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The effects of dosage and the routes of administrations of streptozotocin and alloxan on induction rate of type1 diabetes mellitus and mortality rate in rats

机译:链脲佐菌素和四氧嘧啶的剂量和给药途径对大鼠1型糖尿病的诱导率和死亡率的影响

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摘要

The approach and novelty of this scientific work was to formulate the appropriate Streptozotocin (STZ) and Alloxan dosage in different routes of administration to imply minimum mortality rate and high incidence of diabetes mellitus (DM) in the rat experiment model. Rats were randomly divided into STZ, Alloxan and control groups. 1-Alloxan group was divided into two subgroups: intraperitoneal (ip) subgroups which received a single dose of, 140, 120, 100 and 80 mg/kg; and the subcutaneous (sc) subgroups which received a single dose of, 120, 110, 100, 90, and 80 mg/kg. 2-STZ group was divided into four subgroups of ip route. The ip subgroup which received intraperitoneally a single dose of, 30, 35, 40 and 50 mg/kg. 3-The control group: This group received solo distilled water. The injection day was considered as the day zero. Blood glucose levels and mortality rate were recorded. Subsequently, 30 days after, the logistic regression modeling was used to evaluate the effect of the explanatory variables, the dose levels, and route approaches, on the probability of DM incidence, and mortality. According to the statistical logistic analysis for Alloxan, it is concluded that the minimum dosage needed to induce DM was 120 mg/kg by sc method (probability 0.712). In addition, the logistic analysis for STZ showed that the optimal dose-level for STZ was 40 mg/kg with ip with approximate induction of DM probability 0.764. Based on the data, male Wistar rats in which received a single dosage of Alloxan by sc injection at dose of 120 mg/kg showed the most desirable result of induction of type I DM; furthermore, those in which received STZ by ip injection at the dose of 40 mg/kg developed a persistent and optimal DM state characterized by high rate of DM induction and low- level of mortality.
机译:这项科学工作的方法和新颖性在于在不同的给药途径中制定适当的链脲佐菌素(STZ)和四氧嘧啶剂量,以暗示大鼠实验模型中的最低死亡率和糖尿病的高发生率。将大鼠随机分为STZ,四氧嘧啶和对照组。 1-Alloxan组分为两个亚组:腹膜内(ip)亚组,分别接受140、120、100和80 mg / kg的剂量;皮下(sc)亚组分别接受120、110、100、90和80 mg / kg的剂量。 2-STZ组被分为ip路由的四个子组。腹膜内接受腹膜内单剂量30、35、40和50 mg / kg的ip亚组。 3-对照组:该组接受单独蒸馏水。注射日被认为是零日。记录血糖水平和死亡率。随后,在30天后,使用逻辑回归模型评估解释变量,剂量水平和途径对DM发生率和死亡率的影响。根据对四氧嘧啶的统计逻辑分析,得出的结论是,通过sc法诱导DM所需的最低剂量为120 mg / kg(概率0.712)。此外,对STZ的逻辑分析表明,腹腔注射ip的最佳剂量水平为40 mg / kg,诱发DM的可能性约为0.764。根据这些数据,雄性Wistar大鼠通过皮下注射以120 mg / kg的剂量注射单剂量的四氧嘧啶,表现出最理想的诱导I型DM的结果。此外,那些以40 mg / kg的剂量经腹膜内注射接受STZ的患者,其持续性和最佳DM状态以DM诱导率高和死亡率低为特征。

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