Glaucoma is a progressive optic neuropathy, characterized by the selective loss of retinal ganglion cells (RGCs). Therefore, monitoring the change of number or morphology of RGC is essential for the early detection as well as investigation of pathophysiology of glaucoma. Since RGC layer is transparent and hyporeflective, the direct optical visualization of RGCs has not been successful so far. Therefore, glaucoma evaluation mostly depends on indirect diagnostic methods such as the evaluation of optic disc morphology or retinal nerve fiber layer thickness measurement by optical coherence tomography.
We have previously demonstrated single photoreceptor cell imaging with differential interference contrast (DIC) microscopy. Herein, we successfully visualized single RGC using DIC microscopy. Since RGC layer is much less reflective than photoreceptor layer, various techniques including the control of light wavelength and bandwidth using a tunable band pass filter were adopted to reduce the chromatic aberration in z-axis for higher and clearer resolution. To verify that the imaged cells were the RGCs, the flat-mounted retina of Sprague-Dawley rat, in which the RGCs were retrogradely labeled with fluorescence, was observed by both fluorescence and DIC microscopies for direct comparison. We have confirmed that the cell images obtained by fluorescence microscopy were perfectly matched with cell images by DIC microscopy.
As conclusion, we have visualized single RGC with DIC microscopy, and confirmed with fluorescence microscopy.
Juyeong Oh, Yu Jeong Kim, Chul-Ki Kim, Taik Jin Lee, Mina Seo, Seok Lee, Deok Ha Woo, Seong Chan Jun, Ki-Ho Park, Seok Hwan Kim, and Jae Hun Kim, "Imaging of single retinal ganglion cell with differential interference contrast microscopy (Conference Presentation)," Proc. SPIE 10045, Ophthalmic Technologies XXVII, 100450N (Presented at SPIE BiOS: January 29, 2017; Published: 16 May 2017); https://doi.org/10.1117/12.2251585.5370275052001.
Conference Presentations are recordings of oral presentations given at SPIE conferences and published as part of the proceedings. They include the speaker's narration with video of the slides and animations. Most include full-text papers. Interactive, searchable transcripts and closed captioning are now available for most presentations.
Search our growing collection of more than 22,000 conference presentations, including many plenaries and keynotes.