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Effect of ticlopidine in the prevention of radiation enteropathy.

机译:噻氯匹定在预防放射性肠病中的作用。

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Impairment of vascular function is considered to play an important role in chronic radiation enteropathy. In this experimental study, the role of ticlopidine, an inhibitor of ADP-induced platelet aggregation, was investigated in radiation enteropathy. 80 male Wistar albino rats, each weighing 170-200 g, were divided into four groups: (a) radiation alone (n 20); (b) radiotherapy plus ticlopidine (n (n = 20) and (d) control (n = 20). Both radiation groups received 19 Gy radiation to the exteriorized intestinal segments in a single fraction. Ticlopidine or vehicle was administered 12 h after radiotherapy and continued for 1 month. Rats from every group were euthanized randomly at intervals of 6 weeks from 2 weeks to 26 weeks. Histopathological radiation injury was assessed using radiation injury scoring (RIS). Radiation with ticlopidine or radiation alone groups showed significant RIS deterioration compared with controls in all time points studied. Comparison of median RIS of radiotherapy and radiotherapy+ticlopidine groups at the 2nd, 14th and 26th weeks yielded statistically significant RIS in favour of radiotherapy+ticlopidine group (p = 0.05). However, these differences were less pronounced at the 8th and 20th week (p = 0.07). Both radiation groups had poor weight gain when compared with control and ticlopidine groups. The weight gain in radiotherapy+ticlopidine group was significantly superior to only radiation group between 10th and 20th weeks (p = 0.05). This study showed that inhibition of platelet aggregation with ticlopidine might be useful in radiation enteropathy. However, the precise role of antiaggregant therapies on radiation enteropathy should be comprehensively studied before clinical consideration.
机译:血管功能障碍被认为在慢性放射性肠病中起重要作用。在这项实验研究中,研究了噻氯匹定(ADP诱导的血小板聚集的抑制剂)在放射性肠病中的作用。将80只雄性Wistar白化病大鼠(每只重170-200 g)分为四组:(a)单独辐射(n = 20); (b)放疗加噻氯匹定(n(n = 20)和(d)对照(n = 20)。两个放疗组均在单个部分中对外部肠段接受19 Gy放疗,在放疗后12 h给予噻氯匹定或溶媒并持续1个月,每组从2周到26周的6周间隔内,对每组大鼠进行安乐死,使用放射损伤评分(RIS)评估组织病理学放射损伤,与噻氯匹定或单独放射组相比,放射显着恶化在第2、14和26周放疗和放疗+噻氯匹定组的中位RIS比较,在统计学上有显着的RIS,有利于放疗+噻氯匹定组(p = 0.05),但是这些差异较小在第8周和第20周时明显(p = 0.07)。与对照组和噻氯匹定相比,两个放疗组的体重增加均较差。在第10周和第20周之间,iotherapy +噻氯匹定组显着优于仅放疗组(p = 0.05)。这项研究表明,噻氯匹定抑制血小板聚集可能对放射性肠病有用。但是,在临床考虑之前,应全面研究抗凝治疗在放射性肠病中的确切作用。

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