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首页> 外文期刊>The Journal of Urology >Photodynamic therapy as novel nephron sparing treatment option for small renal masses
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Photodynamic therapy as novel nephron sparing treatment option for small renal masses

机译:光动力疗法是小肾脏肿块的一种新的保留肾单位的治疗选择

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摘要

Purpose: Photodynamic therapy has great potential as nephron sparing therapy for small renal masses. Using mTHPC [meso-tetra(hydroxyphenyl)chlorin] (BioLitec Pharma, Dublin, Ireland), a photosensitizer that targets vasculature and tissue, we determined whether renal tumors could be ablated using mTHPC mediated photodynamic therapy in a translational renal carcinoma mouse model. Materials and Methods: We administered mTHPC intravenously in kidney tumor bearing mice. Tumor diameter was about 7 mm. At several drug-light intervals a cylindrical laser fiber was placed intratumorally for interstitial illumination using a wavelength of 652 nm. We determined mTHPC biodistribution up to 48 hours after administration and tumor destruction after mTHPC mediated photodynamic therapy. In vitro mTHPC uptake and photodynamic therapy induced cytotoxicity were studied in human endothelial, renal and renal cell carcinoma cell lines. Results: Ablated regions with a maximum diameter of 9.3 mm and complete loss of cell viability were observed at a drug-light interval of 4 hours, when mTHPC was increased in blood and tissue. Viable renal tissue remained detectable outside the illuminated area. In endothelial cells mTHPC uptake and sensitivity to photodynamic therapy were increased compared to those in renal cell carcinoma and renal cells. Conclusions: mTHPC mediated photodynamic therapy is a nephron sparing therapy. The extent of renal tumor destruction is adequate for clinical translation. Localization of mTHPC in tumor vasculature and tissue produces a strong combined effect. Our findings justify further preclinical studies of the applicability of photodynamic therapy for renal cell carcinoma before photodynamic therapy can become a valuable addition to current minimally invasive treatments of small renal masses.
机译:目的:光动力疗法作为小肾脏肿块的肾保留疗法具有巨大潜力。使用靶向血管和组织的光敏剂mTHPC [间-四(羟苯基)二氢卟酚](BioLitec Pharma,爱尔兰都柏林),我们确定了在转化型肾癌小鼠模型中,是否可以使用mTHPC介导的光动力疗法消融肾肿瘤。材料和方法:我们在患有肾肿瘤的小鼠中静脉内施用mTHPC。肿瘤直径约为7mm。在几个药物光间隔处,将圆柱形激光纤维瘤内放置以使用652 nm波长进行间隙照明。我们确定了给药后48小时内mTHPC的生物分布以及mTHPC介导的光动力治疗后肿瘤的破坏。在人内皮,肾和肾细胞癌细胞系中研究了体外mTHPC摄取和光动力疗法诱导的细胞毒性。结果:当血液和组织中的mTHPC增加时,在4小时的药物光照间隔观察到最大直径为9.3 mm的消融区域,并且细胞活力完全丧失。在照明区域外仍可检测到存活的肾组织。与肾细胞癌和肾细胞相比,内皮细胞中mTHPC的摄取和对光动力疗法的敏感性增加。结论:mTHPC介导的光动力疗法是一种保护肾单位的疗法。肾肿瘤破坏的程度足以进行临床翻译。 mTHPC在肿瘤血管和组织中的定位产生强大的联合作用。我们的发现证明在光动力疗法可以成为当前对小肾脏肿块的微创治疗的有价值的补充之前,对光动力疗法在肾细胞癌中的适用性进行进一步的临床前研究是合理的。

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