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BONE MARROW–DERIVED DENDRITIC CELL PROGENITORS (NLDC 145+ MHC CLASS II+ B7–1dim B7–2−) INDUCE ALLOANTIGEN-SPECIFIC HYPORESPONSIVENESS IN MURINE T LYMPHOCYTES

机译：骨髓来源的树突状细胞祖细胞（NLDC 145 +MHC CLASS II +B7–1dimB7–2−）在小鼠T淋巴细胞中引起异基因特异性低反应性。

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The functional maturation of dendritic cells (DC) and other antigen-presenting cells is believed to reflect the upregulation of cell surface major histocompatibility complex (MHC) class II and other T cell co-stimulatory molecules, especially the CD28 ligands B7–1 (CD80) and B7–2 (CD86). In this study, we propagated cells exhibiting characteristics of DC precursors from the bone marrow (BM) of BIO mice (H-2^b; I-A¹) in response to granulocyte-macrophage colony stimulating factor (GM-CSF). The methods used were similar to those employed previously to propagate DC progenitors from normal mouse liver. Cells expressing DC lineage markers (NLDC 145⁺, 33D1⁺ N418⁺) harvested from 8–10-day GM-CSF stimulated BM cell cultures were CD45⁺, heat-stable antigen⁺, CD54⁺, CD44⁺, MHC class II⁺, B7–1^dim but B7–2⁻ (costimulatory molecule-deficient). Supplementation of cultures with interleukin-4 (IL-4) in addition to GM-CSF however, resulted in marked upregulation of MHC class II and B7–2 expression. These latter cells exhibited potent allostimulatory activity in primary mixed leukocyte cultures. In contrast, the cells stimulated with GM-CSF alone were relatively weak stimulators and induced alloantigen-specific hyporesponsiveness in allogeneic T cells (C3H; H-2^k; I-E⁺) detected upon re-stimulation in secondary MLR. This was associated with blockade of IL-2 production. Reactivity to third-party stimulators was intact. The hyporesponsiveness induced by the GM-CSF stimulated, costimulatory molecule-deficient cells was prevented by incorporation of anti-CD28 monoclonal antibody in the primary MLR and was reversed by addition of IL-2 to restimulated T cells. The findings show that MHC class II⁺ B7–2⁻ cells with a DC precursor phenotype can induce alloantigen-specific hyporesponsiveness in vitro. Under the appropriate conditions, such costimulatory molecule-deficient cells could contribute to the induction of donor-specific unresponsiveness in vivo.

机译：树突状细胞（DC）和其他抗原呈递细胞的功能成熟被认为反映了细胞表面主要组织相容性复合体（MHC）II类和其他T细胞共刺激分子的上调，尤其是CD28配体B7-1（CD80 ）和B7–2（CD86）。在这项研究中，我们繁殖了对BIO小鼠（H-2 ^{b ; IA ^{1 ）的骨髓（BM）表现出DC前体特征的细胞。巨噬细胞集落刺激因子（GM-CSF）。使用的方法与以前从正常小鼠肝脏繁殖DC祖细胞所使用的方法相似。从8-10天GM-CSF刺激的BM细胞培养物中收获的表达DC谱系标记的细胞（NLDC 145 ^{+ ，33D1 ^{+ N418 ^{+ ） CD45 ^{+ ，热稳定抗原^{+ ，CD54 ^{+ ，CD44 ^{+ ，MHC II类^{+ ，B7-1 ^{dim ，但B7-2 ^{-（共刺激分子缺陷）。然而，除了GM-CSF外，还补充白介素4（IL-4）培养物，导致II类MHC和B7-2表达明显上调。后面的这些细胞在原代混合白细胞培养物中表现出有效的同种异体刺激活性。相反，仅由GM-CSF刺激的细胞是相对较弱的刺激物，并在同种异体T细胞（C3H； H-2 ^{k ； IE ^{+ ）中诱导同种抗原特异性低反应性在次级MLR中重新刺激后检测到。这与IL-2产生的阻断有关。对第三方刺激物的反应性是完整的。通过在原代MLR中掺入抗CD28单克隆抗体可防止GM-CSF刺激的共刺激分子缺陷细胞诱导的机能减退，并通过向再刺激的T细胞中添加IL-2来逆转这种反应。研究结果表明，具有DC前体表型的MHC II ^{+ B7-2 ^{-细胞可以在体外诱导同种抗原特异性低反应性。在适当的条件下，这种共刺激分子不足的细胞可能有助于诱导体内供体特异性无反应性。}}}}}}}}}}}}}}}}

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Lina Lu; Delbert McCaslin; Thomas E. Starzl; Angus W. Thomson;
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年(卷),期 -1(60),12
年度 -1
页码 1539–1545
总页数 18
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专利

1. Evidence that an OX-2-positive cell can inhibit the stimulation of type 1 cytokine production by bone marrow-derived B7-1 (and B7-2)-positive dendritic cells. [J] . Gorczynski L, Chen Z, Hu J, The Journal of Immunology: Official Journal of the American Association of Immunologists . 1999,第2期

机译：OX-2阳性细胞可以抑制骨髓来源的B7-1（和B7-2）阳性树突状细胞刺激1型细胞因子产生的证据。
2. Induction of alloantigen-specific hyporesponsiveness in human T lymphocytes by blocking interaction of CD28 with its natural ligand B7/BB1. [J] . P Tan, C Anasetti, J A Hansen, The Journal of Experomental Medicine . 1993,第1期

机译：通过阻断CD28及其天然配体B7 / BB1的相互作用，在人T淋巴细胞中诱导同种抗原特异性低反应性。
3. Purification of antigenic peptide from murine hepatoma cells recognized by Class-I major histocompatibility complex molecule-restricted cytotoxic T-lymphocytes induced with B7-1-gene-transfected hepatoma cells. [J] . Nakatsuka K, Sugiyama H, Nakagawa Y, Journal of Hepatology: The Journal of the European Association for the Study of the Liver . 1999,第6期

机译：从被I型主要组织相容性复合物分子限制的B7-1基因转染的肝癌细胞诱导的鼠肝细胞中纯化抗原肽。
4. RNA interference on TLR9 expression affects the response of bone marrow-derived murine dendritic cells to CpG [C] . Ma Ling, Li Xiao-Xi, Xu Yi-Xin, International Symposium on Medical and Pharmaceutical Biotechnology(医药生物技术国际研讨会) . 2009

机译：RNA对TLR9表达的干扰影响骨髓来源的鼠树突状细胞对CpG的反应
5. Effects of cannabinoid receptor deletion on bone marrow-derived dendritic cell subtype development, maturation and antigen loading on MHC class I [D] . Suarez-Martinez, Jose E. 2016

机译：大麻素受体缺失对骨髓衍生的树突式细胞亚型发育，成熟和抗原载荷对MHC级的影响
6. Induction of alloantigen-specific hyporesponsiveness in human T lymphocytes by blocking interaction of CD28 with its natural ligand B7/BB1 [O] . 1993

机译：通过阻断CD28与其天然配体B7 / BB1的相互作用诱导人T淋巴细胞中同种抗原特异性低反应性
7. Bone marrow-derived dendritic cell progenitors (NLDC 145+, MHC class II+, B7-1dim, B7-2-) induce alloantigen-specific hyporesponsiveness in murine T lymphocytes. [O] . Lu L, McCaslin D, Starzl TE, 1995

机译：骨髓来源的树突状细胞祖细胞（NLDC 145 +，II类MHC，B7-1dim，B7-2-）在鼠T淋巴细胞中诱导同种抗原特异性低反应性。

BONE MARROW–DERIVED DENDRITIC CELL PROGENITORS (NLDC 145+ MHC CLASS II+ B7–1dim B7–2−) INDUCE ALLOANTIGEN-SPECIFIC HYPORESPONSIVENESS IN MURINE T LYMPHOCYTES

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