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本文引用的文献

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FOLFIRINOX versus gemcitabine for metastatic pancreatic cancer.FOLFIRINOX 对比吉西他滨治疗转移性胰腺癌。
N Engl J Med. 2011 May 12;364(19):1817-25. doi: 10.1056/NEJMoa1011923.
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Updates of adjuvant therapy in pancreatic cancer: where are we and where are we going? Highlights from the "2010 ASCO Annual Meeting". Chicago, IL, USA. June 4-8, 2010.胰腺癌辅助治疗的进展:我们现状如何,又将走向何方?“2010年美国临床肿瘤学会年会”亮点。美国伊利诺伊州芝加哥。2010年6月4日至8日。
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3
Phase I clinical trial using peptide vaccine for human vascular endothelial growth factor receptor 2 in combination with gemcitabine for patients with advanced pancreatic cancer.一项使用肽疫苗联合吉西他滨治疗晚期胰腺癌患者的人血管内皮生长因子受体 2 的 I 期临床试验。
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Improved expression and reactivity of transduced tumor-specific TCRs in human lymphocytes by specific silencing of endogenous TCR.通过内源性TCR的特异性沉默提高转导的肿瘤特异性TCR在人淋巴细胞中的表达和反应性。
Cancer Res. 2009 Dec 1;69(23):9003-11. doi: 10.1158/0008-5472.CAN-09-1450. Epub 2009 Nov 10.
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The prioritization of cancer antigens: a national cancer institute pilot project for the acceleration of translational research.癌症抗原的优先级排序:美国国立癌症研究所加速转化研究的试点项目
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3,3'-Diindolylmethane enhances chemosensitivity of multiple chemotherapeutic agents in pancreatic cancer.3,3'-二吲哚甲烷增强胰腺癌对多种化疗药物的化疗敏感性。
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Nuclear factor-kappaB p65/relA silencing induces apoptosis and increases gemcitabine effectiveness in a subset of pancreatic cancer cells.核因子-κB p65/relA沉默诱导一部分胰腺癌细胞凋亡并增强吉西他滨的疗效。
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Cancer statistics, 2008.2008年癌症统计数据。
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Erlotinib plus gemcitabine compared with gemcitabine alone in patients with advanced pancreatic cancer: a phase III trial of the National Cancer Institute of Canada Clinical Trials Group.厄洛替尼联合吉西他滨与吉西他滨单药治疗晚期胰腺癌患者的比较:加拿大国家癌症研究所临床试验组的一项III期试验
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Curcumin potentiates antitumor activity of gemcitabine in an orthotopic model of pancreatic cancer through suppression of proliferation, angiogenesis, and inhibition of nuclear factor-kappaB-regulated gene products.姜黄素通过抑制增殖、血管生成以及抑制核因子-κB调节的基因产物,增强吉西他滨在胰腺癌原位模型中的抗肿瘤活性。
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吉西他滨增强肾母细胞瘤基因 WT1 的表达,并增强 WT1 特异性 T 细胞介导的抗肿瘤免疫反应的人胰腺癌细胞敏感性。

Gemcitabine enhances Wilms' tumor gene WT1 expression and sensitizes human pancreatic cancer cells with WT1-specific T-cell-mediated antitumor immune response.

机构信息

Division of Gastroenterology and Hepatology, Department of Internal Medicine, Jikei University School of medicine, Tokyo, Japan.

出版信息

Cancer Immunol Immunother. 2011 Sep;60(9):1289-97. doi: 10.1007/s00262-011-1033-3. Epub 2011 May 24.

DOI:10.1007/s00262-011-1033-3
PMID:21607557
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11029139/
Abstract

Wilms' tumor gene (WT1), which is expressed in human pancreatic cancer (PC), is a unique tumor antigen recognized by T-cell-mediated antitumor immune response. Gemcitabine (GEM), a standard therapeutic drug for PC, was examined for the regulation of WT1 expression and the sensitizing effect on PC cells with WT1-specific antitumor immune response. Expression of WT1 was examined by quantitative PCR, immunoblot analysis, and confocal microscopy. Antigenic peptide of WT1 presented on HLA class I molecules was detected by mass spectrometry. WT1-specific T-cell receptor gene-transduced human T cells were used as effecter T cells for the analysis of cytotoxic activity. GEM treatment of human MIAPaCa2 PC cells enhanced WT1 mRNA levels, and this increase is associated with nuclear factor kappa B activation. Tumor tissue from GEM-treated MIAPaCa2-bearing SCID mice also showed an increase in WT1 mRNA. Some human PC cell lines other than MIAPaCa2 showed up-regulation of WT1 mRNA levels following GEM treatment. GEM treatment shifted WT1 protein from the nucleus to the cytoplasm, which may promote proteasomal processing of WT1 protein and generation of antigenic peptide. In fact, presentation of HLA-A*2402-restricted antigenic peptide of WT1 (CMTWNQMNL) increased in GEM-treated MIAPaCa2 cells relative to untreated cells. WT1-specific cytotoxic T cells killed MIAPaCa2 cells treated with an optimal dose of GEM more efficiently than untreated MIAPaCa2 cells. GEM enhanced WT1 expression in human PC cells and sensitized PC cells with WT1-specific T-cell-mediated antitumor immune response.

摘要

Wilms 瘤基因(WT1)在人类胰腺癌(PC)中表达,是 T 细胞介导的抗肿瘤免疫反应识别的独特肿瘤抗原。吉西他滨(GEM)是 PC 的标准治疗药物,研究了其对 WT1 表达的调节作用,以及对具有 WT1 特异性抗肿瘤免疫反应的 PC 细胞的致敏作用。通过定量 PCR、免疫印迹分析和共聚焦显微镜检查 WT1 的表达。通过质谱法检测 HLA Ⅰ类分子上呈现的 WT1 抗原肽。用转导 WT1 特异性 T 细胞受体基因的人 T 细胞作为效应 T 细胞,分析细胞毒性活性。GEM 处理人 MIAPaCa2 PC 细胞增强 WT1 mRNA 水平,这种增加与核因子 kappa B 激活有关。GEM 处理的 MIAPaCa2 荷瘤 SCID 小鼠的肿瘤组织也显示 WT1 mRNA 增加。除 MIAPaCa2 以外的一些人 PC 细胞系在 GEM 处理后 WT1 mRNA 水平上调。GEM 处理将 WT1 蛋白从细胞核转移到细胞质,这可能促进 WT1 蛋白的蛋白酶体加工和抗原肽的产生。事实上,与未处理的细胞相比,GEM 处理的 MIAPaCa2 细胞中 HLA-A*2402 限制性 WT1 抗原肽(CMTWNQMNL)的呈递增加。与未处理的 MIAPaCa2 细胞相比,用最佳剂量的 GEM 处理的 WT1 特异性细胞毒性 T 细胞更有效地杀死 MIAPaCa2 细胞。GEM 增强了人 PC 细胞中的 WT1 表达,并敏化了具有 WT1 特异性 T 细胞介导的抗肿瘤免疫反应的 PC 细胞。