have been quantified for midget/parvocellular ganglion cells. Here, based on partial reconstructions from serial electron micrographs, we quantify synaptic circuits for two other types of ganglion cell: the familiar parasol/magnocellular cell and a smaller type, termed garland. The excitatory circuits both derive from two types of OFF diffuse cone bipolar cell, DB3 and DB2, which collected unselectively from at least 6 +/- 1 cones, including the S type. Cone contacts to DB3 dendrites were usually located between neighboring triads, whereas half of the cone contacts to DB2 were triad associated. Ribbon outputs were as follows: DB3, 69 +/- 5; DB2, 48 +/- 4. A complete parasol cell (30 mu m dendritic field diameter) would collect from similar to 50 cones via similar to 120 bipolar and similar to 85 amacrine contacts; a complete garland cell (25 mu m dendritic field) would collect from similar to 40 cones via similar to 75 bipolar and similar to 145 amacrine contacts. The bipolar types contributed differently: the parasol cell received most contacts (60%) from DB3, whereas the garland cell received most contacts (67%) from DB2. We hypothesize that DB3 is a transient bipolar cell and that DB2 is sustained. This would be consistent with their relative inputs to the brisk-transient (parasol) ganglion cell. The garland cell, with its high proportion of DB2 inputs plus its high proportion of amacrine synapses (70%) and dense mosaic, might correspond to the local-edge cell in nonprimate retinas, which serves finer acuity at low temporal frequencies. The convergence of S cones onto both types could contribute S-cone input for cortical areas primary visual cortex and the middle temporal area.

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