Primary porcine endothelial cells express membrane-bound B7-2 (CD86) and a soluble factor that co-stimulate cyclosporin A-resistant and CD28-dependent human T cell proliferation
スポンサーリンク
概要
著者
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June Carl
Immune Cell Biology Program Naval Medical Research Institute
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Davis Thomas
Immune Cell Biology Program Naval Medical Research Institute
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CRAIGHEAD Nancy
Immune Cell Biology Program, Naval Medical Research Institute
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WILLIAMS Amanda
Immune Cell Biology Program, Naval Medical Research Institute
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SCADRON Andrea
Immune Cell Biology Program, Naval Medical Research Institute
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LEE Kelvin
Immune Cell Biology Program, Naval Medical Research Institute
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Craighead Nancy
Immune Cell Biology Program Naval Medical Research Institute
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Lee Kelvin
Immune Cell Biology Program Naval Medical Research Institute
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Scadron Andrea
Immune Cell Biology Program Naval Medical Research Institute
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Williams Amanda
Immune Cell Biology Program Naval Medical Research Institute
関連論文
- The lgV domain of human B7-2 (CD86) is sufficient to co-stimulate T lymphocytes and induce cytokine secretion
- Both CD28 ligands CD80(B7-1) and CD86(B7-2) activate phosphatidylinositol 3-kinase, and wortmannin reveals heterogeneity in the regulation of T cell IL-2 secretion
- CD28 ligands CD80(B7-1) and CD86(B7-2) induce long-term autocrine growth of CD4+T cells and induce similar patterns of cytokine secretion in vitro
- Primary porcine endothelial cells express membrane-bound B7-2 (CD86) and a soluble factor that co-stimulate cyclosporin A-resistant and CD28-dependent human T cell proliferation