Signal transduction by HLA class II molecules in human T cells: induction of LFA-1-dependent and independent adhesion

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Signal transduction by HLA class II molecules in human T cells: induction of LFA-1-dependent and independent adhesion. / Odum, Niels; Yoshizumi, H; Okamoto, Y; Kamikawaji, N; Kimura, A; Nishimura, Y; Sasazuki, T.

In: Human Immunology, Vol. 35, No. 2, 1992, p. 71-84.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Odum, N, Yoshizumi, H, Okamoto, Y, Kamikawaji, N, Kimura, A, Nishimura, Y & Sasazuki, T 1992, 'Signal transduction by HLA class II molecules in human T cells: induction of LFA-1-dependent and independent adhesion', Human Immunology, vol. 35, no. 2, pp. 71-84.

APA

Odum, N., Yoshizumi, H., Okamoto, Y., Kamikawaji, N., Kimura, A., Nishimura, Y., & Sasazuki, T. (1992). Signal transduction by HLA class II molecules in human T cells: induction of LFA-1-dependent and independent adhesion. Human Immunology, 35(2), 71-84.

Vancouver

Odum N, Yoshizumi H, Okamoto Y, Kamikawaji N, Kimura A, Nishimura Y et al. Signal transduction by HLA class II molecules in human T cells: induction of LFA-1-dependent and independent adhesion. Human Immunology. 1992;35(2):71-84.

Author

Odum, Niels ; Yoshizumi, H ; Okamoto, Y ; Kamikawaji, N ; Kimura, A ; Nishimura, Y ; Sasazuki, T. / Signal transduction by HLA class II molecules in human T cells: induction of LFA-1-dependent and independent adhesion. In: Human Immunology. 1992 ; Vol. 35, No. 2. pp. 71-84.

Bibtex

@article{5de03780fd9611ddb219000ea68e967b,
title = "Signal transduction by HLA class II molecules in human T cells: induction of LFA-1-dependent and independent adhesion",
abstract = "Crosslinking HLA-DR molecules by monoclonal antibodies (moAbs) induces protein tyrosine phosphorylation and results in a secondary elevation of free cytoplasmic calcium concentrations in activated human T cells. Binding of bacterial superantigens or moAbs to DR molecules on activated T cells was recently reported to induce homotypic aggregation through activation of protein kinase C (PKC) and mediated by CD11a/CD54 (LFA-1/CAM-1) adhesion molecules. Here, we report that moAbs directed against framework DR, but neither DR1, 2- and DRw52- nor DQ- and DP-specific moABs induced homotypic aggregation of antigen- and alloantigen-activated T cells, antigen-specific CD4+ T-cell lines, a CD8+ T-cytotoxic cell line, and T-leukemia cells (HUT78). Protein tyrosine kinase (PTK) inhibitor herbimycin A partly blocked class-II-induced aggregation responses. In contrast, phorbol ester (PMA)-induced aggregation was essentially unaffected. A potent inhibitor of PKC, staurosporin, inhibited both moAb- and PMA-induced aggregation responses. The aggregation responses were completely inhibited by low temperatures, cytochalasins B and E, and partly inhibited by EDTA and CD18 moAbs, but unaffected by aphidicolin, mitomycin C, an adenylate cyclase inhibitor (2'5'-dideoxyadenosine), and moAbs against other adhesion molecules (CD2/CD58 [LFA-3], CD28/CD28 ligand B7, CD4, and CD44). In conclusion, HLA class-II-induced aggregation responses in activated T cells appear to involve PTK and PKC activation and to be mediated through CD11a-dependent and independent adhesion pathways.",
author = "Niels Odum and H Yoshizumi and Y Okamoto and N Kamikawaji and A Kimura and Y Nishimura and T Sasazuki",
note = "Keywords: Alkaloids; Antigens, CD; Aphidicolin; Benzoquinones; Cell Adhesion; Cell Line; Colchicine; Cold Temperature; Cytochalasin B; Cytochalasins; Dideoxyadenosine; Dose-Response Relationship, Drug; Edetic Acid; HLA-DR Antigens; Humans; Lactams, Macrocyclic; Lymphocyte Function-Associated Antigen-1; Mitomycin; Protein Kinase C; Protein-Tyrosine Kinases; Quinones; Signal Transduction; Staurosporine; T-Lymphocytes; Tetradecanoylphorbol Acetate",
year = "1992",
language = "English",
volume = "35",
pages = "71--84",
journal = "Human Immunology",
issn = "0198-8859",
publisher = "Elsevier",
number = "2",

}

RIS

TY - JOUR

T1 - Signal transduction by HLA class II molecules in human T cells: induction of LFA-1-dependent and independent adhesion

AU - Odum, Niels

AU - Yoshizumi, H

AU - Okamoto, Y

AU - Kamikawaji, N

AU - Kimura, A

AU - Nishimura, Y

AU - Sasazuki, T

N1 - Keywords: Alkaloids; Antigens, CD; Aphidicolin; Benzoquinones; Cell Adhesion; Cell Line; Colchicine; Cold Temperature; Cytochalasin B; Cytochalasins; Dideoxyadenosine; Dose-Response Relationship, Drug; Edetic Acid; HLA-DR Antigens; Humans; Lactams, Macrocyclic; Lymphocyte Function-Associated Antigen-1; Mitomycin; Protein Kinase C; Protein-Tyrosine Kinases; Quinones; Signal Transduction; Staurosporine; T-Lymphocytes; Tetradecanoylphorbol Acetate

PY - 1992

Y1 - 1992

N2 - Crosslinking HLA-DR molecules by monoclonal antibodies (moAbs) induces protein tyrosine phosphorylation and results in a secondary elevation of free cytoplasmic calcium concentrations in activated human T cells. Binding of bacterial superantigens or moAbs to DR molecules on activated T cells was recently reported to induce homotypic aggregation through activation of protein kinase C (PKC) and mediated by CD11a/CD54 (LFA-1/CAM-1) adhesion molecules. Here, we report that moAbs directed against framework DR, but neither DR1, 2- and DRw52- nor DQ- and DP-specific moABs induced homotypic aggregation of antigen- and alloantigen-activated T cells, antigen-specific CD4+ T-cell lines, a CD8+ T-cytotoxic cell line, and T-leukemia cells (HUT78). Protein tyrosine kinase (PTK) inhibitor herbimycin A partly blocked class-II-induced aggregation responses. In contrast, phorbol ester (PMA)-induced aggregation was essentially unaffected. A potent inhibitor of PKC, staurosporin, inhibited both moAb- and PMA-induced aggregation responses. The aggregation responses were completely inhibited by low temperatures, cytochalasins B and E, and partly inhibited by EDTA and CD18 moAbs, but unaffected by aphidicolin, mitomycin C, an adenylate cyclase inhibitor (2'5'-dideoxyadenosine), and moAbs against other adhesion molecules (CD2/CD58 [LFA-3], CD28/CD28 ligand B7, CD4, and CD44). In conclusion, HLA class-II-induced aggregation responses in activated T cells appear to involve PTK and PKC activation and to be mediated through CD11a-dependent and independent adhesion pathways.

AB - Crosslinking HLA-DR molecules by monoclonal antibodies (moAbs) induces protein tyrosine phosphorylation and results in a secondary elevation of free cytoplasmic calcium concentrations in activated human T cells. Binding of bacterial superantigens or moAbs to DR molecules on activated T cells was recently reported to induce homotypic aggregation through activation of protein kinase C (PKC) and mediated by CD11a/CD54 (LFA-1/CAM-1) adhesion molecules. Here, we report that moAbs directed against framework DR, but neither DR1, 2- and DRw52- nor DQ- and DP-specific moABs induced homotypic aggregation of antigen- and alloantigen-activated T cells, antigen-specific CD4+ T-cell lines, a CD8+ T-cytotoxic cell line, and T-leukemia cells (HUT78). Protein tyrosine kinase (PTK) inhibitor herbimycin A partly blocked class-II-induced aggregation responses. In contrast, phorbol ester (PMA)-induced aggregation was essentially unaffected. A potent inhibitor of PKC, staurosporin, inhibited both moAb- and PMA-induced aggregation responses. The aggregation responses were completely inhibited by low temperatures, cytochalasins B and E, and partly inhibited by EDTA and CD18 moAbs, but unaffected by aphidicolin, mitomycin C, an adenylate cyclase inhibitor (2'5'-dideoxyadenosine), and moAbs against other adhesion molecules (CD2/CD58 [LFA-3], CD28/CD28 ligand B7, CD4, and CD44). In conclusion, HLA class-II-induced aggregation responses in activated T cells appear to involve PTK and PKC activation and to be mediated through CD11a-dependent and independent adhesion pathways.

M3 - Journal article

C2 - 1286978

VL - 35

SP - 71

EP - 84

JO - Human Immunology

JF - Human Immunology

SN - 0198-8859

IS - 2

ER -

ID: 10636185