quantification of retinal ganglion cell somas following cauterization-induced ocular hypertension 

Quantification of Retinal Ganglion Cell Somas Following Cauterization-Induced Ocular Hypertension 

After isolating the retinas, transfer them into a 24-well culture plate containing 1 milliliter PBS, keeping the inner retina facing up. Permeabilize the tissue by washing with a 0.5% non-ionic surfactant diluted in PBS.&#160;Then, incubate the tissue in blocking solution for one hour at room temperature with gentle shaking. During the incubation, prepare BRM 3A primary antibody solution and store at 4 degree celsius.After tissue blocking, incubate the retinas in 200 microliters of primary antibody solution at 4 degrees celsius for 72 hours with gentle shaking. Next, wash the tissue with PBS. Incubate the tissue in 200 microliters of the secondary antibody solution for two hours at room temperature, and then with nuclear counterstain solution for 10 minutes for fluorescent nuclei staining.After three PBS washes, transfer the retina onto a glass microscope slide using two small brushes, maintaining the vitreous side up. Position the dorsal retinal quadrant up on the microscope slide. Finally, apply 200 microliters of anti-fade mounting medium on a glass coverslip and place it onto the flat mounted retina for microscopic analysis. Under a confocal epi-fluorescence microscope using a 40 times magnifying objective, examine the flat mounts to estimate retinal ganglion cells.

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All procedures involving animal samples have been reviewed and approved by the appropriate animal ethical review committee.&#160;&#160;&#160;&#160;1. Quantification of retinal ganglion cells somasNOTE: The following procedure is for quantification of RGC somas, based on immunohistochemical staining of retinal flat-mounts with an antibody against the brain-specific homeobox/POU domain protein 3A (Brn3a).<ol><li>Transfer isolated retinas into a 24-well culture plate (one retina per well) containing 1 mL of 1x PBS and keep the inner retina facing up.</li><li>Permeabilize tissue by washing 3x for 10 min with a non-ionic surfactant 0.5% diluted in 1x PBS (0.3 mL). Then keep the tissue gently shaking in 5% bovine serum albumin (BSA) in non-ionic surfactant 2% and 1x PBS (blocking solution; 0.25 mL) for 60 min at room temperature.</li><li>During step 1.2, prepare the Brn3a primary antibody solution by diluting 1:200 in non-ionic surfactant 0.5% and 1x PBS plus 5% BSA, and store it at 4 &#176;C.</li><li>After 60 min of tissue blocking, incubate retinas in 0.2 mL of primary antibody solution at 4 &#176;C for 72 h with gentle shaking.</li><li>Wash the tissue 3x for 10 min with 1x PBS, then incubate the tissue for 2 h at room temperature in 0.2 mL of the secondary antibody solution diluted 1:750 in 1x PBS plus 5% BSA.</li><li>Further, incubate the tissue for 10 min in nuclear counterstain solution for fluorescent nuclei staining. Conclude immunohistochemistry with a final washing step with 1x PBS (0.3 mL) repeated 3x.</li><li>Transfer retinas with the aid of two small brushes onto glass microscope slides, maintaining the vitreous side up. Position the dorsal retinal quadrant up on the microscope slides. Make two more radial cuts towards the optic nerve head to delimit the other 3 quadrants (nasal, ventral, and temporal). NOTE: The cut dimensions are not fixed. They should not be too short that impairs an efficient flattening of the retina on the slide and should not be too long so that it reaches the optic nerve foramen and completely separates the delimited retinal quadrant from the rest of the tissue.</li><li>Finally, apply 0.2 mL of antifade mounting medium on a glass coverslip and place this onto the flat-mounted retina for tissue microscopic analysis. To estimate RGCs density, examine the flat mounts under a confocal epifluorescence microscope using a 40x/1.3 objective.</li><li>For each quadrant of the retina, take eight photos: two from the central retina (~0.9 mm from optic disc), three from mid-retina (~2.0 mm from optic disc), and three from the peripheral retina (~3.7 mm from optic disc), totaling to 32 photos per retina. Use the FIJI software to count Brn3a-positive cells and estimate the mean cell density.</li></ol>

<figure class='table' style='width:844pt;'><table class='ck-table-resized'><colgroup><col style='width:20.26%;'><col style='width:28.08%;'><col style='width:13.39%;'><col style='width:38.27%;'></colgroup><tbody><tr><td style='border-top-style:none;height:15.5pt;width:171pt;'>DAKO</td><td style='border-left-style:none;border-top-style:none;width:237pt;'>Dako North America</td><td style='border-left-style:none;border-top-style:none;width:113pt;'>S3023</td><td style='border-left-style:none;border-top-style:none;width:323pt;'>Antifade mounting medium</td></tr><tr><td style='border-top-style:none;height:15.5pt;width:171pt;'>LSM 510 Meta</td><td style='border-left-style:none;border-top-style:none;width:237pt;'>Carl Zeiss</td><td style='border-left-style:none;border-top-style:none;width:113pt;'>-</td><td style='border-left-style:none;border-top-style:none;width:323pt;'>Confocal epifluorescence microscope</td></tr><tr><td style='border-top-style:none;height:31.0pt;width:171pt;'>Monoclonal IgG1 mouse anti-Brn3a</td><td style='border-left-style:none;border-top-style:none;width:237pt;'>MilliporeSigma</td><td style='border-left-style:none;border-top-style:none;width:113pt;'>MAB-1585</td><td style='border-left-style:none;border-top-style:none;width:323pt;'>Brn3a primary antibody solution</td></tr><tr><td style='border-top-style:none;height:15.75pt;width:171pt;'>TO-PRO-3</td><td style='border-left-style:none;border-top-style:none;width:237pt;'>Thermo Fisher Scientific</td><td style='border-left-style:none;border-top-style:none;width:113pt;'>T3605</td><td style='border-left-style:none;border-top-style:none;width:323pt;'>Far red-fluorescent nuclear counterstain; emission at 661 nm</td></tr><tr><td style='border-top-style:none;height:15.75pt;width:171pt;'>Triton X-100</td><td style='border-left-style:none;border-top-style:none;width:237pt;'>Sigma-Aldrich</td><td style='border-left-style:none;border-top-style:none;width:113pt;'>9036-19-5</td><td style='border-left-style:none;border-top-style:none;width:323pt;'>Non-ionic surfactant</td></tr><tr><td style='border-top-style:none;height:33.0pt;width:171pt;'>IgG donkey anti-mouse antibody + Alexa Fluor 555</td><td style='border-left-style:none;border-top-style:none;width:237pt;'>Thermo Fisher Scientific</td><td style='border-left-style:none;border-top-style:none;width:113pt;'>A31570</td><td style='border-left-style:none;border-top-style:none;width:323pt;'>Secondary antibody solution</td></tr><tr><td style='border-top-style:none;height:32.0pt;'>DAPI</td><td style='border-left-style:none;border-top-style:none;'>Thermo Fisher Scientific</td><td style='border-left-style:none;border-top-style:none;'>28718-90-3</td><td style='border-left-style:none;border-top-style:none;width:323pt;'>diamidino-2-phenylindole; blue fluorescent nuclear counterstain; emission at 452&#177;3 nm</td></tr></tbody></table></figure>

<a href='https://app.jove.com/v/63442/full-circle-cauterization-limbal-vascular-plexus-for-surgically'>Source: Lani-Louzada, R., et al.&#160; Full-Circle Cauterization of Limbal Vascular Plexus for Surgically Induced Glaucoma in Rodents. J. Vis. Exp. (2022).</a>This video demonstrates the quantification of retinal ganglion cells from chemically fixed rat retinas subjected to full-circle cauterization of the limbal vascular plexus. The process includes permeabilization, antibody staining, and nuclear counterstaining, followed by visualization under an epifluorescence microscope to assess the impact of elevated intraocular pressure on retinal ganglion cell viability.

Source: Lani-Louzada, R., et al.&#160; Full-Circle Cauterization of Limbal Vascular Plexus for Surgically Induced Glaucoma in Rodents. J. Vis. Exp. ...

Take a chemically-fixed retina isolated from a rat's eye.The eye exhibits heat-induced damage to the limbal vascular plexus, a network of blood vessels surrounding the cornea.This damage blocks fluid drainage, increasing intraocular pressure (IOP) and causing retinal ganglion cell (RGC) degeneration.Treat the retina with a permeabilization solution to permeabilize the cell and nuclear membranes.Apply a blocking solution to prevent non-specific antibody binding.Remove the blocking solution.Introduce primary antibodies that target a transcription factor predominantly expressed in RGCs.Wash to remove unbound antibodies.Introduce fluorophore-conjugated secondary antibodies that bind to the primary antibodies.Wash to remove unbound antibodies.Counterstain the nuclei with a DNA-binding dye.Wash the retina and mount it on a glass slide using an appropriate mounting medium.Visualize the retina under an epifluorescence microscope.A reduced cell density in the damaged eye compared to the control confirms RGC degeneration due to increased IOP.

9 Views. Quantification of Retinal Ganglion Cell Somas Following Cauterization-Induced Ocular Hypertension 

Video: Quantification of Retinal Ganglion Cell Somas Following Cauterization-Induced Ocular Hypertension  - Experiment

Experimental Glaucoma Induced by Ocular Injection of Magnetic Microspheres

Progress in understanding the pathophysiology, and providing novel treatments for glaucoma is dependent on good animal models of the disease. We present here a protocol for elevating intraocular pressure (IOP) in the rat, by injecting magnetic microspheres into the anterior chamber of the eye. The use of magnetic particles allows the user to manipulate the beads into the iridocorneal angle, thus providing a very effective blockade of fluid outflow from the trabecular meshwork. This leads to long-lasting IOP rises, and eventually neuronal death in the ganglion cell layer (GCL) as well as optic nerve pathology, as seen in patients with the disease. This method is simple to perform, as it does not require machinery, specialist surgical skills, or many hours of practice to perfect. Furthermore, the pressure elevations are very robust, and reinjection of the magnetic microspheres is not usually required unlike in some other models using plastic beads. Additionally, we believe this method is suitable for adaptation for the mouse eye.

We present a method for inducing elevated intraocular pressure (IOP), by injecting magnetic microspheres into the rat eye, to model glaucoma. This leads to strong pressure rises, and extensive neuronal death. This protocol is easy to perform, does not require repeat injections, and produces stable long-lasting IOP rises.

Progress in understanding the pathophysiology, and providing novel treatments for glaucoma is dependent on good animal models of the disease. We present ...

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Medicine

A Magnetic Microbead Occlusion Model to Induce Ocular Hypertension-Dependent Glaucoma in Mice

The use of rodent models of glaucoma has been essential to understand the molecular mechanisms that underlie the pathophysiology of this multifactorial neurodegenerative disease. With the advent of numerous transgenic mouse lines, there is increasing interest in inducible murine models of ocular hypertension. Here, we present an occlusion model of glaucoma based on the injection of magnetic microbeads into the anterior chamber of the eye using a modified microneedle with a facetted bevel. The magnetic microbeads are attracted to the iridocorneal angle using a handheld magnet to block the drainage of aqueous humour from the anterior chamber. This disruption in aqueous dynamics results in a steady elevation of intraocular pressure, which subsequently leads to the loss of retinal ganglion cells, as observed in human glaucoma patients. The microbead occlusion model presented in this manuscript is simple compared to other inducible models of glaucoma and also highly effective and reproducible. Importantly, the modifications presented here minimize common issues that often arise in occlusion models. First, the use of a bevelled glass microneedle prevents backflow of microbeads and ensures that minimal damage occurs to the cornea during the injection, thus reducing injury-related effects. Second, the use of magnetic microbeads ensures the ability to attract most beads to the iridocorneal angle, effectively reducing the number of beads floating in the anterior chamber avoiding contact with other structures (e.g., iris, lens). Lastly, the use of a handheld magnet allows flexibility when handling the small mouse eye to efficiently direct the magnetic microbeads and ensure that there is little reflux of the microbeads from the eye when the microneedle is withdrawn. In summary, the microbead occlusion mouse model presented here is a powerful investigative tool to study neurodegenerative changes that occur during the onset and progression of glaucoma.

Here, we present a protocol to induce ocular hypertension in the murine eye that results in the loss of retinal ganglion cells as observed in glaucoma. Magnetic microbeads are injected into the anterior chamber and attracted to the iridocorneal angle using a magnet to block the outflow of aqueous humour.

The use of rodent models of glaucoma has been essential to understand the molecular mechanisms that underlie the pathophysiology of this multifactorial ...

A Model of Glaucoma Induced by Circumlimbal Suture in Rats and Mice

The circumlimbal suture is a technique for inducing experimental glaucoma in rodents by chronically elevating intraocular pressure (IOP), a well-known risk factor for glaucoma. This protocol demonstrates a step-by-step guide on this technique in Long Evans rats and C57BL/6 mice. Under general anesthesia, a "purse-string" suture is applied on the conjunctiva, around the equator and behind the limbus of the eye. The fellow eye serves as an untreated control. Over the duration of our study, which was a period of 8 weeks for rats and 12 weeks for mice, IOP remained elevated, as measured regularly by rebound tonometry in conscious animals without topical anesthesia. In both species, the sutured eyes showed electroretinogram features consistent with preferential inner retinal dysfunction. Optical coherence tomography showed selective thinning of the retinal nerve fiber layer. Histology of the rat retina in cross-section found reduced cell density in the ganglion cell layer, but no change in other cellular layers. Staining of flat-mounted mouse retinae with a ganglion cell specific marker (RBPMS) confirmed ganglion cell loss. The circumlimbal suture is a simple, minimally invasive and cost-effective way to induce ocular hypertension that leads to ganglion cell injury in both rats and mice.

Chronic ocular hypertension is induced by applying a circumlimbal suture in rats and mice, leading to functional and structural deterioration of the retinal ganglion cells consistent with glaucoma.

The circumlimbal suture is a technique for inducing experimental glaucoma in rodents by chronically elevating intraocular pressure (IOP), a well-known ...

Quantification of Retinal Ganglion Cell Somas Following Cauterization-Induced Ocular Hypertension

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Quantification of Retinal Ganglion Cell Somas Following Cauterization-Induced Ocular Hypertension