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Characterisation of systemic dissemination of nonreplicating adenoviral vectors from tumours in local gene delivery

机译:在局部基因传递中从肿瘤系统传播非复制型腺病毒载体的特征

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Systemic virus dissemination is a potential problem during local gene delivery in solid tumours. However, the kinetics and pathways of the dissemination have not been well characterised during the first 24?h after the infusion is started. To this end, we infused adenoviral vectors for luciferase or enhanced green fluorescence protein into three different tumour models in mice. During and/or after the infusion, we determined the amount of adenoviruses in the tumour, blood, and liver, and examined the transgene expression in the liver, lung, blood, and tumour. In addition, we intravenously injected tumour cells expressing luciferase and examined the biodistribution of these cells in the body. We observed transgene expression in the liver and tumour at 24?h after the infusion, but could not detect transgene expression in the blood and lung. The peak concentration of viral vectors in the plasma occurred during the intratumoral infusion. At 10?min after the infusion, few viral vectors remained in the blood and the ratio of copy numbers of adenoviruses between liver and tumour was >2 in 80% and 10 in 40% of the mice. Most tumour cells injected intravenously accumulated in the lung within the first 24?h. Taken together, these data indicated that systemic virus dissemination occurred mainly during the first 10?min after the intratumoral infusion was started, and that the dissemination was due to infusion-induced convective transport of viral vectors into leaky tumour microvessels.
机译:在实体瘤中局部基因递送期间,全身性病毒传播是潜在的问题。然而,在输注开始后的最初24小时内,尚未很好地表征传播的动力学和途径。为此,我们将用于荧光素酶或增强型绿色荧光蛋白的腺病毒载体注入小鼠的三种不同的肿瘤模型中。在输注期间和/或之后,我们确定了肿瘤,血液和肝脏中腺病毒的数量,并检查了肝,肺,血液和肿瘤中转基因的表达。此外,我们静脉注射了表达荧光素酶的肿瘤细胞,并检查了这些细胞在体内的生物分布。我们在输注后24小时观察到肝和肿瘤中的转基因表达,但未检测到血液和肺中的转基因表达。血浆中病毒载体的峰值浓度发生在肿瘤内输注期间。输注后10分钟,血液中几乎没有病毒载体,肝和肿瘤之间腺病毒的拷贝数比在80%的小鼠中大于2,在40%的小鼠中为10。在最初的24小时内,大多数静脉注射的肿瘤细胞在肺中积累。综上所述,这些数据表明,全身病毒的传播主要发生在肿瘤内输注开始后的前10分钟内,而这种传播是由于输注引起的对流转移病毒载体进入渗漏的肿瘤微血管。

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