Oncolytic adenoviral mutants with E1B19K gene deletions enhance gemcitabine-induced apoptosis in pancreatic carcinoma cells and anti-tumor efficacy in vivo.

Leitner S; Sweeney K; Oberg D; Davies D; Miranda E; Lemoine NR; Hallden G

首页> 外文期刊>Clinical cancer research: an official journal of the American Association for Cancer Research >Oncolytic adenoviral mutants with E1B19K gene deletions enhance gemcitabine-induced apoptosis in pancreatic carcinoma cells and anti-tumor efficacy in vivo.

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Oncolytic adenoviral mutants with E1B19K gene deletions enhance gemcitabine-induced apoptosis in pancreatic carcinoma cells and anti-tumor efficacy in vivo.

机译：具有E1B19K基因缺失的溶瘤腺病毒突变体增强了吉西他滨诱导的胰腺癌细胞凋亡和体内抗肿瘤功效。

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PURPOSE: Pancreatic adenocarcinoma is a rapidly progressive malignancy that is highly resistant to current chemotherapeutic modalities and almost uniformly fatal. We show that a novel targeting strategy combining oncolytic adenoviral mutants with the standard cytotoxic treatment, gemcitabine, can markedly improve the anticancer potency. EXPERIMENTAL DESIGN: Adenoviral mutants with the E1B19K gene deleted with and without E3B gene expression (AdDeltaE1B19K and dl337 mutants, respectively) were assessed for synergistic interactions in combination with gemcitabine. Cell viability, mechanism of cell death, and antitumor efficacy in vivo were determined in the pancreatic carcinoma cells PT45 and Suit2, normal human bronchial epithelial cells, and in PT45 xenografts. RESULTS: The DeltaE1B19K-deleted mutants synergized with gemcitabine to selectively kill cultured pancreatic cancer cells and xenografts in vivo with no effect in normal cells. The corresponding wild-type virus (Ad5) stimulated drug-induced cellkilling to a lesser degree. Gemcitabine blocked replication of all viruses despite the enhanced cell killing activity due to gemcitabine-induced delay in G1/S-cell cycle progression, with repression of cyclin E and cdc25A, which was not abrogated by viral E1A-expression. Synergistic cell death occurred through enhancement of gemcitabine-induced apoptosis in the presence of both AdDeltaE1B19K and dl337 mutants, shown by increased cell membrane fragmentation, caspase-3 activation, and mitochondrial dysfunction. CONCLUSIONS: Our data suggest that oncolytic mutants lacking the antiapoptotic E1B19K gene can improve efficacy of DNA-damaging drugs such as gemcitabine through convergence on cellular apoptosis pathways. These findings imply that less toxic doses than currently practiced in the clinic could efficiently target pancreatic adenocarcinomas when combined with adenoviral mutants.

机译：目的：胰腺腺癌是一种快速进展的恶性肿瘤，对目前的化疗方法具有高度抵抗力，并且几乎是致命的。我们表明结合溶瘤腺病毒突变体与标准细胞毒性治疗吉西他滨的新型靶向策略可以显着提高抗癌效力。实验设计：评估具有E1B19K基因缺失和不具有E3B基因表达的腺病毒突变体（分别为AdDeltaE1B19K和dl337突变体）与吉西他滨的协同相互作用。在胰腺癌细胞PT45和Suit2，正常人支气管上皮细胞以及PT45异种移植物中，确定了体内的细胞活力，细胞死亡机制和抗肿瘤功效。结果：缺失DeltaE1B19K的突变体与吉西他滨协同作用，在体内选择性杀死培养的胰腺癌细胞和异种移植物，而对正常细胞没有影响。相应的野生型病毒（Ad5）在较小程度上刺激了药物诱导的细胞杀伤作用。尽管吉西他滨诱导了G1 / S细胞周期进程的延迟，并抑制了细胞周期蛋白E和cdc25A，但并未被病毒E1A的表达消除，吉西他滨仍能阻止所有病毒的复制。在存在AdDeltaE1B19K和dl337突变体的情况下，通过增强吉西他滨诱导的凋亡发生了协同细胞死亡，这表现为细胞膜碎片增多，caspase-3活化和线粒体功能障碍。结论：我们的数据表明，缺乏抗凋亡E1B19K基因的溶瘤突变体可以通过细胞凋亡途径的融合来提高DNA破坏性药物（如吉西他滨）的疗效。这些发现表明，与腺病毒突变体联合使用时，毒性剂量低于临床上目前可以有效靶向胰腺癌的剂量。

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《Clinical cancer research: an official journal of the American Association for Cancer Research》 |2009年第5期|共11页
作者
Leitner S; Sweeney K; Oberg D; Davies D; Miranda E; Lemoine NR; Hallden G;
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正文语种 eng
中图分类肿瘤学;
关键词
gemcitabine; in vivo; Apoptosis; Pancreatic polypeptide; avian; 脱噬作用;

机译：gemcitabine;in vivo;Apoptosis;Pancreatic polypeptide;avian;脱噬作用;

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专利

1. Oncolytic adenoviral mutants with E1B19K gene deletions enhance gemcitabine-induced apoptosis in pancreatic carcinoma cells and anti-tumor efficacy in vivo. [J] . Leitner S, Sweeney K, Oberg D, Clinical cancer research: an official journal of the American Association for Cancer Research . 2009,第5期

机译：具有E1B19K基因缺失的溶瘤腺病毒突变体增强了吉西他滨诱导的胰腺癌细胞凋亡和体内抗肿瘤功效。
2. Improved potency and selectivity of an oncolytic E1ACR2 and E1B19K deleted adenoviral mutant in prostate and pancreatic cancers. [J] . Oberg D, Yanover E, Adam V, Clinical cancer research: an official journal of the American Association for Cancer Research . 2010,第2期

机译：在前列腺癌和胰腺癌中，溶瘤的E1ACR2和E1B19K缺失的腺病毒突变体的效力和选择性得到了提高。
3. Transgene expression by oncolytic adenoviruses is modulated by E1B19K deletion in a cell type-dependent manner. [J] . Rohmer S, Quirin C, Hesse Virology . 2009,第2期

机译：溶瘤腺病毒的转基因表达通过E1B19K缺失以细胞类型依赖性方式调节。
4. Predictive Efficacy of Low Burden EGFR Mutation Detected by Next-Generation Sequencing on Response to EGFR Tyrosine Kinase Inhibitors in Non-Small-Cell Lung Carcinoma [C] . Yeul Hong Kim, Hye Sook Kim, Jae Sook Sung, Molecular Medicine TRI-CON. . 2014

机译：下一代测序对非小细胞肺癌抗蛋白酶激酶抑制剂进行下一代测序检测的低负荷EGFR突变的预测疗效
5. Anti-tumor activity of an oncolytic adenoviral construct expressing a small interfering RNA transgene. [D] . Samuel, Shirley Kulangara. 2007

机译：表达小干扰RNA转基因的溶瘤腺病毒构建体的抗肿瘤活性。
6. Oncolytic Adenoviral Mutants with E1B19K Gene Deletions Enhance Gemcitabine-induced Apoptosis in Pancreatic Carcinoma Cells and Anti-Tumor Efficacy In vivo [O] . Stephan Leitner, Katrina Sweeney, Daniel Öberg, -1

机译：具有E1B19K基因缺失的溶瘤腺病毒突变体增强吉西他滨诱导的胰腺癌细胞凋亡和体内抗肿瘤功效。
7. Oncolytic Adenoviral Mutants with E1B19K Gene Deletions Enhance Gemcitabine-induced Apoptosis in Pancreatic Carcinoma Cells and Anti-Tumor Efficacy In vivo [O] . Stephan Leitner, Katrina Sweeney, Daniel Öberg, 2009

机译：具有E1B19K基因缺失的溶瘤腺病毒突变体增强吉西众林诱导的胰腺癌细胞细胞凋亡，体内抗肿瘤疗效

Oncolytic adenoviral mutants with E1B19K gene deletions enhance gemcitabine-induced apoptosis in pancreatic carcinoma cells and anti-tumor efficacy in vivo.

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