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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >SYK -targeted dendritic cell-mediated cytotoxic T lymphocytes enhance the effect of immunotherapy on retinoblastoma
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SYK -targeted dendritic cell-mediated cytotoxic T lymphocytes enhance the effect of immunotherapy on retinoblastoma

机译:Syk -Targeted树突细胞介导的细胞毒性T淋巴细胞增强了免疫疗法对视网膜母细胞瘤的作用

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Abstract Purpose Retinoblastoma (RB) is the most common primary intraocular tumor in children. Chemotherapy is currently the main method of RB treatment. Unfortunately, RB often becomes chemoresistant and turns lethal. Here, we used in vitro cell immunotherapy to explore whether adoptive immunotherapy could be used as a potential treatment for RB. We focused on spleen tyrosine kinase (SYK), which is significantly upregulated in RB cells and serves as a marker for RB cells. Methods Using lentiviruses, we genetically modified dendritic cells (DCs) to express and present the SYK peptide antigen to cytotoxic T lymphocytes (CTLs) in vitro. We used SYK-negative cell lines (MDA-MB-231, MCF-10A, and hTERT-RPE1) and SYK-positive cell lines (MCF-7 and RB-Y79) to evaluate the specificity and cytotoxicity of DC presented CTLs using FACS, live-cell imaging, and RNA interference. Results The cytotoxicity of CTLs induced by SYK-overexpressing DCs (SYK-DC–CTLs) was enhanced more than three times in SYK-positive cell lines compared with SYK-negative cell lines. DCs primed with SYK could drive CTL cytotoxicity against SYK-positive cell lines but not against SYK-negative cell lines. Moreover, SYK -silenced RB-Y79 cells successfully evaded the cytotoxic attack from SYK-DC–CTLs. However, SYK-DC–CTLs could target SYK overexpressed hTERT-RPE1 cells, suggesting that SYK is a specific antigen for RB. Furthermore, SYK-DC–CTL exhibited specific cytotoxicity against carboplatin-resistant RB-Y79 cells in vitro. Conclusions Our data showed that SYK could be a potential immunotherapy target mediated by DCs. We propose SYK as a candidate target for treatment of chemoresistant RB.
机译:摘要目的视网膜母细胞瘤(RB)是儿童中最常见的主要眼肿瘤。化疗目前是RB治疗的主要方法。不幸的是,RB经常变成化学诱使并转动致命。在这里,我们使用的体外细胞免疫疗法探索是否可以用作RB的潜在治疗方法。我们专注于脾脏酪氨酸激酶(Syk),其在RB细胞中显着上调,用作Rb细胞的标志物。方法使用Lentiviruses,我们将遗传修饰的树突细胞(DCS)表达并将Syk肽抗原在体外表达细胞毒性T淋巴细胞(CTL)。我们使用Syk-Negal Cell系(MDA-MB-231,MCF-10A和HTERT-RPE1)和SYK阳性细胞系(MCF-7和RB-Y79)来评估DC呈现的CTLS的特异性和细胞毒性使用FACS ,活细胞成像和RNA干扰。结果与SYK阴性细胞系相比,SYK-DC-CTLS(SYK-DC-CTL)诱导的CTL的细胞毒性增强了SYK阳性细胞系的三次以上。用Syk灌注的DC可以驱动CTL细胞毒性对Syk阳性细胞系但不抵抗Syk阴性细胞系。此外,Syk -Silenced RB-Y79细胞成功地从Syk-DC-CTLS中脱落了细胞毒性攻击。然而,Syk-DC-CTL可以靶向SYK过表达HTERT-RPE1细胞,表明SYK是RB的特定抗原。此外,SYK-DC-CTL在体外表现出针对卡铂抗性RB-Y79细胞的特异性细胞毒性。结论我们的数据显示SYK可能是由DCS介导的潜在免疫疗法靶标。我们将Syk作为治疗化学抑制RB的候选目标。

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