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Suicide gene therapy with HSV-TK in pancreatic cancer has no effect in vivo in a mouse model.

机译:HSV-TK在胰腺癌中的自杀基因疗法在小鼠模型中没有体内作用。

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AIM: To study in vivo whether pancreatic cancer tumour growth and metastasis can be modified by a gene construct with HSV-TK suicide gene and IL2 co-expression.METHODS: Seventy-eight female SCID mice were i.p. inoculated with retrovirally transduced or control MIA PaCa 2, CAPAN-1 and PANC-1 cell lines. The animals were then randomly selected for saline or ganciclovir (GCV) treatment from the second week, for a total of two weeks.RESULTS: Most inoculated mice developed tumour nodules and spleen metastases. The liver was colonized by control CAPAN-1 and MIA PaCa 2, but not by PANC-1. Tumours in transduced MIA PaCa 2 cell injected mice were smaller, and in transduced CAPAN-1 injected mice larger, than in control-inoculated mice. There were increased pancreatic and decreased spleen metastases from transduced CAPAN-1, and diminished liver involvement from transduced MIA PaCa 2. No differences were found between mice inoculated with transduced and control PANC-1 cell lines. GCV treatment had no effect on tumour's size or metastases.CONCLUSIONS: The HSV-TK suicide gene does not confer GCV sensitivity to pancreatic cancer in this in vivo model. Different pancreatic cancer cell lines cause different growth and metastasis patterns after inoculation in SCID mice, possibly because of variations in their inherent characteristics. The different effects of our vector on cell growth and metastasis may be attributable to the effects of the immunostimulatory cytokine IL2.
机译:目的:研究体内是否可以通过具有HSV-TK自杀基因和IL2共表达的基因构建物来修饰胰腺癌的生长和转移。方法:78只雌性SCID小鼠经腹腔注射。接种逆转录病毒转导或控制的MIA PaCa 2,CAPAN-1和PANC-1细胞系。然后从第二周开始随机选择动物进行盐水或更昔洛韦(GCV)治疗,共进行两周。结果:大多数接种的小鼠出现了瘤状结节和脾脏转移。肝脏被对照CAPAN-1和MIA PaCa 2定植,但不被PANC-1定植。与对照接种的小鼠相比,转染的MIA PaCa 2细胞注射的小鼠中的肿瘤更小,而转导的CAPAN-1注射的小鼠中的肿瘤更大。转导的CAPAN-1引起的胰腺转移增加,脾脏转移减少,转导的MIA PaCa 2引起的肝脏受累减少。在转导的和对照的PANC-1细胞系接种的小鼠之间未发现差异。结论:HSV-TK自杀基因并不赋予GCV对胰腺癌敏感性的体内模型。接种SCID小鼠后,不同的胰腺癌细胞系会导致不同的生长和转移方式,这可能是由于其固有特性的差异。我们的载体对细胞生长和转移的不同作用可能归因于免疫刺激性细胞因子IL2的作用。

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