To characterize DS in presynaptic RGC axon terminals in the neuropil, we used the panneuronal Tg(huC:Gal4;UAS:GCaMP3) line and isolated presynaptic Ca2+ signals by locally applying blockers of glutamatergic transmission to the tectum using a local perfusion Selleck Enzalutamide pipette
( Figure 6A; Figure S4). The dorsal half of the tectal neuropil (including SFGS and SO) was imaged and a sliding window was used to assign local PD and DSI values as a function of distance from the SPV/neuropil boundary ( Figures 6A–6C). Remarkably, presynaptic compartments exhibited strong, directionally tuned Ca2+ signals (e.g., Figures 6B and 6C), indicating that DS-RGCs carry retinally processed DS signals
to the tectal neuropil. More importantly, the PDs of presynaptic DS Ca2+ transients were distributed in a layered fashion, with a strong check details preference for CR motion in a narrow band near the 78% level of tectal neuropil and RC motion components in more distal and proximal regions ( Figures 6C and 6D). The CR-preferring thin layer (red band in Figure 6C, top) colocalized with a brightly labeled boundary in Tg(huC:Gal4;UAS:GCaMP3) fish ( Figure 6C, bottom), which could represent a superficial sublayer of the SFGS, but below the SO. To test for colocalization of pre- and postsynaptic DS signals with respect to their PDs, we plotted the averaged PD histograms of pharmacologically isolated RGC-terminal Ca2+ transients ( Figure 6E, top) and of postsynaptic Ca2+ transients in type 1 and type 2 cell dendrites in the Tg(Oh:G-3;Oh:G-4;UAS:GCaMP3) fish ( Figure 6E, bottom) and compared their direction-specific intensity
profiles ( Figure 6F). This analysis showed that the distribution of CR-DS postsynaptic compartments overlapped considerably too with the accumulation of CR-DS presynaptic compartments near the 78% level of the distal neuropil ( Figure 6F, red traces). Similarly, the position of RC-DS postsynaptic compartments was in good agreement with the location of a distal band in the distribution of RC-DS presynaptic compartments. The data can also be used to analyze the distribution of PDs of presynaptic Ca2+ signals in the top third of the neuropil (levels > 65%). We observed three peaks from Gaussian fits to the histogram of summed DSIs, at 5° (corresponding to CR motion), 129° (RC-DU motion), and 218° (RC-UD motion) (Figure 6G), in good agreement with the PD of three DS-RGC types projecting to the teleost tectum (Maximov et al., 2005; Nikolaou et al., 2012). Figure 6H shows that local perfusion with blockers of glutamatergic transmission effectively abolished postsynaptic activity in response to visual stimulation (see also Figures S4B and S4C).