2024 年及以后的炎症性肠病

IF 6.6 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Alimentary Pharmacology & Therapeutics Pub Date : 2024-10-15 DOI:10.1111/apt.18295
Richard B. Gearry, Cynthia H. Seow, Sreedhar Subramanian
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Looking back through the journal listings, this is the ninth special edition focused on IBD, but the first for 16 years. As associate editors, we are proud of this collection of cutting-edge reviews written by an exceptional group of IBD experts, all with strong connections to the journal.</p><p>In 1987, the possibility of disease prevention would have seemed fanciful. However, as we learn from prevention trials in type 1 diabetes mellitus and rheumatoid arthritis, several critical steps have emerged that need to be followed if we are to advance prediction and prevention. Bronze et al. present a road map for how we can navigate a journey to IBD prevention via validated predictive biomarkers to develop a multi-dimensional predictive tool. While science advances, we must also be aware of ethical issues including the preferences of first-degree relatives of those with IBD and how we use predictive information. Finally, bringing together expertise and patients in high-risk clinics should enable appropriate prevention trials.<span><sup>2</sup></span></p><p>The question as to what comprises severe IBD has been one that has long vexed clinicians and patients with IBD. Over time, interest has moved from symptoms to both markers of inflammation (endoscopic, histologic and biomarkers) and a more holistic view (quality of life, disability and psychosocial health). Swaminathan et al. walk us through these concepts before defining disease severity and how this includes all these facets of IBD. Understanding how these interact enables clinicians to focus on specific therapeutic targets and improve outcomes for individuals with IBD.<span><sup>3</sup></span></p><p>Understanding the wider burden of disease includes a focus on the gut–brain axis in patients with IBD. Riggott et al. describe the bi-directional relationship between psychological wellbeing and adverse longitudinal disease activity outcomes, and the high prevalence of irritable bowel syndrome-type symptoms. Treatments that target the gut–brain axis include behavioural treatments, neuromodulators and dietary interventions. Proactive management of psychological health is a critical component in the overall disease management of IBD patients.<span><sup>4</sup></span></p><p>In their review of evidence-based dietary management of IBD, Gibson et al. present the four pillars of dietary management. This paradigm provides an excellent approach to dietary strategies for patients with IBD. Firstly, nutritional status should be optimized through accurate body composition measurement and attention to sarcopenia and visceral adiposity. Secondly, exclusive enteral nutrition and the Crohn's disease exclusion diet with partial enteral nutrition are effective at reducing intestinal inflammation in patients with Crohn's disease. Thirdly, there are a range of dietary approaches to managing non-inflammatory symptoms in patients with IBD. Finally, following a healthy diet is fundamental to the general health of patients with IBD. There must also be a clear focus on the risks of nutritional inadequacy and maladaptive eating behaviours.<span><sup>5</sup></span></p><p>For more than 25 years we have used biologic drugs for the treatment of IBD. Over time the number of these has increased with more targets now in scope, and our ability to use each of these drugs smarter has led to benefits for patients. Chaemsupaphan et al. describe how biologic drugs can be optimized using therapeutic drug monitoring and measurement of neutralizing antibodies. Optimizing treatment effect increases the likelihood of clinical and deeper levels of remission in a treat-to-target paradigm. While guidelines of when to escalate and when to switch agents have emerged for the use of anti-TNF drugs, non-TNF inhibitors demonstrate less robust exposure-response relationships and therapeutic drug monitoring may not prove as beneficial.<span><sup>6</sup></span></p><p>In the final paper in this special edition, Noor et al. provide a pragmatic guide for clinicians on recently approved and emerging therapies and address key challenges of optimal sequencing and timing of treatment. For many of these new therapies, further data from long term extension studies, real world studies and head-to-head trials are needed to inform long term safety and sequencing strategies.<span><sup>7</sup></span></p><p>We would like to thank the 24 authors from eight countries for contributing to this special edition of <i>Alimentary Pharmacology and Therapeutics</i>. 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引用次数: 0

摘要

1 引言 1987 年,罗伊-庞德(Roy Pounder)教授创办了《食品药理学与治疗学》(Alimentary Pharmacology and Therapeutics)杂志,并作为资深作者在该杂志上发表了一篇关于环孢素治疗克罗恩病的回顾性研究报告。37 年来,《食品药理学与治疗学》通过 60 卷高质量的出版物为肠胃病学家提供了广泛的临床相关期刊文章。我们为本期《食品药理学与治疗学》IBD 特刊收集的期刊文章反映了这些文章的广泛性。回顾期刊列表,这是第九期以 IBD 为主题的特刊,但却是 16 年来第一期。作为副主编,我们为这本由一群出色的 IBD 专家撰写的前沿综述集感到自豪,他们都与本刊有着密切的联系。然而,随着我们从 1 型糖尿病和类风湿性关节炎的预防试验中吸取经验教训,我们发现,如果要推进预测和预防工作,就必须遵循几个关键步骤。Bronze 等人提出了一个路线图,告诉我们如何通过经过验证的预测性生物标记物来开发多维预测工具,从而实现 IBD 预防。在科学进步的同时,我们也必须意识到伦理问题,包括 IBD 患者一级亲属的偏好以及我们如何使用预测信息。最后,将专家和高危诊所的患者聚集在一起,应能进行适当的预防试验。2 什么是严重 IBD 一直是困扰临床医生和 IBD 患者已久的问题。随着时间的推移,人们的兴趣已经从症状转移到炎症标志物(内窥镜、组织学和生物标志物)和更全面的视角(生活质量、残疾和社会心理健康)。斯瓦米纳坦等人在定义疾病严重性之前向我们介绍了这些概念,以及疾病严重性如何包括 IBD 的所有这些方面。了解了这些方面如何相互作用,临床医生就能将重点放在特定的治疗目标上,并改善 IBD 患者的预后。Riggott 等人描述了心理健康与不利的纵向疾病活动结果之间的双向关系,以及肠易激综合征类型症状的高患病率。针对肠-脑轴的治疗包括行为治疗、神经调节剂和饮食干预。积极的心理健康管理是 IBD 患者整体疾病管理的重要组成部分。4 Gibson 等人在对 IBD 循证饮食管理的综述中提出了饮食管理的四大支柱。这一范式为 IBD 患者的饮食策略提供了极好的方法。首先,应通过精确测量身体成分、关注肌肉疏松症和内脏脂肪症来优化营养状况。其次,纯肠内营养和克罗恩病排除饮食加部分肠内营养可有效减轻克罗恩病患者的肠道炎症。第三,有一系列饮食方法可以控制 IBD 患者的非炎症性症状。最后,健康的饮食是 IBD 患者总体健康的基础。我们还必须明确关注营养不足和不良饮食行为的风险。5 25 年多来,我们一直在使用生物制剂药物治疗 IBD。随着时间的推移,生物制剂药物的数量在不断增加,现在有了更多的靶点。Chaemsupaphan等人描述了如何利用治疗药物监测和中和抗体测量来优化生物药物。在 "对靶治疗 "范式中,优化治疗效果可提高临床缓解和更深层次缓解的可能性。6 在本特刊的最后一篇论文中,Noor 等人为临床医生提供了一份实用指南,介绍了最近批准的新疗法,并探讨了最佳治疗顺序和时机的关键问题。对于这些新疗法中的许多疗法,还需要从长期扩展研究、实际研究和头对头试验中获得更多数据,以便为长期安全性和排序策略提供依据。 7我们要感谢来自八个国家的 24 位作者为《食品药理学与治疗学》这一特刊所做的贡献。我们希望您能喜欢阅读这些有思想的论文,以及今后在《食品药理学与治疗学》上发表的其他作品。
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Inflammatory bowel disease in 2024 and beyond

In 1987, Professor Roy Pounder launched Alimentary Pharmacology and Therapeutics and in that very issue, he was the senior author on a retrospective study of cyclosporin for the management of Crohn's disease.1 Since that time, the incidence and prevalence of inflammatory bowel disease (IBD) has risen exponentially, reaching all corners of the globe and all ethnicities. Alimentary Pharmacology and Therapeutics has provided gastroenterologists with a broad spectrum of clinically relevant journal articles for 37 years through 60 volumes of high-quality publications. The breadth of these is reflected in the range of journal articles that we have assembled for this special IBD edition of Alimentary Pharmacology and Therapeutics. Looking back through the journal listings, this is the ninth special edition focused on IBD, but the first for 16 years. As associate editors, we are proud of this collection of cutting-edge reviews written by an exceptional group of IBD experts, all with strong connections to the journal.

In 1987, the possibility of disease prevention would have seemed fanciful. However, as we learn from prevention trials in type 1 diabetes mellitus and rheumatoid arthritis, several critical steps have emerged that need to be followed if we are to advance prediction and prevention. Bronze et al. present a road map for how we can navigate a journey to IBD prevention via validated predictive biomarkers to develop a multi-dimensional predictive tool. While science advances, we must also be aware of ethical issues including the preferences of first-degree relatives of those with IBD and how we use predictive information. Finally, bringing together expertise and patients in high-risk clinics should enable appropriate prevention trials.2

The question as to what comprises severe IBD has been one that has long vexed clinicians and patients with IBD. Over time, interest has moved from symptoms to both markers of inflammation (endoscopic, histologic and biomarkers) and a more holistic view (quality of life, disability and psychosocial health). Swaminathan et al. walk us through these concepts before defining disease severity and how this includes all these facets of IBD. Understanding how these interact enables clinicians to focus on specific therapeutic targets and improve outcomes for individuals with IBD.3

Understanding the wider burden of disease includes a focus on the gut–brain axis in patients with IBD. Riggott et al. describe the bi-directional relationship between psychological wellbeing and adverse longitudinal disease activity outcomes, and the high prevalence of irritable bowel syndrome-type symptoms. Treatments that target the gut–brain axis include behavioural treatments, neuromodulators and dietary interventions. Proactive management of psychological health is a critical component in the overall disease management of IBD patients.4

In their review of evidence-based dietary management of IBD, Gibson et al. present the four pillars of dietary management. This paradigm provides an excellent approach to dietary strategies for patients with IBD. Firstly, nutritional status should be optimized through accurate body composition measurement and attention to sarcopenia and visceral adiposity. Secondly, exclusive enteral nutrition and the Crohn's disease exclusion diet with partial enteral nutrition are effective at reducing intestinal inflammation in patients with Crohn's disease. Thirdly, there are a range of dietary approaches to managing non-inflammatory symptoms in patients with IBD. Finally, following a healthy diet is fundamental to the general health of patients with IBD. There must also be a clear focus on the risks of nutritional inadequacy and maladaptive eating behaviours.5

For more than 25 years we have used biologic drugs for the treatment of IBD. Over time the number of these has increased with more targets now in scope, and our ability to use each of these drugs smarter has led to benefits for patients. Chaemsupaphan et al. describe how biologic drugs can be optimized using therapeutic drug monitoring and measurement of neutralizing antibodies. Optimizing treatment effect increases the likelihood of clinical and deeper levels of remission in a treat-to-target paradigm. While guidelines of when to escalate and when to switch agents have emerged for the use of anti-TNF drugs, non-TNF inhibitors demonstrate less robust exposure-response relationships and therapeutic drug monitoring may not prove as beneficial.6

In the final paper in this special edition, Noor et al. provide a pragmatic guide for clinicians on recently approved and emerging therapies and address key challenges of optimal sequencing and timing of treatment. For many of these new therapies, further data from long term extension studies, real world studies and head-to-head trials are needed to inform long term safety and sequencing strategies.7

We would like to thank the 24 authors from eight countries for contributing to this special edition of Alimentary Pharmacology and Therapeutics. We hope that you will enjoy reading these thoughtful papers and other work published in Alimentary Pharmacology and Therapeutics in the future.

Richard B. Gearry: Conceptualization; writing – original draft; writing – review and editing; visualization; project administration. Cynthia H. Seow: Conceptualization; writing – review and editing; project administration. Sreedhar Subramanian: Conceptualization; writing – review and editing; visualization; project administration.

R.B.G. has received research grants, served on advisory boards or received honoraria for educational activities for Janssen, AbbVie and Zespri (unrelated to this manuscript). C.H.S has received research grants, served on advisory boards or received honoraria from Janssen, AbbVie, Takeda, Lilly, Ferring, Shire, Pfizer, Sandoz, Pharmascience, Fresenius Kabi and Amgen, Bristol Myers Squibb, ACHRI, CIHR, Calgary Health Trust, New South Wales Government Health. S.S. has received research grants, served on advisory boards or received honoraria from MSD, Ipsen, AbbVie, Dr. Falk pharmaceuticals, Takeda, Janssen, Celltrion and Vifor pharmacceuticals.

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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.
期刊最新文献
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