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首页> 外文期刊>Journal of immunotherapy >Bromohydrin pyrophosphate-stimulated Vgamma9delta2 T cells expanded ex vivo from patients with poor-prognosis neuroblastoma lyse autologous primary tumor cells.
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Bromohydrin pyrophosphate-stimulated Vgamma9delta2 T cells expanded ex vivo from patients with poor-prognosis neuroblastoma lyse autologous primary tumor cells.

机译:预后差的神经母细胞瘤溶解自体原发性肿瘤细胞的患者体内用焦磷酸溴代醇刺激的Vgamma9delta2 T细胞离体扩增。

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摘要

Gamma/delta T cells (Vgamma9delta2) contribute to innate immunity and exert natural cytotoxicity against a variety of tumors. Using a synthetic phosphoantigen (Bromohydrin Pyrophosphate, BrHPP), we amplified Vgamma9delta2 T cells in vitro from neuroblastoma patients. In the presence of BrHPP and low doses of IL-2, robust proliferation of Vgamma9delta2 T cells was obtained from peripheral blood mononuclear cells (PBMC) harvested at diagnosis. Moderate proliferation was observed from PBMC harvested after stem cell transplantation, whereas modest levels of Vgamma9delta2 T cells were obtained from PBMC harvested after induction therapy. Proliferation was observed after a single in vitro stimulation with BrHPP. After 21 days in culture, Vgamma9delta2 T cells represented more than 80% of cultured cells (a 50-fold expansion from baseline). Moreover, BrHPP-amplified Vgamma9delta2 T cells from patients-expressed activation markers and were able to lyse allogeneic and autologous neuroblasts. This cytotoxic activity was gammadelta T-cell receptor-dependent. Clinical trials using BrHPP are warranted in patients with poor-prognosis neuroblastoma, either to expand patient-derived Vgamma9delta2 T cells ex vivo or by direct administration to in vivo to boost the pool of resident Vgamma9delta2 T cells in vivo.
机译:γ/δT细胞(Vgamma9delta2)有助于先天免疫,并对多种肿瘤产生天然细胞毒性。使用合成的磷酸抗原(溴代磷酸焦磷酸,BrHPP),我们从成神经细胞瘤患者体外扩增了Vgamma9delta2 T细胞。在BrHPP和低剂量IL-2的存在下,从诊断时收集的外周血单个核细胞(PBMC)获得了Vgamma9delta2 T细胞的强劲增殖。从干细胞移植后收获的PBMC中观察到中等增殖,而从诱导治疗后收获的PBMC中获得了适度水平的Vgamma9delta2 T细胞。用BrHPP单次体外刺激后观察到增殖。培养21天后,Vgamma9delta2 T细胞占培养细胞的80%以上(相对于基线扩增50倍)。此外,来自患者的BrHPP扩增的Vgamma9delta2 T细胞表达了激活标记,并且能够裂解同种异体和自体成神经细胞。这种细胞毒性活性是γ-T细胞受体依赖性的。对于预后较差的神经母细胞瘤,必须使用BrHPP进行临床试验,以扩大患者来源的Vgamma9delta2 T细胞在体外或直接向体内给药以增强体内驻留的Vgamma9delta2 T细胞库。

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