Name: identifying kinase inhibitors that modulate the thymocyte response to strong tcr signals
Uploaded: 2023-08-31T09:44:29.000+00:00
Duration: 2 min 2 s
Description: Source: Chen, E. W., et al. Identification of Mediators of T-cell Receptor Signaling via the Screening of Chemical Inhibitor Libraries. J. Vis. Exp. ...

identifying kinase inhibitors that modulate the thymocyte response to strong tcr signals

Identifying Kinase Inhibitors that Modulate the Thymocyte Response to Strong TCR Signals

To begin the treatment of thymocytes with kinase inhibitors, use a multi-channel pipette to add 40 microliters per well of thymocytes to a small-volume plate. Put the plate on ice. Then, pipette one part of kinase inhibitors, DMSO, and dexamethasone, and four parts of the complete RPMI media into a 96-well plate.
Designate eight wells of the small-volume plate to untreated controls, four wells to dexamethasone-treated positive controls for cell death, by adding the diluted dexamethasone at the 5-micromolar concentration, and four wells to vehicle-treated controls by adding 0.5 microliters of the diluted DMSO. Next, from the corresponding wells of the inhibitor plate, add 0.5 microliters of each diluted inhibitor to the 96-well plate.
To begin thymocytes&#39; stimulation, first, make sure anti-CD3 and CD28 beads are uniformly resuspended. Next, wash 1 milliliter of the beads with 2 milliliters of the PBS buffer. Put the tube on a magnetic stand to separate beads from supernatant, and aspirate the solution. Then, resuspend the beads in 1 milliliter of the complete RPMI medium.
Add 10 microliters per well of the bead suspension to each inhibitor-treated sample, the four DMSO-treated samples, and four of the 8 untreated samples. Add 10 microliters of the complete RPMI to the remaining four untreated wells.
Use a microplate orbital shaker to gently agitate the plate. Next, incubate the thymocytes in 37 degrees Celsius and 5% carbon dioxide environment for 17 to 20 hours or overnight.
Prime an automated laminar flow plate washer, first, with 150 milliliters of ethanol-Tween solution, then, with deionized water supplemented with 1% Tween-20, and finally, with FACS wash buffer. At the end of the incubation, using the plate washer system, wash the plate with FACS wash buffer using a nine times washing cycle. Each wash adds and removes 55 microliters of wash buffer by laminar flow, resulting in exponential dilution of the reagents in the wells.
To stain surface antigens, first, dilute one unit volume of anti-CD3, anti-CD4, anti-CD8, and anti-CD69 antibodies in 100 unit volumes of the FACS wash buffer. Then, resuspend the cells in 25 microliters of the staining antibody mixture. Use a microplate orbital shaker to gently agitate the plate, and then leave the plate on ice for 30 minutes.
To fix the cells, first, wash the plate with 55 microliters of FACS wash buffer using nine times washing cycle as described before. Then, add 50 microliters of the fixation and permeabilization buffer to each well. Mix well, and incubate the plate on ice for 30 minutes. After the incubation, prepare a 1x perm/wash buffer by diluting 25 milliliters of the provided 10x stock in 225 milliliters of ultra-pure water.
Prime the plate washer with 1x buffer, and wash the plate with 55 microliters of the 1x buffer using a nine times washing cycle as described before. Mix 1 milliliter of the anti-caspase-3 antibody with 2 milliliters of the 1x perm and wash buffer. Add 25 microliter per well of the mixture to the fixed cells.
Use a microplate orbital shaker to gently agitate the plate. Leave the plate on ice for an hour. At the end of incubation, repeat the wash step, nine times with the 1x perm and wash buffer. Then, add 25 microliters of the FACS wash buffer to all wells of the plate, pipette up and down a few times to mix the solution.
Finally, transfer the mixed samples into microtiter tubes. Top up the tubes with the FACS wash buffer to a total volume of 200 microliters and proceed to the flow cytometry analysis.

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1. Kinase Inhibitor Library Screening (Centrifuge-independent Assay)
<ol>
	<li>Treatment of thymocytes with kinase inhibitors
	<ol>
		<li>Prepare a thymocyte suspension.</li>
		<li>Dilute the thymocytes in complete RPMI to obtain a thymocyte suspension of 25 x 106 cells/mL.</li>
		<li>Add 40 &#956;L of thymocytes to each well of a small-volume plate, using a multichannel pipette. Place the plate on ice.</li>
		<li>Dilute the inhibitors from the stock plate, DMSO, and dexamethasone in complete RPMI at a ratio of four parts of complete RPMI to one part of inhibitor/DMSO/dexamethasone (dilution factor of 5). 
		NOTE: As the volumes used in this small-volume plate are 5x smaller than in the conventional method, the inhibitors and the control reagents are diluted fivefold before adding them to the thymocytes in the plate.</li>
		<li>Add 0.5 &#956;L of kinase inhibitors to the 96-well plate from the corresponding wells of the inhibitor plate prepared in step 1.1.4.</li>
		<li>Prepare eight wells of untreated controls. Prepare four wells of vehicle-treated controls by adding 0.5 &#956;L of the DMSO prepared in step 1.1.4. Prepare four wells of 5 &#956;M dexamethasone-treated controls, using the diluted dexamethasone prepared in step 1.1.4 (Figure 1).</li>
	</ol>
	</li>
</ol>
2. Stimulation of thymocytes using anti-CD3/CD28 beads
<ol>
	<li>Make sure that the beads are uniformly resuspended. Take 1 mL of beads and wash them with 2 mL of PBS. Separate the beads using a magnetic stand and aspirate the solution. Resuspend the beads in 1 mL of complete RPMI. 
	NOTE: The ratio of beads to cells is 1 to 2.5. Adjust the amount of beads, depending on the number of wells to stimulate and the number of thymocytes used.</li>
	<li>Add 10 &#956;L of bead suspension to each inhibitor-treated sample, the four DMSO-treated samples, and four of the eight untreated samples. Add 10 &#956;L of complete RPMI to the remaining four untreated wells. Figure 1 shows the general plate layout. 
	NOTE: The final volume of the wells is 50 &#956;L, which is within the maximum capacity of the wells. It is important to exercise caution and to hold the plates upright, to avoid cross-well spillage.</li>
	<li>To mix, agitate the plate using a microplate orbital shaker. Alternatively, mix the contents of the wells using a multichannel pipette.</li>
	<li>Incubate the thymocytes in a 37 &#176;C, 5% CO2 incubator for 17 - 20 h (or overnight) with an anti-evaporation lid.</li>
</ol>
3. Setup of the plate washer
NOTE: The instructions for setting up the plate washer are provided by the manufacturer. The steps are mentioned in brief below. Roughly 150 mL of solution is needed for each priming step.
<ol>
	<li>Prime the wash system with 70% ethanol containing 1% Tween 20.</li>
	<li>Prime the wash system with deionized water containing 1% Tween 20.</li>
	<li>Prime the wash system with FACS wash buffer.</li>
</ol>
4. Staining of surface antigens
<ol>
	<li>Prepare an antibody staining mixture containing anti-TCR&#946;, anti-CD4, anti-CD8, and anti-CD69 antibodies. Dilute the antibodies in FACS wash buffer at a ratio of 1:100 (v/v).</li>
	<li>Wash the plate 9x, using 55 &#956;L of FACS wash buffer per wash, using the automated laminar flow washing system. 
	NOTE: At the end of the washes, there will be 25 &#956;L of residual volume in each well.</li>
	<li>Resuspend the cells in 25 &#956;L of the staining antibody mixture prepared in step 1.4.1.</li>
	<li>If the samples are transferred from a 96-well plate, resuspend the cells in 50 &#956;L of the antibody mixture, and transfer the samples to the small-volume plate. This step corresponds to method number 2, as depicted in Figure 2A.</li>
	<li>To mix, agitate the plate with a microplate orbital shaker or mix the samples using a multichannel pipette, and incubate on ice for 30 min.</li>
</ol>
5. Fixation of cells
<ol>
	<li>Wash the plate 9x, using 55 &#956;L of FACS wash buffer per wash, using the automated laminar flow washing system.</li>
	<li>Add fixation/permeabilization buffer (comes with the active caspase-3 apoptosis kit; same with the 10x perm/wash buffer mentioned in step 1.6.1 and the anti-caspase-3 antibody in step 1.6.2) at 50 &#956;L per well.</li>
	<li>Incubate on ice for 30 min.</li>
</ol>
6. Intracellular staining for active caspase 3
<ol>
	<li>Prepare 1x perm/wash buffer by diluting 25 mL of 10x perm/wash buffer in 225 mL of ultrapure water.</li>
	<li>Prepare intracellular active caspase stain by adding 1 mL of anti-caspase-3 antibody to 2 mL of 1x perm/wash buffer. The ratio of antibody to perm/wash buffer is 1:2.</li>
	<li>Prime the wash system with 1x perm/wash buffer.</li>
	<li>Wash the plate 9x with 1x perm/wash buffer, at 55 &#956;L for each wash.</li>
	<li>Add 25 &#956;L of the intracellular caspase stain prepared in step 1.6.2 to all wells.</li>
	<li>To mix, agitate the plate with a microplate orbital shaker or mix the samples using a multichannel pipette, and incubate on ice for 1 h.</li>
	<li>Wash the plate 9x with 1x perm/wash buffer, at 55 &#956;L for each wash.</li>
	<li>Add 25 &#956;L of FACS wash buffer to all wells.</li>
	<li>Transfer the samples to microtiter tubes after adequate mixing via pipetting.</li>
	<li>Add another 50 &#956;L of FACS wash buffer to the empty wells and repeat step 1.6.9.</li>
	<li>Repeat steps 1.6.9 and 1.6.10 2x until 200 &#956;L of the samples are collected in the microtiter tubes. 
	NOTE: The purpose of the procedures described in steps 1.6.10 and 1.6.11 is to ensure maximum recovery of the cells from the small-volume plate. If cell numbers are not a concern, after step 1.6.10, simply top up the microtiter tubes to 200 &#956;L with FACS wash buffer.</li>
	<li>Run a flow cytometric analysis of the samples and analyze the results with a FACS analysis program. Caspase-3 activation and CD69 expression are analyzed in the gate containing CD4+CD8+DP thymocytes.</li>
</ol>

Source: Chen, E. W., et al. <a href="https://appjove.unicartagenaproxy.elogim.com/v/58946">Identification of Mediators of T-cell Receptor Signaling via the Screening of Chemical Inhibitor Libraries.</a> J. Vis. Exp. (2019).
In this video, we describe a method to identify the small-molecule kinase inhibitors that modulate the apoptosis of self-reactive CD4+CD8+ double-positive immature thymocytes. Apoptosis is induced in the double-positive thymocytes by activating them with anti-CD3- and anti-CD28-coated magnetic beads; this is followed by a small-molecule inhibitor treatment and flow cytometry analysis to detect if the inhibitors modulate the apoptotic marker expression.

<img alt="Figure 1" src="/files/ftp_upload/21605/21605_Figure1.jpg" /> 
Figure 1: Plate layout of the thymocyte activation assay. (Top) Columns 1 and 12 are reserved for controls, while columns 2 to 11 are inhibitor-treated samples (beige). The negative control (nonstimulated [NS]; grey) occupies wells A1 to D1, and the positive control for cell death (dexamethasone-treated [DEX]; purple) occupies wells E1 to H1. Columns 2 to 12 contain thymocytes stimulated with anti-CD3/CD28 beads. The positive co...

Source: Chen, E. W., et al. Identification of Mediators of T-cell Receptor Signaling via the Screening of Chemical Inhibitor Libraries. J. Vis. Exp. ...

Begin with mice thymocyte cells in a multi-well plate. Add magnetic beads coated with anti-CD3 and anti-CD28 antibodies. To a subset of wells, add an appropriate concentration of the test kinase inhibitor. Incubate.
The antibodies bind to the cell-surface CD3 and CD28 receptors on the double-positive thymocytes and activate them, causing downregulation of T cell receptors, TCRs, and activation of cytosolic protein kinase.&#160;
These protein kinases activate downstream signaling pathways, leading to increased cell-surface CD69 expression and cytosolic caspase-3 activation. Activated caspase-3 cleaves essential cellular proteins &#8212; initiating thymocyte apoptosis.
In cells treated with the kinase inhibitor, the inhibitors block the cytosolic kinases, modulating CD69 expression and caspase-3 activation.
Pipette in a fluorophore-tagged antibody cocktail that binds to the thymocytes&#39; TCR, CD4, and CD8 co-receptors, and CD69 receptors. Treat the thymocytes with a buffer to fix and permeabilize them.
Incubate with a fluorophore-tagged anti-caspase-3 antibody that binds to cytosolic caspase-3. Analyze the thymocytes using flow cytometry.
Control double-positive thymocytes express the fluorescent cell-surface markers CD4, CD8, and CD69 and intracellular caspase-3 and show TCR downregulation. In contrast, inhibitor-treated thymocytes exhibit lower levels of fluorescent CD69 and caspase-3.

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Identifying Kinase Inhibitors that Modulate the Thymocyte Response to Strong TCR Signals

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Identifying Kinase Inhibitors that Modulate the Thymocyte Response to Strong TCR Signals