一种新的癌症治疗方法,由于适当的摄取和保留动力学的四羟基苯基氯在人成纤维细胞系。

Cancer biochemistry biophysics Pub Date : 1996-04-01
F Wierrani, D Fiedler, G Schnitzhofer, J C Stewart, K Gharehbaghi, M Henry, W Grin, W Grünberger, B Krammer
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引用次数: 0

摘要

研究表明,间四羟基苯基氯是激光光动力治疗中一种有效的肿瘤靶向药物。这种方法治疗癌症的有效性取决于药物浓度、培养时间和细胞外蛋白。我们研究了mTHPC在人成纤维细胞系中的摄取和保留动力学。我们的结果清楚地表明,在37℃的孵育温度下,与20℃和4℃的孵育温度相比,细胞外mTHPC的数量有所不同。ph值总是恒定的,而不是增加的原因。此外,mTHPC在正常体温下的吸收和荧光均增加。用mTHPC (10 μ g/mL)孵育人成纤维细胞,发现细胞内mTHPC呈线性增加,24小时后达到饱和,48小时后下降,同时上清mTHPC增加。因此,我们认为PDT治疗肿瘤细胞的最佳时间是在给药后24小时,对周围正常组织的损伤最小。
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A new approach to cancer therapy due to appropriate uptake and retention kinetics of meta-tetrahydroxy-phenylchlorin in a human fibroblast cell line.

Studies have shown that meta-tetrahydroxy-phenylchlorin is an efficient tumor targeting agent for laser photodynamic therapy. The effectiveness of this approach for cancer treatment depends on drug concentration, incubation time and extracellular protein. We studied uptake and retention kinetics of mTHPC in a human fibroblast cell line. Our results clearly demonstrate a difference in the amount of extracellular mTHPC at an incubation temperature of 37 degrees C compared to 20 degrees C and 4 degrees C. pH-values were always constant and not responsible for the increase. Furthermore, both absorption and fluorescence of mTHPC increase when incubated at normal human body temperature. Incubation of human fibroblast cells with mTHPC (10 micg/mL) showed that intracellular mTHPC increases in a linear manner reaching saturation after 24 hours and declining until 48 hours with concommitant increase of supernatant mTHPC. Therefore, we believe that tumor cells can be treated optimally with PDT following a delay > 24 hours after drug administration with a minimum of damage to surrounding normal tissues.

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