奥利司他对Wistar大鼠凝血酶原时间和部分凝血活素时间的影响

Mohammad Mahdi Tavana, Taha Yegani, S. Hajiaghajani
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引用次数: 1

摘要

背景:奥利司他是少数被FDA批准的抗肥胖药物之一。它通过可逆抑制胃肠道脂肪酶使治疗剂量的脂质吸收减少30%。目的:由于维生素K(一种脂溶性维生素)在凝血级联因子2,7,9和10的合成中起重要作用,我们假设脂质吸收减少可导致维生素K吸收不良,从而导致凝血功能障碍。实验对象:Wistar大鼠18只,分为三组。为了验证我们的假设,我们决定给Wistar大鼠奥利司他(以酒精溶液的形式),为期一周,一个月和三个月。因此,我们将其分为三组:仅用水的对照组1组,用水和酒精的对照组2组,用水、酒精和奥利司他作为饮料的对照组3组。在测量每只大鼠的PT和PTT后,我们使用变异的单向分析对结果进行分析。结果:PT和PTT在每个系列实验中都没有遵循可预测的模式,因此不可能在不同系列实验之间进行比较。但在每三个系列中,由于奥利司他的消耗,PT和PTT均增加,并且对照2与病例组之间差异的显著性随着实验时间的延长而增加。在1周、1个月和3个月的试验中,PTT的显著性分别为0.905、0.820和0.495,PTT的显著性分别为0.888、0.734和0.538。结论:我们的研究结果显示,在我们的研究期间(<3个月),奥利司他对PT和PTT均无显著影响。然而,可以预见的是,更长时间的奥利司他消耗可能导致PT和PTT的显著影响。
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Effect of Orlistat on Prothrombin Time (PT) and Partial Thromboplastin Time (PTT) in Wistar Rats
Context: Orlistat is one of the few anti-obesity drugs that have been approved by FDA. It reduces the lipid absorption by 30% in its therapeutic dose by means of reversible inhibition of gastrointestinal lipases. Objective: Since vitamin K (a lipid soluble vitamin) is important in the synthesis of factors 2, 7, 9 and 10 of the coagulation cascade, we hypothesized that reduction in lipid absorption can cause vitamin K malabsorption and thus coagulation dysfunction. Subject: 18 Wistar rats divided in three groups. For the purpose of testing our hypothesis, we decided to give Orlistat to Wistar rats (in the form of solution in alcohol), for one week, one month and three months. Thus we made three groups including Control 1 group which only used water, Control 2 group which used water and alcohol and control 3 groups which used water, alcohol and Orlistat as its drink. After measuring PT and PTT of each rat, we used one way analysis of variants for the analysis of the results. Results: PT and PTT didn’t follow a predictable pattern through each series of experiments and therefore comparison wasn’t possible between different series of experiments. However, in every three series, both PT and PTT increased as a result of Orlistat consumption and the significancy of difference between control 2 and case group increased as the time of experiments got longer. This mentioned significancy was 0.905, 0.820 and 0.495 for PT, and 0.888, 0.734 and 0.538 for PTT during one week, one month and three months experiment, respectively. Conclusion: Our results showed that Orlistat didn’t have a significant effect on neither PT nor on PTT in the duration of our research (<3 months). However, it can be predicted that longer times of Orlistat consumption may lead to significant effects on PT and PTT.
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