Combination with low-dose gemcitabine and hTERT-promoter-dependent conditionally replicative adenovirus enhances cytotoxicity through their crosstalk mechanisms in pancreatic cancer.

Onimaru M; Ohuchida K; Nagai E; Mizumoto K; Egami T; Cui L; Sato N; Uchino J; Takayama K; Hashizume M; Tanaka M

首页> 外文期刊>Cancer letters >Combination with low-dose gemcitabine and hTERT-promoter-dependent conditionally replicative adenovirus enhances cytotoxicity through their crosstalk mechanisms in pancreatic cancer.

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Combination with low-dose gemcitabine and hTERT-promoter-dependent conditionally replicative adenovirus enhances cytotoxicity through their crosstalk mechanisms in pancreatic cancer.

机译：与低剂量吉西他滨和hTERT启动子相关的条件复制腺病毒联合使用可通过它们在胰腺癌中的串扰机制增强细胞毒性。

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To overcome the limited clinical efficacy of conditionally replicative adenoviruses (CRAds), we investigated the effects of combination therapy with gemcitabine (GEM) and the hTERT-promoter-dependent CRAd (hTERT-CRAd), Ad5/3hTERTE1. This combination therapy exhibited enhanced cytotoxic effects on pancreatic cancer both in vitro and in vivo. Furthermore, we revealed that this enhancement effect was due to the multiple bidirectional interactions between hTERT-CRAd and GEM. The GEM-sensitizing effect of E1 expression derived from hTERT-CRAd, and the enhancement effect by GEM on hTERT promoter activity which led to the increase of adenovirus E1 and viral infectivity. This combination therapy may be a promising therapeutic approach for pancreatic cancer.

机译：为克服条件复制腺病毒（CRAds）的有限临床疗效，我们研究了吉西他滨（GEM）和依赖hTERT启动子的CRAd（hTERT-CRAd），Ad5 / 3hTERTE1联合治疗的效果。该组合疗法在体外和体内均显示出对胰腺癌的增强的细胞毒性作用。此外，我们揭示了这种增强作用是由于hTERT-CRAd与GEM之间的多个双向相互作用。源自hTERT-CRAd的E1表达对GEM的增敏作用，以及GEM对hTERT启动子活性的增强作用，导致腺病毒E1和病毒感染性增加。这种联合疗法可能是胰腺癌的有前途的治疗方法。

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《Cancer letters》 |2010年第2期|共9页
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Onimaru M; Ohuchida K; Nagai E; Mizumoto K; Egami T; Cui L; Sato N; Uchino J; Takayama K; Hashizume M; Tanaka M;
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1. Combination with low-dose gemcitabine and hTERT-promoter-dependent conditionally replicative adenovirus enhances cytotoxicity through their crosstalk mechanisms in pancreatic cancer. [J] . Onimaru M, Ohuchida K, Nagai E, Cancer letters . 2010,第2期

机译：与低剂量吉西他滨和hTERT启动子相关的条件复制腺病毒联合使用可通过它们在胰腺癌中的串扰机制增强细胞毒性。
2. Combination of gemcitabine and Ad5/3-Delta24, a tropism modified conditionally replicating adenovirus, for the treatment of ovarian cancer. [J] . Raki M, Kanerva A, Ristimaki A, Gene therapy . 2005,第15期

机译：吉西他滨和Ad5 / 3-Delta24（一种有向性修饰的条件复制腺病毒）的组合，用于治疗卵巢癌。
3. Combination of conditionally replicative adenovirus and standard chemotherapies shows synergistic antitumor effect in pancreatic cancer. [J] . Nelson AR, Davydova J, Curiel DT Cancer science. . 2009,第11期

机译：条件复制性腺病毒和标准化学疗法的组合在胰腺癌中显示出协同的抗肿瘤作用。
4. Effect of Cromolyn in PEGylated Liposome in Combination with Gemcitabine for Pancreatic Cancer [C] . Min Ji Koo, Cha Eun Kim, Hye Jin Kim, Annual meeting exposition of the Controlled Release Society . 2011

机译：克罗莫林联合吉西他滨在聚乙二醇化脂质体中对胰腺癌的作用
5. Multiscale Pharmacodynamic Studies of Combination Gemcitabine and Trabectedin for the Treatment of Pancreatic Cancer. [D] . Miao, Xin. 2017

机译：吉西他滨联合曲贝汀联合治疗胰腺癌的多尺度药效学研究。
6. Combination of conditionally replicative adenovirus and standard chemotherapies shows synergistic antitumor effect in pancreatic cancer [O] . Amy R Nelson, Julia Davydova, David T Curiel, -1

机译：有条件复制的腺病毒和标准化学疗法的组合在胰腺癌中显示出协同的抗肿瘤作用
7. hTERT-promoter-dependent oncolytic adenovirus enhances the transduction and therapeutic efficacy of replication-defective adenovirus vectors in pancreatic cancer cells [O] . Manabu Onimaru, Kenoki Ohuchida, Kazuhiro Mizumoto, 2010

机译：HTERT-PRENDINER依赖于溶解剂腺病毒增强了复制缺陷腺病毒载体在胰腺癌细胞中的转导和治疗疗效

Combination with low-dose gemcitabine and hTERT-promoter-dependent conditionally replicative adenovirus enhances cytotoxicity through their crosstalk mechanisms in pancreatic cancer.

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