首页> 外文会议>World congress of the International Photodynamic Association >Uptake of Verteporfin by Orthotopic Xenograft Pancreas Models with Different Levels of Aggression
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Uptake of Verteporfin by Orthotopic Xenograft Pancreas Models with Different Levels of Aggression

机译:不同侵袭水平的异种异种移植胰腺模型对Verteporfin的摄取

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Pancreatic cancer is an aggressive disease with a poor prognosis, usually treated with chemoradiation therapy. Interstitial photodynamic therapy is a potentially effective adjuvant treatment that is under development. In the current study, two orthotopic pancreatic cancer models (AsPC-1 and Panc-1), have been characterized with respect to growth rates, morphology and liposomal drug (Verteporfin) uptake and distribution in SCID mice. Fluorescence of Verteporfin was measured in liver and tumor in vivo using a PDT fluorescence dosimeter with measurements taken before and up to one hour after tail vein injection. Fluorescence reached a plateau by about 15 minutes and did not decrease over the first hour. At time points from 15 minutes to 24 hrs, the internal organs (kidney, spleen, pancreas, tumor, muscle, lung, liver, and skin were excised and scanned on a Typhoon imager. The ratio of fluorescence in tumor versus normal tissues was analyzed with image processing, calculated at each time point and compared to in vivo results. Tissue distribution of Verteporfin in relation to functional vasculature marked by DiOc7 was carried out on frozen sections. Final analysis will result in determination of the ideal time point to administer light to achieve maximum tumor destruction while preserving normal tissue.
机译:胰腺癌是一种侵袭性疾病,预后较差,通常采用化学放射疗法进行治疗。间质性光动力疗法是一种正在开发中的潜在有效的辅助疗法。在当前的研究中,已就SCID小鼠的生长速率,形态和脂质体药物(Verteporfin)的摄取和分布对两种原位胰腺癌模型(AsPC-1和Panc-1)进行了表征。使用PDT荧光剂量计在体内肝脏和肿瘤中测量Verteporfin的荧光,并在尾静脉注射之前和之后一小时进行测量。荧光在约15分钟后达到平稳状态,并且在最初的一个小时内没有减少。在15分钟至24小时的时间点,切除内脏器官(肾脏,脾脏,胰腺,肿瘤,肌肉,肺,肝和皮肤),并在台风成像仪上进行扫描,分析肿瘤与正常组织中的荧光比。在每个时间点计算图像并与体内结果进行比较在冷冻切片上进行以DiOc7标记的Verteporfin与功能性脉管系统的组织分布,最终分析将确定理想的时间点,以便对动物进行光照射。在保留正常组织的同时实现最大程度的肿瘤破坏。

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