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首页> 外文期刊>Journal of Translational Medicine >Characterization of terminal-ileal and colonic Crohn’s disease in treatment-na?ve paediatric patients based on transcriptomic profile using logistic regression
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Characterization of terminal-ileal and colonic Crohn’s disease in treatment-na?ve paediatric patients based on transcriptomic profile using logistic regression

机译:基于转录组剖面的治疗 - Naα患者末端 - 髂骨和结肠克罗恩病的表征

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摘要

Inflammatory bowel disease (IBD) is a chronic and idiopathic inflammatory disorder of the gastrointestinal tract and comprises ulcerative colitis (UC) and Crohn’s disease (CD). Crohn’s disease can affect any part of the gastrointestinal tract, but mainly the terminal ileum and colon. In the present study, we aimed to characterize terminal-ileal CD (ICD) and colonic CD (CCD) at the molecular level, which might enable a more optimized approach for the clinical care and scientific research of CD. We analyzed differentially expressed genes in samples from 23 treatment-na?ve paediatric patients with CD and 25 non-IBD controls, and compared the data with previously published RNA-Seq data using multi-statistical tests and confidence intervals. We implemented functional profiling and proposed statistical methods for feature selection using a logistic regression model to identify genes that are highly associated in ICD or CCD. We also validated our final candidate genes in independent paediatric and adult cohorts. We identified 550 genes specifically expressed in patients with CD compared with those in healthy controls (p??0.05). Among these DEGs, 240 from patients with CCD were mainly involved in mitochondrial dysfunction, whereas 310 from patients with ICD were enriched in the ileum functions such as digestion, absorption, and metabolism. To choose the most effective gene set, we selected the most powerful genes (p-value?≤?0.05, accuracy?≥?0.8, and AUC?≥?0.8) using logistic regression. Consequently, 33 genes were identified as useful for discriminating CD location; the accuracy and AUC were 0.86 and 0.83, respectively. We then validated the 33 genes with data from another independent paediatric cohort (accuracy?=?0.93, AUC?=?0.92) and adult cohort (accuracy?=?0.88, AUC?=?0.72). In summary, we identified DEGs that are specifically expressed in CCD and ICD compared with those in healthy controls and patients with UC. Based on the feature selection analysis, 33 genes were identified as useful for discriminating CCD and ICD with high accuracy and AUC, for not only paediatric patients but also independent cohorts. We propose that our approach and the final gene set are useful for the molecular classification of patients with CD, and it could be beneficial in treatments based on disease location.
机译:炎症性肠病(IBD)是胃肠道的慢性和特发性炎症疾病,包括溃疡性结肠炎(UC)和CROHN疾病(CD)。克罗恩病可以影响胃肠道的任何部分,但主要是终端回肠和结肠。在本研究中,我们的目的是在分子水平下表征末端 - 髂曲线CD(ICD)和结肠CD(CCD),这可能能够更优化的临床护理和CD的科学研究方法。我们分析了来自CD和25个非IBD对照的23例治疗-NA ve患者的样品中的差异表达基因,并使用多统计测试和置信区间将数据与先前公布的RNA-SEQ数据进行了比较。我们利用逻辑回归模型实现了功能分析和建议的特征选择统计方法,以识别ICD或CCD中高度相关的基因。我们还验证了我们在独立的儿科和成人队列中的最终候选基因。我们确定了与CD患者特异性表达的550个基因,与健康对照(P = 0.05)相比。在这些DEG中,来自CCD患者的240名主要涉及线粒体功能障碍,而ICD患者310则富集在回肠功能,例如消化,吸收和代谢。为了选择最有效的基因集,我们选择了最强大的基因(p值?≤≤0.05,精度?≥?0.8和AUC?≥?0.8)使用Logistic回归。因此,将33个基因鉴定为可辨别CD位置的有用;精度和AUC分别为0.86和0.83。然后,我们用来自另一种独立的儿科队列的数据验证了33个基因(准确性?=?= 0.93,AUC?0.92)和成人队列(准确性?=?0.88,AUC?= 0.72)。总之,与健康对照和UC患者的患者相比,我们确定了在CCD和ICD中具体表达的DEG。基于特征选择分析,33个基因被确定为具有高精度和AUC的CCD和ICD,不仅是儿科患者而且还有独立的群组。我们提出我们的方法和最终基因集可用于CD患者的分子分类,并且在基于疾病位置的治疗可能是有益的。

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