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DNA damages after SIM01 photodynamics treatment

机译:SIM01光动力学处理后的DNA损伤

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Photodynamic therapy (PDT) is a new approach to cancer treatment for a variety of malignant tumors. A new photosensitizer, 2,3-dihydro-5,15-di(3,5-dihydroxyphenyl)porphyrin (SIM01), had been evaluated for its genotoxic effects on glioma cells (C6). Comet assay had been used to evaluate the potential genotoxic effect induced by SIM01 on the C6 cells. When SIM01 had been shown to be a powerful sensitizer no DNA strand break was detected in the absence of light. SIM01 localized in cytoplasm but not in the nucleus of the tumors cells, which supported the finding of undetectable DNA damage under darkness and low photodynamic dose. Cell exposure to 20 J em~(-2) after an incubation time of 2h with 0, 0.25, 0.5, 2 or 4 μg mL~(-1) induced less than 25% of cell death but significant Tail Moment changes. If DNA damage intensity increased according to SIM01 doses under light exposure, importance of repair seemed to increase proportionally to PDT-induced damage. Positive controls consisted of doxorubicin-treated C6 cells this mutagen being known to induce genetic damage. Whatever the conditions used SIM01 appeared to be less deleterious than doxorubicin. As the comet assay can not give us the certitude that no mutation, photoadducts or oxidative damage had been developed under light exposure this point will have to be verified with another mutagenicity assay. SIM01 appears to be safe from a mutagenic point of view something of importance as tumors of small volume in patients with a long lifespan are at first indicated for PDT.
机译:光动力疗法(PDT)是一种用于治疗各种恶性肿瘤的新方法。评估了一种新型光敏剂2,3-二氢-5,15-二(3,5-二羟基苯基)卟啉(SIM01)对神经胶质瘤细胞(C6)的遗传毒性作用。彗星试验已用于评估SIM01对C6细胞的潜在遗传毒性作用。当SIM01被证明是一种强大的敏化剂时,在没有光照的情况下没有检测到DNA链断裂。 SIM01位于肿瘤细胞的细胞质中而不是细胞核中,这支持在黑暗和低光动力剂量下发现不可检测的DNA损伤。在与0、0.25、0.5、2或4μgmL〜(-1)孵育2小时后,将细胞暴露于20 J em〜(-2)导致少于25%的细胞死亡,但尾巴矩变化明显。如果DNA损伤强度根据SIM01剂量在光照下增加,则修复的重要性似乎与PDT诱导的损伤成比例地增加。阳性对照由阿霉素处理过的C6细胞组成,已知该诱变剂诱导遗传损伤。无论使用哪种条件,SIM01看起来都比阿霉素具有更少的有害性。由于彗星分析无法确定我们在光照下未发生突变,光加合物或氧化损伤的确定性,因此必须使用另一种诱变性分析来验证这一点。从诱变的角度看,SIM01似乎是安全的,因为起初建议将PDT用于长寿命患者的小体积肿瘤。

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