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MEK inhibitor trametinib in combination with gemcitabine regresses a patient-derived orthotopic xenograft (PDOX) pancreatic cancer nude mouse model

机译:Mek抑制剂Trametinib与Gemcitabine组合回归患者衍生的原位异种移植物(Pdox)胰腺癌裸鼠模型

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Pancreatic cancer is resistant to treatment and needs precision individualized therapy to improve the outcome of this disease. Previously, we demonstrated that trametinib (TRA), a MEK inhibitor, could inhibit a pancreatic cancer patient-derived orthotopic xenograft (PDOX). In the present study, we show that gemcitabine (GEM) in combination with TRA was more effective than TRA alone. We implanted a patient pancreatic cancer orthotopically in the pancreatic tail of nude mice to establish the PDOX model. After seven weeks of tumor growth, we divided 32 pancreatic-cancer PDOX nude mice into 4 groups of eight: untreated control; GEM (once a week for 2 weeks); TRA (14 consecutive days); GEM + TRA (GEM: once a week for 2 weeks, TRA:14 consecutive days). We found that treated mice on day 14 had significantly reduced tumor volume in comparison to untreated control. TRA and the combination of GEM + TRA therapy significantly inhibited tumor development in comparison to GEM alone. However, GEM + TRA inhibited the PDOX tumor growth significantly greater than TRA alone. These results suggest the clinical potential of the combination of TRA and GEM for pancreatic cancer.
机译:胰腺癌是治疗的抗性,需要精确个体化治疗,以改善这种疾病的结果。以前,我们证明枪滴虫(TRA)是MEK抑制剂,可抑制胰腺癌患者衍生的原位异种移植物(PDOX)。在本研究中,我们表明吉西他滨(宝石)与TRA的组合单独比TRA更有效。我们在裸鼠的胰腺尾部植入患者胰腺癌以建立PDOX模型。经过七周的肿瘤生长,我们将32个胰腺癌PDOX裸鼠分成4组八:未处理的对照;宝石(每周一次2周); TRA(连续14天);宝石+ TRA(宝石:每周一次2周,TRA:连续14天)。我们发现,与未处理的对照相比,第14天的治疗小鼠显着降低了肿瘤体积。仅与单独的宝石相比,TRA和宝石+ TRA治疗的组合显着抑制肿瘤发育。然而,GEM + TRA抑制PDOX肿瘤生长明显大于TRA。这些结果表明了TRA和GEM用于胰腺癌的临床潜力。

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