Identification of a novel surface protein on activated CD4+ T cells that induces contact-dependent B cell differentiation (help).

Lederman, Seth; Yellin, Michael; Krichevsky, Alexander; Belko, John; Lee, Julie J.; Chess, Leonard

doi:10.1084/jem.175.4.1091

Cited by 328 publications

(204 citation statements)

References 81 publications

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“…We verified that all mutant CD4OLs were expressed and indirectly assessed their structural integrity by immunoprecipitation of detergent lysates from metabolically labeled cells with polyclonal antibodies directed against synthetic peptides corresponding to the N-and C-terminal portion of CD4OL (Hsu et al, 1997), or with the anti-CD4OL mAb 5c8 (Fig. 7), which can block CI)rU)/CD40L-mediated signaling (Lederman et al, 1992;Yellin et al, 1994). Cell surface expression of CD4OL of selected mutants positive for 5c8 binding was verified by FACS staining of intact assayed by binding to the N-and C-terminal-specific antisera (Table 1).…”

Section: Mutagenesis Of Cd40-ig and Cd4olmentioning

confidence: 81%

The role of polar interactions in the molecular recognition of CD40L with its receptor CD40

et al. 1998

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CD40 Ligand (CD40L) is transiently expressed on the surface of T-cells and binds to CD40, which is expressed on the surface of B-cells. This binding event leads to the differentiation, proliferation, and isotype switching of the B-cells. The physiological importance of CD40L has been demonstrated by the fact that expression of defective CD40L protein causes an immunodeficiency state characterized by high IgM and low IgG serum levels, indicating faulty T-cell dependent B-cell activation. To understand the structural basis for CD40L/CD40 association, we have used a combination of molecular modeling, mutagenesis, and X-ray crystallography. The structure of the extracellular region of CD4OL was determined by protein crystallography, while the CD40 receptor was built using homology modeling based upon a novel alignment of the TNF receptor superfamily, and using the X-ray structure of the TNF receptor as a template. The model shows that the interface of the complex is composed of charged residues, with CD4OL presenting basic side chains (K143, R203, R207), and CD40 presenting acidic side chains (D84, El 14, E l 17). These residues were studied experimentally through site-directed mutagenesis, and also theoretically using electrostatic calculations with the program Delphi. The mutagenesis data explored the role of the charged residues in both CD40L and CD40 by switching to Ala (K143A, R203A, R207A of CD40L, and E74A, D84A, El14A, E l 17A of CD40), charge reversal (K143E, R203E, R207E of CD40L, and D84R, E l 14R, El 17R of CD40), mutation to a polar residue (K143N, R207N, R207Q of C340L, and D84N, E l 17N of CD40), and for the basic side chains in CD40L, isosteric substitution to a hydrophobic side chain (R203M, R207M). All the charge-reversal mutants and the majority of the Met and Ala substitutions led to loss of binding, suggesting that charged interactions stabilize the complex. This was supported by the Delphi calculations which confirmed that the CD40/CD40L residue pairs E74-R203, D84-R207, and El 17-R207 had a net stabilizing effect on the complex. However, the substitution of hydrophilic side chains at several of the positions was tolerated, which suggests that although charged interactions stabilize the complex, charge per se is not crucial at all positions. Finally, we compared the electrostatic surface of TNFjTNFR with CD40L/CD40 and have identified a set of polar interactions surrounded by a wall of hydrophobic residues that appear to be similar but inverted between the two complexes.

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Section: Mutagenesis Of Cd40-ig and Cd4olmentioning

confidence: 81%

The role of polar interactions in the molecular recognition of CD40L with its receptor CD40

et al. 1998

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“…Other more complex steps in B cell development, such as germinal center formation, somatic hypermutation, and creation of memory, clearly require CD40L-CD40, as demonstrated by murine models in which these pathways are inhibited by germline mutations, infusion of blocking Abs, or soluble receptors (12)(13)(14)(15)(16)(17). A few reports have demonstrated CD40-independent B cell responses in T cell-independent systems (9,39,40). However, the in vivo role of T celldependent responses in the absence of CD40L-CD40 interactions have not been studied.…”

Section: Discussionmentioning

confidence: 99%

Th2-Dependent B Cell Responses in the Absence of CD40-CD40 Ligand Interactions

Chirmule

Tazelaar

Wilson

2000

The Journal of Immunology

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CD40 is thought to play a central role in T cell-dependent humoral responses through two distinct mechanisms. CD4+ T helper cells are activated via CD40-dependent Ag presentation in which CD80/CD86 provides costimulation through CD28. In addition, engagement of CD40 on B cells provides a direct pathway for activation of humoral responses. We used a model of adenovirus-mediated gene transfer of β-galactosidase (lacZ) into murine lung to evaluate the specific CD40-dependent pathways required for humoral immunity at mucosal surfaces of the lung. Animals deficient in CD40L failed to develop T and B cell responses to vector. Activation of Th2 cells, which normally requires CD40-dependent stimulation of APCs, was selectively reconstituted in CD40 ligand-deficient mice by systemic administration of an Ab that is agonistic to CD28. Surprisingly, this resulted in the development of a functional humoral response to vector as evidenced by formation of germinal centers and production of antiadenovirus IgG1 and IgA that neutralized and prevented effective readministration of vector. The CD28-dependent B cell response required CD4+ T cells and was mediated via IL-4. These studies indicate that CD40 signals to the B cells are not necessary for CD4+ Th2 cell-dependent humoral responses to be generated.

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“…T lymphocytes Introduction CD154 is a type II transmembrane protein, member of the TNF superfamily, originally detected on the surface of stimulated CD4 1 T cells. Since then, CD154 was found on the surface of activated CD8 1 T cells, gd T cells, B cells, basophils, mast cells, macrophages, dendritic cells, activated platelets, and nonhematopoietic cells such as endothelial cells and fibroblasts [1][2][3][4][5][6][7]. In addition to its transmembrane form, CD154 is also released as a soluble protein by cleavage of the extracellular domain [8,9].…”

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confidence: 99%

Critical role of lipid rafts in CD154‐mediated T cell signaling

et al. 2010

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Although signal pathways triggered via the CD40 molecule are well characterized, those induced via CD154 are less known. This study demonstrates that engagement of CD154 in Jurkat D1.1 cells with soluble CD40 leads to PKC a and d activation, calcium mobilization, and phosphorylation of the Map kinases ERK1/2 and p38. Such response is accompanied by significant recruitment of CD154 into lipid rafts. Disruption of lipid rafts integrity with nystatin or methyl b-cyclodextrin abrogated PKCa PKCd and p38 phosphorylation, but had no effect on ERK1/2 phosphorylation. Inhibition of PKC activation completely abolished p38 phosphorylation but had no effect on ERK1/2 phosphorylation, suggesting that localization of CD154 within lipid rafts is an absolute requirement for CD154-induced PKCaand PKCd-dependent p38 phosphorylation. Furthermore, CD154 acts as co-stimulator for the production of IL-2 in an APC-superantigen-T-cell activation model. The results obtained demonstrate for the first time, that lipid rafts are of immunological relevance for CD154-triggered signals, and reinforce the importance of CD154 in T-cell activation.Key words: CD154 . Lipid rafts . Signaling . T lymphocytes Introduction CD154 is a type II transmembrane protein, member of the TNF superfamily, originally detected on the surface of stimulated CD4 1 T cells. Since then, CD154 was found on the surface of activated CD8 1 T cells, gd T cells, B cells, basophils, mast cells, macrophages, dendritic cells, activated platelets, and nonhematopoietic cells such as endothelial cells and fibroblasts [1][2][3][4][5][6][7]. In addition to its transmembrane form, CD154 is also released as a soluble protein by cleavage of the extracellular domain [8,9]. CD154 acts as a ligand for its classical receptor CD40 that is expressed on various cell types of hematopoietic and nonhematopoietic origin such as B cells, macrophages, dendritic cells, platelets, and endothelial and epithelial cells [5]. Recently, three other functional receptors for CD154 have been described, namely the integrins aIIbb3 [6], a5b1 [10], and Mac-1 [11].CD154 is a crucial costimulatory molecule for the development of both humoral and cellular immune responses [5], and plays an important role in the development and/or maintenance of autoimmune and inflammatory diseases [12][13][14][15]. The absence of CD154 leads to hyper-IgM syndrome, abrogation of germinal center formation and failure of B cells to proliferate and differentiate [5,16].The downstream signals triggered via CD40 molecule are extensively studied [5]. However, the signaling pathways linked to CD154 remain poorly known. Previous studies indicate that CD154 accumulate at T cell-APC contact sites in the immunological synapse [17], and that ligation of CD154 on T cells with specific Ab triggers the activation of src kinases, PKC, and MAP kinases [18][19][20], leading to cytokines secretion [21,22] 770CD3-induced T-cell proliferation [23] and apoptosis [22]. However, the precise mechanism by which CD154-triggered signaling is accomplished r...

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Identification of a novel surface protein on activated CD4+ T cells that induces contact-dependent B cell differentiation (help).

Cited by 328 publications

References 81 publications

The role of polar interactions in the molecular recognition of CD40L with its receptor CD40

The role of polar interactions in the molecular recognition of CD40L with its receptor CD40

Th2-Dependent B Cell Responses in the Absence of CD40-CD40 Ligand Interactions

Critical role of lipid rafts in CD154‐mediated T cell signaling

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