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首页> 外文期刊>Journal of immunotherapy >Cellular and functional characterization of immunoresistant human glioma cell clones selected with alloreactive cytotoxic T lymphocytes reveals their up-regulated synthesis of biologically active TGF-beta.
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Cellular and functional characterization of immunoresistant human glioma cell clones selected with alloreactive cytotoxic T lymphocytes reveals their up-regulated synthesis of biologically active TGF-beta.

机译:用同种异体反应性细胞毒性T淋巴细胞选择的免疫抵抗性人类神经胶质瘤细胞克隆的细胞和功能表征揭示了它们具有生物活性的TGF-β的上调合成。

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摘要

Two immunoresistant (IR) glioma cell variants, 13-06-IR29 and 13-06-IR30, were cloned from 13-06-MG glioma cell populations after receiving continuous immunoselective pressure from multiple alloreactive cytotoxic T lymphocyte (aCTL) preparations. Reapplication of aCTL immunoselective pressure to the IR clones, displaying a partial regain in sensitivity to aCTL after removal of the selective pressure, restored the resistance. The IR variants exhibited cross-resistance to non-human leukocyte antigen (HLA)-restricted effector cells and gamma-irradiation, but not to carmustine. The IR clones were characterized for factors that might contribute to the immunoresistance. The aCTL adhesion to extracellular matrix extracts derived from either the IR clones or the parental cells was similar and not impaired. Furthermore, aCTL binding to parental cells and IR clones was equal. Down-regulation of the cell recognition molecules, class I HLA or intercellular adhesion molecule-1 (ICAM-1), that would inhibit their recognition by aCTL was not observed on the IR clones. The down-regulation of Fas by the IR clones correlated with their resistance to FasL-induced apoptosis. HLA-G or FasL that might provide an immunotolerant environment or provide a means of counterattack to aCTL, respectively, were not associated with the IR phenotype. The aCTL, coincubated with the IR clones and parental cells, displayed up-regulation of multiple secreted cytokines. A significant up-regulation of bioactive transforming growth factor (TGF)-beta was observed in the IR clones compared with the parental cells. These data suggest that increased secretion of bioactive TGF-beta may inhibit aCTL lysis of the IR clones. Disruption of the TGF-beta signaling pathway may circumvent the resistance.
机译:在接受来自多种同种异体反应性细胞毒性T淋巴细胞(aCTL)制剂的连续免疫选择压力后,从13-06-MG胶质瘤细胞群体克隆了两种免疫抵抗(IR)胶质瘤细胞变体13-06-IR29和13-06-IR30。将aCTL免疫选择压力重新施加至IR克隆,去除选择压力后,部分恢复了对aCTL的敏感性,从而恢复了耐药性。 IR变体表现出对非人类白细胞抗原(HLA)限制的效应细胞和伽玛射线的交叉抗性,但对卡莫司汀没有交叉抗性。 IR克隆的特征在于可能有助于免疫抵抗的因子。 aCTL对源自IR克隆或亲代细胞的细胞外基质提取物的粘附性相似且未受损。此外,aCTL与亲本细胞和IR克隆的结合是相等的。在IR克隆上未观察到下调细胞识别分子,I类HLA或细胞间粘附分子1(ICAM-1)的表达,这可能会抑制aCTL对它们的识别。 IR克隆对Fas的下调与其对FasL诱导的细胞凋亡的抗性相关。可能分别提供免疫耐受环境或提供对aCTL的反击手段的HLA-G或FasL与IR表型无关。与IR克隆和亲代细胞共同孵育的aCTL表现出多种分泌型细胞因子的上调。与亲本细胞相比,在IR克隆中观察到生物活性转化生长因子(TGF)-β的显着上调。这些数据表明,增加的生物活性TGF-β的分泌可能会抑制IR克隆的aCTL裂解。 TGF-β信号通路的破坏可能会绕过耐药性。

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