Strande Vibeke, Hagen Milada, Lund Charlotte, Asak Øyvind, Bengtson May-Bente, Boyar Raziye, Detlie Trond Espen, Frigstad Svein Oskar, Henriksen Magne, Holten Kristina I Aass, Hovde Øistein, Huppertz-Hauss Gert, Høie Ole, Johansen Ingunn, Medhus Asle W, Olsen Bjørn Christian, Opheim Randi, Perminow Gøri, Ricanek Petr, Torp Roald, Valeur Jørgen, Vatn Simen, Aabrekk Tone Bergene, Moum Bjørn, Høivik Marte Lie, Kristensen Vendel A
Unger-Vetlesen Institute, Lovisenberg Diaconal Hospital, Oslo, Norway.
Institute of Clinical Medicine, University of Oslo, Oslo, Norway.
Scand J Gastroenterol. 2025 Jul;60(7):716-727. doi: 10.1080/00365521.2025.2512591. Epub 2025 Jun 8.
Identifying patients at risk of developing severe inflammatory bowel disease (IBD) can aid treatment decisions. However, predicting disease course remains challenging. We aimed to identify predictive factors associated with severe disease course in the first year after IBD diagnosis.
Newly diagnosed adult (≥18 years) patients with IBD were recruited from a population-based inception cohort (IBSEN III study). Preselected baseline factors were tested for associations with severe disease course, defined as IBD-related hospitalisation, surgery, treatment with ≥2 steroid courses, >2 biologics and/or new event of complication (stricture, fistula, abscess only applicable Crohn's disease (CD)). From a best fitted multivariable logistic regression model stratified by diagnosis and age (18-40/>40 years), probability of severe disease for given combinations of predictive factors was summarised in prediction matrices.
At one-year follow-up, 90/559 (16%) patients with ulcerative colitis (UC) and 74/312 (24%) with CD had severe disease. Treatment with systemic steroids, vitamin D deficiency, Simple Clinical Colitis Activity Index >2, and hypoalbuminemia at diagnosis were all significantly associated with severe disease in UC patients. CD patients with stricturing or penetrating disease behaviour, systemic steroids and hypoalbuminemia at diagnosis were associated with severe disease course. The least favourable combination of these factors increased the probability of severe disease from 3% (95%CI[0-5%]) to 72% (95%CI[66-79%]) for UC and from 8% (95%CI[3-13%]) to 88% (95%CI[84-93%]) for CD.
Our study identified predictive factors associated with severe disease the first year after diagnosis. The probability of severe disease summarised in matrices enables easy risk stratification.
识别有发展为重度炎症性肠病(IBD)风险的患者有助于治疗决策。然而,预测疾病进程仍然具有挑战性。我们旨在确定与IBD诊断后第一年的重度疾病进程相关的预测因素。
从基于人群的起始队列(IBSEN III研究)中招募新诊断的成年(≥18岁)IBD患者。对预先选定的基线因素进行测试,以确定其与重度疾病进程的关联,重度疾病进程定义为与IBD相关的住院、手术、接受≥2个疗程的类固醇治疗、>2种生物制剂治疗和/或新的并发症事件(狭窄、瘘管、脓肿,仅适用于克罗恩病(CD))。从按诊断和年龄(18 - 40/ >40岁)分层的最佳拟合多变量逻辑回归模型中,在预测矩阵中总结给定预测因素组合的重度疾病概率。
在一年的随访中,90/559(16%)例溃疡性结肠炎(UC)患者和74/312(24%)例CD患者患有重度疾病。诊断时接受全身类固醇治疗、维生素D缺乏、简易临床结肠炎活动指数>2以及低白蛋白血症均与UC患者的重度疾病显著相关。诊断时具有狭窄或穿透性疾病行为、接受全身类固醇治疗以及低白蛋白血症的CD患者与重度疾病进程相关。这些因素最不利的组合使UC患者的重度疾病概率从3%(95%CI[0 - 5%])增加到72%(95%CI[66 - 79%]),使CD患者的重度疾病概率从8%(95%CI[3 - 13%])增加到88%(95%CI[84 - 93%])。
我们的研究确定了与诊断后第一年的重度疾病相关的预测因素。矩阵中总结的重度疾病概率有助于轻松进行风险分层。
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