首页> 外文期刊>The Tohoku Journal of Experimental Medicine >Potentiating effect of beta-glucans on photodynamic therapy of implanted cancer cells in mice.
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Potentiating effect of beta-glucans on photodynamic therapy of implanted cancer cells in mice.

机译:β-葡聚糖对小鼠体内植入的癌细胞的光动力治疗的增强作用。

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摘要

Photodynamic therapy (PDT) combines a drug or photosensitizer with a specific type of light to kill cancer cells. The cellular damage induced by PDT leads to activation of the DNA damage repair, which is an important factor for modulating tumor sensitivity to this treatment. beta-Glucans are natural polysaccharides that bind complement receptor 3 on the effector cells, thereby activating them to kill tumor cells during PDT. The hypothesis of the present study was that adjuvant therapy with beta-glucans would increase the efficacy of PDT. C57BL/6 female mice were subcutaneously implanted with Lewis lung carcinoma cells. Ten days after implantation, the mice were administered intravenously sodium porfimer (10 mg/kg) 24 h prior to laser irradiation, with or without oral administration of beta-glucan (400 microg/d/mouse, 5 days) from either barley, baker's yeast, or marine brown algae that contains the storage glucan, laminarin. Tumor volume and necrotic area in excised tumors were measured. The expression of proliferating cell nuclear antigen (PCNA) was determined as an indicator of the activity of the DNA damage repair system. PDT in combination with each beta-glucan significantly reduced tumor growth (P < 0.05, n = 10) and expression of PCNA (P < 0.001, n = 9), and increased necrosis in tumor tissues (P < 0.001, n = 9). Furthermore, each structurally different
机译:光动力疗法(PDT)将药物或光敏剂与特定类型的光结合在一起以杀死癌细胞。由PDT诱导的细胞损伤导致DNA损伤修复的激活,这是调节肿瘤对该治疗敏感性的重要因素。 β-葡聚糖是天然的多糖,可结合效应细胞上的补体受体3,从而激活它们以在PDT期间杀死肿瘤细胞。本研究的假设是β-葡聚糖的辅助治疗将增加PDT的疗效。 C57BL / 6雌性小鼠皮下植入Lewis肺癌细胞。植入后十天,在激光照射前24小时给小鼠静脉内静脉给予porfimer钠(10 mg / kg),无论是否口服大麦,面包师的β-葡聚糖(400 microg / d /小鼠,5天)酵母或含有储存葡聚糖,层板蛋白的海洋褐藻。测量切除的肿瘤中的肿瘤体积和坏死面积。确定增殖细胞核抗原(PCNA)的表达作为DNA损伤修复系统活性的指标。 PDT与每种β-葡聚糖组合可显着降低肿瘤生长(P <0.05,n = 10)和PCNA表达(P <0.001,n = 9),并增加肿瘤组织的坏死程度(P <0.001,n = 9)。 。此外,每种结构上不同的β-葡聚糖对PDT均具有相似的增强作用。目前的发现表明β-葡聚糖增强了对PDT的肿瘤反应,导致PDT治疗的肿瘤明显坏死并抑制了DNA损伤修复系统。

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