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In vivo evaluation of the antimutagenic and antigenotoxic effects of β-glucan extracted from Saccharomyces cerevisiae in acute treatment with multiple doses

机译:从酿酒酵母中提取的β-葡聚糖在多剂量急性治疗中的抗突变和抗原毒性的体内评价

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摘要

Ample evidence suggests that cancer is triggered by mutagenic damage and diets or supplements capable of reducing such incidences can be related to the prevention of neoplasy development or to an improvement in life quality of patients who undergo chemotherapy. This research aimed to evaluate the antimutagenic and antigenotoxic activity of β-glucan. We set up 8 experimental groups: control (Group 1), cyclophosphamide (Group 2), Groups 3–5 to assess the effect of β-glucan administration, and Groups 6–8 to evaluate the association between cyclophosphamide and β-glucan. The intraperitonial concentrations of β-glucan used were 100, 150 and 200 mg/kg. Micronucleus and comet assays showed that within the first week of treatment β-glucan presented a damage reduction rate between 100–62.04% and 94.34–59.52% for mutagenic and genotoxic damages, respectively. This activity decreased as the treatment was extended. During the sixth week of treatment antimutagenicity rates were reduced to 59.51–39.83% and antigenotoxicity was not effective. This leads to the conclusion that the efficacy of β-glucan in preventing DNA damage is limited when treatment is extended, and that its use as a chemotherapeutic adjuvant need to be better clarified.
机译:大量证据表明,癌症是由诱变性损害触发的,能够减少此类发生率的饮食或补品可能与预防瘤形成发展或改善接受化疗的患者的生活质量有关。这项研究旨在评估β-葡聚糖的抗突变和抗原毒性活性。我们设置了8个实验组:对照组(第1组),环磷酰胺(第2组),第3-5组以评估β-葡聚糖的给药效果,第6-8组以评估环磷酰胺和β-葡聚糖之间的关系。腹膜内使用的β-葡聚糖的浓度为100、150和200 mg / kg。微核和彗星试验表明,在治疗的第一周内,β-葡聚糖对诱变和遗传毒性的损害减少率分别为100-62.04%和94.34-59.52%。随着治疗时间的延长,该活性降低。在治疗的第六周,抗致突变率降低到59.51–39.83%,抗原毒性无效。由此可得出结论:随着治疗的延长,β-葡聚糖防止DNA损伤的功效受到限制,需要进一步阐明其作为化学治疗佐剂的用途。

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