Prolonged Antigen Persistence Within Nonterminal Late Endocytic Compartments of Antigen-Specific B Lymphocytes

Gondré-Lewis, Timothy; Moquin, Amy; Drake, James R.

doi:10.4049/jimmunol.166.11.6657

Cited by 45 publications

(75 citation statements)

References 28 publications

(40 reference statements)

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“…4 M, there was no significant depletion of b-hex activity during the first 15 min of the assay in untreated cells, consistent with a lack of Ag trafficking in b-hex-positive compartments early after internalization [30]. In agreement with our previous report [29], in signaling-competent cells Ag causes depletion of b-hex activity more prominently after 30 min. However, treatment of cells with Src kinase trafficking of Ag-BCR complexes to processing compartments as suggested by earlier studies.…”

Section: Resultssupporting

confidence: 92%

“…Due to the altered distribution of internalized Ag observed in cells pretreated with PP1 and PP2 (Fig. 4), we determined the effect of inhibition of BCR signaling on the trafficking of HRP-labeled Ag to b-hexosaminidase (b-hex)-positive late endocytic compartments using an HRP-catalyzed 3,3 0 -diaminobenzidine (DAB)-mediated protein cross-linking approach [29]. As a control, the depletion of a-mannosidase, a marker enzyme present in the Golgi complex which is not accessed by the BCR, was also measured.…”

Section: Resultsmentioning

confidence: 99%

“…Ag-BCR complexes were then allowed to internalize at 37 C for 15 or 30 min (in the continued presence of vehicle or inhibitors). Cells were then allowed to bind to alcian blue-treated coverslips, fixed and permeabilized (or not) as previously described [29]. Subsequently, cells were stained with SA-Alexa 594 (Molecular Probes) followed by mouse anti-B220-FITC (Southern Biotechnology).…”

Section: Immunofluorescence Microscopymentioning

confidence: 99%

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Functional and structural requirements for the internalization of distinct BCR‐ligand complexes

et al. 2006

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Antigen (Ag) binding to the BCR rapidly initiates two important events: a phosphorylation cascade that results in the production of secondary signaling intermediaries and the internalization of Ag-BCR complexes. Previous studies using anti-BCR antibodies (Ab) have suggested that BCR signaling is an essential requirement for BCR endocytosis and have further implicated lipid rafts as essential platforms for both BCR functions. However, published data from our laboratory indicate that lipid rafts and consequently raft-mediated signaling are dispensable for BCR-mediated internalization of Ag-specific BCR. Therefore, we investigated the relationship between BCR signaling and endocytosis by defining the role of early kinase signaling in the BCRmediated internalization of a model Ag (haptenated protein). The results demonstrate that Src kinases and Syk-mediated BCR signaling are not essential for BCR-mediated Ag internalization. Moreover, by comparing Ag and Ab, it was determined that while both localize to clathrin-coated pits, the internalization of Ab-BCR complexes is more susceptible to inhibition of signaling and highly sensitive to disruption of lipid rafts and the actin cytoskeleton compared to Ag-BCR complexes. Thus, these results demonstrate that the nature of the ligand ultimately determines the functional requirements and relative contribution of lipid rafts and other membrane structures to the internalization of BCR-ligand complexes.

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Section: Resultssupporting

confidence: 92%

Section: Resultsmentioning

confidence: 99%

Section: Immunofluorescence Microscopymentioning

confidence: 99%

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Functional and structural requirements for the internalization of distinct BCR‐ligand complexes

et al. 2006

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“…Flow Cytometric Antigen Processing and Presentation AssayFlow cytometric analysis of HEL 46 -61 -I-A k expression was done as reported previously (16,18,(27)(28)(29), except for the following modifications. Splenocytes from either MD4.B10.Br or B10.Br mice were pretreated with inhibitors (4-amino-5-(4-methylphenyl)-7-(t-butyl) pyrazolo [3,4- Cells were infected with lentiviral particles at 37°C with constant inversion for 30 min and returned to culture in complete media to allow viral integration for 48 h. After 48 h, flow cytometric analysis confirmed a transfection efficiency of 8 -15% on the basis of GFP expression.…”

Section: Methodsmentioning

confidence: 99%

“…Ag⅐BCR complexes were then allowed to internalize at 37°C for 0 -60 min. Cells were attached to Alcian blue-treated coverslips, fixed, and permeabilized (or not) as described previously (29). For staining of the LAMP-2 positive compartment, cells were permeabilized in 0.01% saponin and stained with anti-LAMP-2 (1:100) and anti-rat IgG (HϩL) Alexa Fluor 647.…”

Section: Methodsmentioning

confidence: 99%

The Syk-binding Ubiquitin Ligase c-Cbl Mediates Signaling-dependent B Cell Receptor Ubiquitination and B Cell Receptor-mediated Antigen Processing and Presentation

Katkere

Rosa

Drake

2012

Journal of Biological Chemistry

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Background: c-Cbl associates with various signaling molecules to regulate diverse signaling networks via ubiquitination of receptors and/or protein tyrosine kinases. Results: c-Cbl drives ubiquitin-dependent Ag⅐BCR trafficking to MIIC and BCR-mediated antigen processing and presentation. Conclusion: c-Cbl directs BCR-mediated antigen processing and presentation. Significance: c-Cbl coordinates antigen-induced BCR signaling and rapid BCR-mediated antigen processing and presentation to drive a strong humoral immune response.

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The preferential ability of B lymphocytes to act as diabetogenic APC in NOD mice depends on expression of self-antigen-specific immunoglobulin receptors

et al. 2002

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B lymphocytes partially contribute to autoimmune type 1 diabetes (T1D) as a subset of APC with a preferential ability to trigger pathogenic CD4 T cells. We hypothesized that this resulted fromthe unique ability of B lymphocytes to take up pancreatic β cell proteins through Ig mediated capture. T1D was significantly delayed, but not prevented, in a NOD stock in which the B lymphocyteIg repertoire was strongly restricted because of the allelic exclusion induced by transgenic Ig molecules specific for the disease irrelevant hen egg lysozyme (HEL) protein (NOD.IgHEL mice). However, introducing the Igμnull mutation to eliminate the small residual numbers of non‐transgenic B lymphocytes in the NOD.IgHEL stock strongly suppressed T1D to the same low levels that characterize B lymphocyte deficient NOD.Igμnull mice. In contrast to standard NOD mice, both the NOD.IgHEL.Igμnull and NOD.Igμnull stocks were unable to generate T cell responses against the candidate diabetes autoantigen, glutamic acid decarboxylase. These results indicate that Ig‐mediated capture of β cell autoantigens accounts for why B lymphocytes have a greater capacity than other APC subtypes to trigger diabetogenic T cells. Hence, defects in B lymphocyte, as well as T lymphocyte, tolerance induction mechanisms may contribute to T1D in NOD mice.

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Prolonged Antigen Persistence Within Nonterminal Late Endocytic Compartments of Antigen-Specific B Lymphocytes

Cited by 45 publications

References 28 publications

Functional and structural requirements for the internalization of distinct BCR‐ligand complexes

Functional and structural requirements for the internalization of distinct BCR‐ligand complexes

The Syk-binding Ubiquitin Ligase c-Cbl Mediates Signaling-dependent B Cell Receptor Ubiquitination and B Cell Receptor-mediated Antigen Processing and Presentation

The preferential ability of B lymphocytes to act as diabetogenic APC in NOD mice depends on expression of self-antigen-specific immunoglobulin receptors

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