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Enhanced effects of aminolaevulinic acid-based photodynamic therapy through local hyperthermia in rat tumours

机译:通过局部高热对大鼠肿瘤中基于氨基乙酰丙酸的光动力疗法的增强作用

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The possibility of enhancing aminolaevulinic acid (ALA)-based photodynamic therapy (PDT) by simultaneous application of localised hyperthermia (HT) was evaluated. Treatments of rat DS-sarcomas included: (i) control, (ii) ALA administration (375?mg?kg?1, i.p.), no illumination, (iii) ‘nonthermal’ illumination, (iv) ALA-PDT: that is, ALA administration, ‘nonthermal’ illumination, (v) localised HT, 43°C, 60?min (vi) ALA-PDT+HT: ALA administration with full spectrum irradiation resulting in ALA-PDT and HT. Tumour volume was monitored for 90 days or until a target volume (3.5?ml) was reached. No differences were seen between the first three groups, with all tumours reaching the target volume by 8–11 days. A total of 13 and 15% of tumours did not reach the target volume by day 90 following HT or ALA-PDT treatment, respectively. ALA-PDT+HT showed the greatest antitumour effect (P=0.0001), with 61% of the tumours not reaching the target volume. Viability and in vitro growth were also assessed in cells from tumours excised after treatment. ALA-PDT+HT reduced the fraction of viable tumour cells by 85%, and in vitro culture showed pronounced growth delay compared to control cells. These results demonstrate an enhanced antitumour effect upon ALA+HT, which appears to involve direct cell toxicity rather than solely vascular damage.
机译:评价了同时应用局部热疗(HT)增强基于氨基乙酰丙酸(ALA)的光动力疗法(PDT)的可能性。大鼠DS肉瘤的治疗方法包括:(i)对照,(ii)ALA给药(375?mg?kg?1,ip),无光照,(iii)'非热'光照,(iv)ALA-PDT: ,ALA施用,“非热”照明,(v)局部HT,43°C,60?min(vi)ALA-PDT + HT:以全光谱照射进行ALA施用会产生ALA-PDT和HT。监测肿瘤体积90天或直至达到目标体积(3.5?ml)。前三组之间未见差异,所有肿瘤在8-11天时均达到目标体积。 HT或ALA-PDT治疗后第90天,总共有13%和15%的肿瘤未达到目标体积。 ALA-PDT + HT表现出最大的抗肿瘤作用(P = 0.0001),其中61%的肿瘤未达到目标体积。还评估了治疗后切除的肿瘤细胞的生存力和体外生长。 ALA-PDT + HT将存活的肿瘤细胞比例降低了85%,并且与对照细胞相比,体外培养显示出明显的生长延迟。这些结果证明了对ALA + HT的增强的抗肿瘤作用,这似乎涉及直接的细胞毒性而不是单纯的血管损伤。

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