TIF Guidelines for the Management of Transfusion-Dependent β-Thalassemia

IF 7.6 2区医学 Q1 HEMATOLOGY

HemaSphere Pub Date : 2025-03-05 DOI:10.1002/hem3.70095

Khaled M. Musallam, Maria Domenica Cappellini, John B. Porter, Dimitrios Farmakis, Androulla Eleftheriou, Michael Angastiniotis, Ali T. Taher

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Regrettably, access to these advances and optimal application of best practices remain largely confined to nations with robust economies, where comprehensive health and social care systems provide universal access to treatment.2 Consequently, multimorbidity and shortened survival continue to burden patients in countries with limited resources, where most of TDT patients live.3 In high-income settings, improved survival of TDT did not come without its own “side effect,” where aging allowed several previously unrecognized morbidities to manifest, especially in patients who were exposed to the harmful effects of under- or sub-optimal treatment in the past.4, 5 Thus, the “gold standard” in TDT care is now fundamentally recognized as being a multidisciplinary approach to management, preferably in expert or reference centers, and with active engagement of patients and their families.6Since its inception in 1986, the Thalassaemia International Federation (TIF) has remained committed to supporting patients/families and patient organizations, healthcare professionals, and policymakers to promote optimal care for patients with thalassemia and other hemoglobinopathies across the world. The preparation, publication, translation, and free distribution of management guidelines is a cornerstone of its educational mission. Widely recognized for their significant impact on the care of patients with TDT, and broadly endorsed by the international medical community, these guidelines serve as a critical resource for healthcare providers and a foundation upon which national policies and practices can be built.The 5th edition of TIF “Guidelines for the Management of Transfusion-Dependent β-Thalassemia (TDT)” has now become available (available for free download at: https://thalassaemia.org.cy/tif-publications/).7 In keeping with the many and multiple unmet needs of patients in different geographies, the guidelines have been carefully crafted to offer evidence-based recommendations (key points and recommendations from select chapters on diagnosis and disease management are provided in Table 1, and a summary of monitoring recommendations is provided in Supporting Information S1: Table S1) while also suggesting solutions and pathways for care in resource-limited settings. Recommendations are provided by a global and diverse group of experts with decades of experience in patient care, through 17 interconnected chapters that echo the need of “true” multidisciplinary care throughout the patient journey from childhood to adulthood. The guidelines also include a chapter dedicated to the value of patient engagement, emphasizing the transformative power of patients as informed and effective advocates for their own needs. Additionally, patients have contributed to the review of various other chapters, ensuring that issues such as lifestyle and mental health are comprehensively addressed from the patients' perspective.The advent of groundbreaking therapies for TDT in the past decade including curative gene therapy (insertion and editing) approaches as well as disease-modifying treatments approved for clinical use, have been met with great excitement and promise for a brighter future for patients worldwide. Dedicated chapters in the new guidelines present fundamentals of the design, development, and potential place in therapy for these novel agents, while also calling for further real-world evidence to address knowledge gaps. As previously stressed, the vast majority of patients are still unable to access such developments. This disparity highlights the urgent need to devise pragmatic and actionable solutions for countries, particularly those with high disease prevalence, to prioritize disease-specific policies for prevention and optimized care.We strongly encourage healthcare professionals who follow these guidelines to advocate for their full adoption and implementation within their institutions and alert their national competent health authorities about their immense value. Evidence-based practices are vital for enabling early diagnosis and effective management, a basic human right of all patients, while at the same time contributing to safeguarding the sustainability of healthcare systems, which are greatly threatened consequent to immense geopolitical, economic, environmental, and public health crises.All authors contributed to conceptualization and manuscript drafting or critical review.K. M. M. reports consultancy fees from Novartis, Bristol Myers Squibb (Celgene Corp), Agios Pharmaceuticals, CRISPR Therapeutics, Vifor Pharma, Novo Nordisk, and Pharmacosmos; and research funding from Agios Pharmaceuticals and Pharmacosmos. M. D. C. reports consultancy fees from Novartis, Bristol Myers Squibb (Celgene Corp), Vifor Pharma, and Vertex Pharmaceuticals; and research funding from Novartis, Bristol Myers Squibb (Celgene Corp), La Jolla Pharmaceutical Company, Roche, Protagonist Therapeutics, and CRISPR Therapeutics. J. B. 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引用次数: 0

Abstract

The prospect of patients with transfusion-dependent β-thalassemia (TDT), once considered a fatal childhood disorder, has completely transformed over the past 50 years.¹ This is primarily attributed to the adoption of hemovigilance in transfusion therapy, the development of effective iron chelators, the validation of non-invasive tools for monitoring organ-specific iron loading, and the introduction of multidisciplinary care. Regrettably, access to these advances and optimal application of best practices remain largely confined to nations with robust economies, where comprehensive health and social care systems provide universal access to treatment.² Consequently, multimorbidity and shortened survival continue to burden patients in countries with limited resources, where most of TDT patients live.³ In high-income settings, improved survival of TDT did not come without its own “side effect,” where aging allowed several previously unrecognized morbidities to manifest, especially in patients who were exposed to the harmful effects of under- or sub-optimal treatment in the past.^{4, 5} Thus, the “gold standard” in TDT care is now fundamentally recognized as being a multidisciplinary approach to management, preferably in expert or reference centers, and with active engagement of patients and their families.⁶

Since its inception in 1986, the Thalassaemia International Federation (TIF) has remained committed to supporting patients/families and patient organizations, healthcare professionals, and policymakers to promote optimal care for patients with thalassemia and other hemoglobinopathies across the world. The preparation, publication, translation, and free distribution of management guidelines is a cornerstone of its educational mission. Widely recognized for their significant impact on the care of patients with TDT, and broadly endorsed by the international medical community, these guidelines serve as a critical resource for healthcare providers and a foundation upon which national policies and practices can be built.

The 5th edition of TIF “Guidelines for the Management of Transfusion-Dependent β-Thalassemia (TDT)” has now become available (available for free download at: https://thalassaemia.org.cy/tif-publications/).⁷ In keeping with the many and multiple unmet needs of patients in different geographies, the guidelines have been carefully crafted to offer evidence-based recommendations (key points and recommendations from select chapters on diagnosis and disease management are provided in Table 1, and a summary of monitoring recommendations is provided in Supporting Information S1: Table S1) while also suggesting solutions and pathways for care in resource-limited settings. Recommendations are provided by a global and diverse group of experts with decades of experience in patient care, through 17 interconnected chapters that echo the need of “true” multidisciplinary care throughout the patient journey from childhood to adulthood. The guidelines also include a chapter dedicated to the value of patient engagement, emphasizing the transformative power of patients as informed and effective advocates for their own needs. Additionally, patients have contributed to the review of various other chapters, ensuring that issues such as lifestyle and mental health are comprehensively addressed from the patients' perspective.

The advent of groundbreaking therapies for TDT in the past decade including curative gene therapy (insertion and editing) approaches as well as disease-modifying treatments approved for clinical use, have been met with great excitement and promise for a brighter future for patients worldwide. Dedicated chapters in the new guidelines present fundamentals of the design, development, and potential place in therapy for these novel agents, while also calling for further real-world evidence to address knowledge gaps. As previously stressed, the vast majority of patients are still unable to access such developments. This disparity highlights the urgent need to devise pragmatic and actionable solutions for countries, particularly those with high disease prevalence, to prioritize disease-specific policies for prevention and optimized care.

We strongly encourage healthcare professionals who follow these guidelines to advocate for their full adoption and implementation within their institutions and alert their national competent health authorities about their immense value. Evidence-based practices are vital for enabling early diagnosis and effective management, a basic human right of all patients, while at the same time contributing to safeguarding the sustainability of healthcare systems, which are greatly threatened consequent to immense geopolitical, economic, environmental, and public health crises.

All authors contributed to conceptualization and manuscript drafting or critical review.

K. M. M. reports consultancy fees from Novartis, Bristol Myers Squibb (Celgene Corp), Agios Pharmaceuticals, CRISPR Therapeutics, Vifor Pharma, Novo Nordisk, and Pharmacosmos; and research funding from Agios Pharmaceuticals and Pharmacosmos. M. D. C. reports consultancy fees from Novartis, Bristol Myers Squibb (Celgene Corp), Vifor Pharma, and Vertex Pharmaceuticals; and research funding from Novartis, Bristol Myers Squibb (Celgene Corp), La Jolla Pharmaceutical Company, Roche, Protagonist Therapeutics, and CRISPR Therapeutics. J. B. P. reports honoraria from Agios Pharmaceuticals, bluebird bio, Celgene (Bristol Myers Squibb), La Jolla Pharmaceuticals, Protagonism, Silence Therapeutics, and Vifor; and is a consultant for Agios Pharmaceuticals, bluebird bio, and Celgene (Bristol Myers Squibb). D. F. reports speaker honoraria, consultation fees, and/or grants from Abbott, AstraZeneca, Bayer, Boehringer Ingelheim, Leo, Myocardial Solutions, and Roche. A. T. T. reports consultancy fees from Novo Nordisk, Bristol Myers Squibb (Celgene Corp), Agios Pharmaceuticals, Pharmacosmos, and Roche; and research funding from Novo Nordisk, Bristol Myers Squibb (Celgene Corp), Agios Pharmaceuticals, Pharmacosmos, and Roche. All competing interests are outside the present work. The remaining authors have no conflicts of interest to disclose.

Not applicable.

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输血依赖性β-地中海贫血的TIF管理指南

输血依赖性β-地中海贫血（TDT）曾被认为是一种致命的儿童疾病，但在过去的50年里，TDT患者的前景已经完全改变这主要归功于输血治疗中血液警惕的采用，有效铁螯合剂的开发，用于监测器官特异性铁负荷的非侵入性工具的验证，以及多学科护理的引入。遗憾的是，获得这些进步和最佳做法的最佳应用仍然主要局限于经济强劲的国家，在这些国家，全面的卫生和社会保健系统提供了普遍获得治疗的机会因此，在资源有限的国家，多病和缩短的生存期继续给患者带来负担，而大多数TDT患者生活在这些国家在高收入环境中，TDT生存率的提高并非没有其自身的“副作用”，其中年龄的增长使一些以前未被认识到的发病率显现出来，特别是在过去暴露于治疗不足或次优治疗的有害影响的患者中。因此，TDT治疗的“黄金标准”现在基本上被认为是一种多学科的管理方法，最好是在专家或参考中心，并有患者及其家属的积极参与。自1986年成立以来，地中海贫血国际联合会（TIF）一直致力于支持患者/家属和患者组织、医疗保健专业人员和政策制定者，以促进全球地中海贫血和其他血红蛋白疾病患者的最佳护理。管理指南的准备、出版、翻译和免费分发是其教育使命的基石。这些准则因其对TDT患者护理的重大影响而得到广泛认可，并得到国际医学界的广泛认可，是卫生保健提供者的重要资源，也是制定国家政策和做法的基础。第五版TIF“输血依赖性β-地中海贫血（TDT）管理指南”现已发布(可在以下网址免费下载：https://thalassaemia.org.cy/tif-publications/).7为了满足不同地区患者的许多和多种未满足的需求，指南经过精心编写，提供基于证据的建议(表1提供了关于诊断和疾病管理的部分章节的要点和建议，并在支持信息S1中提供了监测建议的摘要：表S1)，同时也为资源有限环境下的护理提供解决方案和途径。具有数十年患者护理经验的全球不同专家小组通过17个相互关联的章节提供建议，这些章节呼应了从儿童到成年整个患者旅程中“真正”的多学科护理需求。该指南还包括一章专门讨论患者参与的价值，强调患者作为其自身需求的知情和有效倡导者的变革力量。此外，患者还参与了对其他章节的审查，以确保从患者的角度全面解决生活方式和心理健康等问题。在过去十年中，突破性的TDT治疗方法的出现，包括治疗性基因治疗（插入和编辑）方法以及批准用于临床使用的疾病修饰治疗，已经引起了极大的兴奋，并为全球患者带来了更光明的未来。新指南中的专门章节介绍了这些新型药物的设计、开发和潜在治疗地位的基本原理，同时也呼吁进一步的现实证据来解决知识差距。如前所述，绝大多数患者仍然无法获得这种发展。这一差距突出表明，迫切需要为各国，特别是疾病流行率高的国家，制定务实和可行的解决办法，优先制定针对特定疾病的预防和优化护理政策。我们强烈鼓励遵循这些准则的卫生保健专业人员倡导在其机构内全面采用和实施这些准则，并提醒其国家主管卫生当局注意这些准则的巨大价值。基于证据的实践对于实现早期诊断和有效管理至关重要，这是所有患者的一项基本人权，同时有助于维护卫生保健系统的可持续性，这些系统因巨大的地缘政治、经济、环境和公共卫生危机而受到极大威胁。所有作者都参与了概念化和手稿起草或评论。M . M。报告诺华、百时美施贵宝（Celgene Corp）、Agios Pharmaceuticals、CRISPR Therapeutics、Vifor Pharma、诺和诺德（Novo Nordisk）和Pharmacosmos的咨询费用；以及Agios制药公司和Pharmacosmos公司的研究经费。m.d.报告诺华、百时美施贵宝（Celgene Corp）、Vifor Pharma和Vertex Pharmaceuticals的咨询费；以及诺华公司、布里斯托尔施贵宝公司（Celgene Corp）、La Jolla制药公司、罗氏公司、主角治疗公司和CRISPR治疗公司的研究资金。j.b.p.报告了Agios制药、bluebird bio、Celgene （Bristol Myers Squibb）、La Jolla制药、主角主义、Silence Therapeutics和Vifor的荣誉报告；他是Agios制药公司、bluebird bio公司和Celgene公司（Bristol Myers Squibb）的顾问。dr . F.报告雅培、阿斯利康、拜耳、勃林格殷格翰、利奥、心肌解决方案和罗氏的演讲者酬金、咨询费和/或资助。a.t.t.报告了诺和诺德（Novo Nordisk）、百时美施贵宝（Bristol Myers Squibb, Celgene Corp）、Agios Pharmaceuticals、Pharmacosmos和罗氏（Roche）的咨询费；以及诺和诺德、百时美施贵宝（新基公司）、Agios制药、Pharmacosmos和罗氏的研究资金。所有相互冲突的利益都不在当前的工作范围之内。其余作者没有任何利益冲突需要披露。不适用。

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来源期刊

HemaSphere Medicine-Hematology

CiteScore

6.10

自引率

4.50%

发文量

2776

审稿时长

7 weeks

期刊介绍： HemaSphere, as a publication, is dedicated to disseminating the outcomes of profoundly pertinent basic, translational, and clinical research endeavors within the field of hematology. The journal actively seeks robust studies that unveil novel discoveries with significant ramifications for hematology. In addition to original research, HemaSphere features review articles and guideline articles that furnish lucid synopses and discussions of emerging developments, along with recommendations for patient care. Positioned as the foremost resource in hematology, HemaSphere augments its offerings with specialized sections like HemaTopics and HemaPolicy. These segments engender insightful dialogues covering a spectrum of hematology-related topics, including digestible summaries of pivotal articles, updates on new therapies, deliberations on European policy matters, and other noteworthy news items within the field. Steering the course of HemaSphere are Editor in Chief Jan Cools and Deputy Editor in Chief Claire Harrison, alongside the guidance of an esteemed Editorial Board comprising international luminaries in both research and clinical realms, each representing diverse areas of hematologic expertise.