eoe sub articles

EoE Sub Articles

1. Preparation of poly-L-lysine coverslips
<ol>
	<li>Before the B cell activation assay with Ag-coated beads, prepare poly-L-lysine-coated coverslips (PLL-coverslips). Use a 50 mL tube containing 40 mL of 0.01% w/v of PLL solution and immerse the 12 mm-diameter coverslips into the solution. Rotate overnight at RT.</li>
	<li>Wash the coverslips with 1xPBS and leave to dry on a 24-well plate lid covered with paraffin film. Proceed with B cell activation.</li>
</ol>
2. B cell activation on antigen-coated coverslips
<ol>
	<li>Preparation of antigen-coated coverslips
	<ol>
		<li>Before activation, prepare the antigen solution (1x PBS containing 10 &#181;g/mL BCR-ligand+ and 0.5 &#181;g/mL rat anti-mouse CD45R/B220).</li>
		<li>NOTE: Consider preparing the coverslips the day before the assay. B220 improves B cell adhesion, however, the BCR-Ligand+ is sufficient to generate the spreading response.</li>
		<li>Place the 12 mm coverslip onto a 24-well plate lid covered with paraffin film, add 40 &#181;L of antigen solution onto each coverslip, and incubate at 4 &#176;C overnight. Seal the plate to avoid evaporation of antigen solution.</li>
		<li>Wash the coverslips with 1x PBS and air dry.</li>
	</ol>
	</li>
	<li>B cell activation
	<ol>
		<li>To start the activation, dilute IIA1.6 B cells to 1.5 x 106 cells/mL in CLICK medium + 5% FBS.</li>
		<li>Add 100 &#181;L of cells onto an antigen-coated coverslip (Ag-coverslip) and activate for different time points in a cell incubator at 37 &#176;C / 5% CO2. The typical activating time points are 0, 30, and 60 min. 
		NOTE: As in section 1, we recommend starting with the longest activating time point in order to fix all the samples at the same time.</li>
		<li>For time 0, place the 24-well plate lid containing the Ag-coverslip on ice and add the cells. Incubate for 5 min on ice.</li>
		<li>Carefully aspirate the media on each Ag-coverslip and then add 100 &#181;L of cold 1x PBS to stop the activation.</li>
	</ol>
	</li>
</ol>

<table border="1" fo:keep-together.within-page="1" fo:keep-with-next.within-page="always">
	<tbody>
		<tr>
			<td>IIA1.6 (A20 variant) mouse B-lymphoma cells</td>
			<td>ATCC</td>
			<td>TIB-208</td>
			<td>Murine B-cell lymphoma of Balb/c origin that expresses an IgG-containing BCR on its surface without Fc&#947;IIR</td>
		</tr>
		<tr>
			<td>CaCl2</td>
			<td>Winkler</td>
			<td>CA-0520</td>
			<td></td>
		</tr>
		<tr>
			<td>Glycine</td>
			<td>Winkler&#160;</td>
			<td>BM-0820</td>
			<td></td>
		</tr>
		<tr>
			<td>HyClone Fetal bovine serum</td>
			<td>Thermo Fisher Scientific</td>
			<td>SH30071.03</td>
			<td>Heat inactivate at 56 C for 30 min</td>
		</tr>
		<tr>
			<td>KCl</td>
			<td>Winkler</td>
			<td>PO-1260</td>
			<td></td>
		</tr>
		<tr>
			<td>NaCl</td>
			<td>Winkler</td>
			<td>SO-1455</td>
			<td></td>
		</tr>
		<tr>
			<td>Parafilm</td>
			<td>M</td>
			<td>P1150-2</td>
			<td></td>
		</tr>
		<tr>
			<td>Penicillin-Streptomycin</td>
			<td>Thermo Fisher Scientific</td>
			<td>15140122</td>
			<td>Liquid</td>
		</tr>
		<tr>
			<td>Poly-L-Lysine</td>
			<td>Sigma</td>
			<td>P8920</td>
			<td>Dilute with sterile water</td>
		</tr>
		<tr>
			<td>RPMI-1640</td>
			<td>Biological Industries</td>
			<td>01-104-1A</td>
			<td></td>
		</tr>
		<tr>
			<td>Sodium pyruvate</td>
			<td>Thermo Fisher Scientific</td>
			<td>11360070</td>
			<td></td>
		</tr>
		<tr>
			<td>Tube 50 ml</td>
			<td>Corning</td>
			<td>353043</td>
			<td></td>
		</tr>
		<tr>
			<td>2-mercaptoethanol</td>
			<td>Thermo Fisher Scientific</td>
			<td>21985023</td>
			<td></td>
		</tr>
		<tr>
			<td>Glutamine</td>
			<td>Thermo Fisher Scientific</td>
			<td>35050061</td>
			<td></td>
		</tr>
		<tr>
			<td>Goat-anti-mouse IgG antibody</td>
			<td>Jackson ImmunoResearch</td>
			<td>315-005-003</td>
			<td>IIA1.6 positive ligand</td>
		</tr>
	</tbody>
</table>

b cell activation on an antigen-coated coverslip

Source: Iba&#241;ez-Vega, J., et al., <a href="https://app.jove.com/v/59621">Studying Organelle Dynamics in B Cells During Immune Synapse Formation.</a> J. Vis. Exp. (2019)
This video demonstrates B cell activation in vitro. The process involves antigen interaction with B cell receptors, leading to cytoskeleton remodeling, immune synapse formation, lysosome movement, antigen internalization, processing, and subsequent presentation on MHC molecules for B cell activation.

B Cell Activation on an Antigen-Coated Coverslip

Source: Iba&#241;ez-Vega, J., et al., Studying Organelle Dynamics in B Cells During Immune Synapse Formation. J. Vis. Exp. (2019)
This video demonstrates ...

B cell activation involves the recognition of antigens by B cell receptors, BCRs, on their surface to elicit an immune response.
To study B cell activation in vitro, begin with a coverslip containing antigens and anti-CD45R antibodies, immobilized over a polymeric material. The negatively-charged antigens and antibodies interact with positively-charged polymers on the coverslip through electrostatic interactions.
Overlay the coated coverslips with a medium containing B cells and incubate. The CD45R &#8212; the transmembrane protein of B cells &#8212; interacts with the immobilized antibodies, facilitating cell adhesion.
The BCRs on the adhered B cell interact with an antigen, forming an immune synapse &#8212; the coordination region for cell signaling and antigen internalization. This promotes cytoskeleton remodeling and initiates cell spreading, which increases the cell surface in contact with the antigens.
Further remodeling causes the movement of BCR-coupled antigens toward the center of the immune synapse. This cellular rearrangement causes the repositioning of the centrosome near the synaptic membrane that guides intracellular organelles, including lysosomes, toward the synapse.
The fusion of lysosomes with the membrane leads to the internalization of the antigen-BCR complexes. The internalized antigens are processed into peptide fragments, loaded onto class-II major histocompatibility complex or MHC molecules, and finally presented on activated B cells.

b-cell-activation-on-an-antigen-coated-coverslip

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JoVE Encyclopedia of Experiments

Immunology

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235 Views. Źródło: Ibañez-Vega, J., et al., Badanie dynamiki organelli w komórkach B podczas tworzenia synaps immunologicznych. J. Vis. Exp. (2019 rok) Ten film pokazuje aktywację limfocytów B in vitro. Proces ten obejmuje interakcję antygenu z receptorami komórek B, prowadzącą do przebudowy cytoszkieletu, tworzenia synaps immunologicznych, ruchu lizosomów, internalizacji antygenu, przetwarzania, a następnie prezentacji na cząsteczkach MHC w celu aktywacji komórek B. 

Video: Aktywacja limfocytów B na szkiełku nakrywkowym pokrytym antygenem - Concept

In Vitro Differentiation Model of Human Normal Memory B Cells to Long-lived Plasma Cells

Plasma cells (PCs) secrete large amounts of antibodies and develop from B cells that have been activated. PCs are rare cells located in the bone marrow or mucosa and ensure humoral immunity. Due to their low frequency and location, the study of PCs is difficult in human. We reported a B to PC in vitro differentiation model using selected combinations of cytokines and activation molecules that allow to reproduce the sequential cell differentiation occurring in vivo. In this in vitro model, memory B cells (MBCs) will differentiate into pre-plasmablasts (prePBs), plasmablasts (PBs), early PCs and finally, into long-lived PCs, with a phenotype close to their counterparts in healthy individuals.&#160;We also built an open access bioinformatics tools to analyze the most prominent information from GEP data related to PC differentiation. These resources can be used to study human B to PC differentiation and in the current study, we investigated the gene expression regulation of epigenetic factors during human B to PC differentiation.

Using multi-step culture systems, we report an in vitro B cell to plasma cell differentiation model.

Plasma cells (PCs) secrete large amounts of antibodies and develop from B cells that have been activated. PCs are rare cells located in the bone marrow or ...

JoVE Journal

Immunology and Infection

Flow Cytometric Characterization of Murine B Cell Development

Extensive studies have characterized the development and differentiation of murine B cells in secondary lymphoid organs. Antibodies secreted by B cells have been isolated and developed into well-established therapeutics. Validation of murine B cell development, in the context of autoimmune prone mice, or in mice with modified immune systems, is a crucial component of developing or testing therapeutic agents in mice and is an appropriate use of flow cytometry. Well established B cell flow cytometric parameters can be used to evaluate B cell development in the murine peritoneum, bone marrow, and spleen, but a number of best practices must be adhered to. In addition, flow cytometric analysis of B cell compartments should also complement additional readouts of B cell development. Data generated using this technique can further our understanding of wild type, autoimmune prone mouse models as well as humanized mice that can be used to generate antibody or antibody-like molecules as therapeutics.

We describe herein a simple analysis of the heterogeneity of the murine immune B cell compartment in the peritoneum, spleen, and bone marrow tissues by flow cytometry. The protocol can be adapted and extended to other mouse tissues.

Extensive studies have characterized the development and differentiation of murine B cells in secondary lymphoid organs. Antibodies secreted by B cells ...

Flow Cytometry-Based Quantification and Analysis of Myocardial B-Cells

A growing body of evidence shows that B-lymphocytes play an important role in the context of myocardial physiology and myocardial adaptation to injury. However, the literature reports contrasting data on the prevalence of myocardial B-cells. B-cells have been reported to be both among the most prevalent immune cells in the rodent heart or to be present, but at a markedly lower prevalence than myeloid cells, or to be quite rare. Similarly, several groups have described that the number of myocardial B-cells increases after acute ischemic myocardial injury, but one group reported no changes in the number of B-cells of the injured myocardium. Implementation of a shared, reproducible method to assess the prevalence of myocardial B-cells is critical to harmonize observations from different research groups and thus promote the advancement of the study of B-cell myocardial interactions. Based on our experience, the seemingly contrasting observations reported in the literature likely stem from the fact that murine myocardial B-cells are mostly intravascular and connected to the microvascular endothelium. Therefore, the number of B-cells recovered from a murine heart is exquisitely sensitive to the perfusion conditions used to clean the organ and to the method of digestion used. Here we report an optimized protocol that accounts for these two critical variables in a specific way. This protocol empowers reproducible, flow cytometry-based analysis of the number of murine myocardial B-cells and allows researchers to distinguish extravascular vs. intravascular myocardial B-cells.

Here we report a protocol for the quantification and differentiation of myocardial B-lymphocytes based on their location in the intravascular or endothelial space using flow cytometry.

A growing body of evidence shows that B-lymphocytes play an important role in the context of myocardial physiology and myocardial adaptation to injury. ...

B Cell Activation on an Antigen-Coated Coverslip

Transkrypcja

B Cell Activation on an Antigen-Coated Coverslip