Editorial: Cumulative Impact of Clinical Disease Activity, Biochemical Activity and Psychological Health on the Natural History of Inflammatory Bowel Disease During 8 Years of Longitudinal Follow-Up. Authors' Reply

IF 6.6 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Christy Riggott, Keeley M. Fairbrass, David J. Gracie, Alexander C. Ford
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引用次数: 0

Abstract

We would like to thank Drs Massouridis and Swaminathan for their editorial dealing with our article and welcome this opportunity for further discussion [1, 2]. Bi-directionality of gut–brain axis communications has been highlighted consistently in inflammatory bowel disease (IBD), with both a high prevalence of symptoms of common mental disorders (CMD) and an association between the presence of these symptoms and future adverse disease outcomes [3]. Although poor psychological health is most apparent during periods of disease activity, the prevalence of symptoms compatible with a CMD remains twice that of the general population even in quiescent disease, suggesting factors beyond inflammatory burden contribute to their development [1, 3]. Furthermore, a recently published longitudinal follow-up study examining trajectories of these symptoms in patients with IBD demonstrates that abnormal anxiety and depression scores persist in almost half of patients, suggesting poor psychological health is a constant for many patients [4]. Psychological health may, therefore, be an important therapeutic target in IBD.

A biopsychosocial model of care is advocated for patients with irritable bowel syndrome (IBS), including access to brain–gut behavioural therapies and gut–brain neuromodulators to manage the associated symptoms [5, 6]. With the current lack of focus on psychological health in IBD management guidelines, holistic care models are yet to translate to routine IBD care. A substantial barrier to the implementation of such models is a lack of informative research. Few randomised controlled trials (RCTs) have assessed the effects of brain–gut behavioural therapies or gut–brain neuromodulators in patients with IBD with pre-existing psychological co-morbidity, who are the patient group most likely to benefit from the addition of such therapies [7]. In addition, identifying patients with symptoms of a CMD may be difficult given the time-sensitive nature of routine IBD care, where the focus is on managing inflammatory burden. Model-based clustering techniques incorporating measures of psychological and gastrointestinal symptom severity have identified clusters of patients with IBD and high psychological symptom burden, and could serve in clinical practice to identify subgroups of patients who may experience a benefit from brain–gut behavioural therapies or gut–brain neuromodulators [8]. Furthermore, one quarter of patients with IBD with endoscopically quiescent disease also report symptoms that are compatible with IBS [9]. Such patients, if identified in clinical practice, may also be best managed with brain–gut behavioural therapies or gut–brain neuromodulators, similar to the paradigm in IBS.

Finally, as suggested, replication of this research is required in ethnically and socioeconomically diverse cohorts [2]. In fact, the underrepresentation of ethnic minorities in all aspects of research is a significant issue, and this lack of inclusivity may, ultimately, result in healthcare inequality for these communities. This is true not only in observational research, but also in RCTs of IBD therapies, where ethnic minority representation is clearly diminished [10]. Strategies to ensure inclusivity of ethnic minority groups and participants from diverse socioeconomic backgrounds in research are essential. Qualitative research studying the barriers to participation among these groups is necessary and should be a priority.

Christy Riggott: writing – original draft. Keeley M. Fairbrass: writing – review and editing. David J. Gracie: writing – review and editing. Alexander C. Ford: writing – review and editing.

This article is linked to Riggott et al papers. To view these articles, visit https://doi.org/10.1111/apt.70068 and https://doi.org/10.1111/apt.70086.

社论:8年纵向随访期间临床疾病活动、生化活动和心理健康对炎症性肠病自然史的累积影响。作者回复
我们要感谢Massouridis博士和Swaminathan博士对我们文章的评论,并欢迎有机会进一步讨论[1,2]。在炎症性肠病(IBD)中,肠-脑轴通信的双向性一直得到强调,这既是常见精神障碍(CMD)症状的高患病率,也是这些症状的存在与未来不良疾病结局之间的关联[10]。尽管心理健康状况不佳在疾病活动期间最为明显,但即使在疾病静止期,与CMD相容的症状的患病率仍是普通人群的两倍,这表明炎症负担以外的因素有助于其发展[1,3]。此外,最近发表的一项纵向随访研究检查了IBD患者这些症状的轨迹,表明几乎一半的患者持续存在异常的焦虑和抑郁评分,这表明心理健康状况不良好是许多患者的常态。因此,心理健康可能是IBD的一个重要治疗靶点。提倡肠易激综合征(IBS)患者的生物心理社会护理模式,包括获得脑-肠行为疗法和肠-脑神经调节剂来管理相关症状[5,6]。由于目前IBD管理指南缺乏对心理健康的关注,整体护理模式尚未转化为常规IBD护理。实施这些模型的一个重大障碍是缺乏翔实的研究。很少有随机对照试验(RCTs)评估脑-肠行为疗法或肠-脑神经调节剂对已有心理合并症的IBD患者的效果,这些患者是最有可能从增加此类疗法中受益的患者群体[10]。此外,考虑到常规IBD护理的时间敏感性,识别有CMD症状的患者可能很困难,因为IBD护理的重点是控制炎症负担。结合心理和胃肠道症状严重程度测量的基于模型的聚类技术已经确定了IBD患者和高心理症状负担的患者群,并且可以在临床实践中用于确定可能从脑-肠行为疗法或肠-脑神经调节剂[8]中获益的患者亚组。此外,四分之一伴有内窥镜下静止疾病的IBD患者也报告了与IBS[9]相容的症状。如果在临床实践中发现这类患者,也可能最好使用脑-肠行为疗法或肠-脑神经调节剂进行治疗,类似于肠易激综合征的范例。最后,正如建议的那样,需要在种族和社会经济不同的队列中重复这项研究[10]。事实上,少数民族在研究的各个方面代表性不足是一个重大问题,这种缺乏包容性可能最终导致这些社区的医疗不平等。这不仅在观察性研究中是正确的,而且在IBD治疗的随机对照试验中也是如此,其中少数民族的代表性明显减少。确保少数民族群体和来自不同社会经济背景的参与者参与研究的战略至关重要。研究这些群体参与的障碍的定性研究是必要的,应该是一个优先事项。
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来源期刊
CiteScore
15.60
自引率
7.90%
发文量
527
审稿时长
3-6 weeks
期刊介绍: Alimentary Pharmacology & Therapeutics is a global pharmacology journal focused on the impact of drugs on the human gastrointestinal and hepato-biliary systems. It covers a diverse range of topics, often with immediate clinical relevance to its readership.
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