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首页> 外文期刊>The American Journal of Gastroenterology >Development and validation of a risk score for post-infectious irritable bowel syndrome.
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Development and validation of a risk score for post-infectious irritable bowel syndrome.

机译:感染后肠易激综合症风险评分的开发和验证。

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OBJECTIVES: Acute gastroenteritis (GE) is an important risk factor for the development of irritable bowel syndrome (IBS). We used observational data from the Walkerton Health Study (WHS) to develop and validate a risk score for post-infectious (PI) IBS. METHODS: Model derivation and validation were based on a split-sample method from a cohort of patients with exposure to GE (n=1,368). Study participants were randomly assigned to the derivation and validation cohorts in a 1:1 ratio. Within the derivation cohort, univariate and multivariable logistic regression were used to identify risk factors associated with IBS. The risk model was then applied to the validation cohort. Overall model performance was assessed using the area under the receiver operating curve (ROC). The risk score was developed using multivariable regression coefficients obtained from the derivation set and validated in the validation set. Classification and regression tree (CART) modeling was used to determine cutoff values for high, intermediate, and low risk based on the total score. RESULTS: Nine variables were identified as important predictors of IBS (gender, age<60, longer duration of diarrhea, increased stool frequency, abdominal cramping, bloody stools, weight loss, fever, and psychological disorders (anxiety and depression)). The discriminatory power of the risk model based on the area under ROC was 0.70 and was similar in the validation set. The risk score model showed good accuracy in both the derivation and validation sets and was able to distinguish among cohorts at low, intermediate, and high risk for developing PI-IBS. Percentages of patients with PI-IBS in the low, intermediate and high risk were 10, 35, and 60% in the derivation cohort and 17, 36, and 62% in the validation cohort. CONCLUSIONS: A simple risk tool that uses demographics and symptoms of acute GE can predict which patients with acute GE are at risk of developing PI-IBS. This tool may be used clinically to assess risk and to guide treatment.
机译:目的:急性肠胃炎(GE)是肠易激综合征(IBS)发展的重要危险因素。我们使用了来自Walkerton Health Study(WHS)的观察数据来开发和验证感染后(PI)IBS的风险评分。方法:模型的推导和验证是基于拆分样本方法,该方法来自一组暴露于GE(n = 1368)的患者。将研究参与者以1:1的比例随机分配到派生和验证队列中。在派生队列中,单变量和多变量logistic回归用于确定与IBS相关的危险因素。然后将风险模型应用于验证队列。使用接收器工作曲线(ROC)下的面积评估整体模型性能。使用从衍生集获得并在验证集中进行验证的多元回归系数来开发风险评分。分类和回归树(CART)建模用于根据总得分确定高,中和低风险的临界值。结果:九个变量被确定为IBS的重要预测指标(性别,年龄<60岁,腹泻时间更长,大便次数增加,腹部绞痛,大便血腥,体重减轻,发烧和心理疾病(焦虑和抑郁))。基于ROC下面积的风险模型的判别力为0.70,在验证集中相似。风险评分模型在派生和验证集上均显示出良好的准确性,并且能够区分发生PI-IBS的低,中和高风险人群。在低,中和高风险中,PI-IBS患者的比例在派生队列中分别为10%,35%和60%,在验证队列中分别为17%,36%和62%。结论:使用人口统计学和急性GE症状的简单风险工具可以预测哪些急性GE患者有发展PI-IBS的风险。该工具可在临床上用于评估风险和指导治疗。

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