Performing clinical drug trials in children with a rare disease

Victoria Hedley, Rebecca Leary, Anando Sen, Anna Irvin, Emma Heslop, Volker Straub
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Abstract

Over the past 50 years, the advancements in medical and health research have radically changed the epidemiology of health conditions in neonates, children, and adolescents; and clinical research has on the whole, moved forward. However, large sections of the pediatric community remain vulnerable and underserved, by clinical research. One reason for this is the fact that most pediatric diseases are also rare diseases (i.e., they fit the EU definition of a rare condition, by affecting no more than 5 in 10,000 individuals), and indeed the majority of conditions under this umbrella heading are in fact much rarer, affecting fewer than 1 in 100,000. Rare pediatric diseases incur particular challenges, both in terms of actually conducting clinical trials but also planning trials (and indeed, stimulating the preclinical research and knowledge generation necessary to embark on clinical trials in the first place). The pediatric regulation and orphan regulation (covering rare diseases) were introduced to address the complexities in research and development of medicines specifically for children and for people living with a rare disease, respectively. The regulations have been reasonably effective, particularly in areas where adult and pediatric diseases overlap, driving the development of more pediatric medicines; however, challenges still remain, often exacerbated by the rarity of the diseases. These include issues around trial planning, the need for more innovative methodologies in smaller populations, significant delays in trial start up and recruitment, recruitment issues (due to small populations and the nature of the conditions), lack of endpoints, and scarce data. This chapter will discuss some of the major challenges in delivering trials in pediatric rare diseases while also assessing current and future solutions to address these.
对患有罕见疾病的儿童进行临床药物试验
在过去的 50 年里,医学和健康研究的进步不断改变着新生儿、儿童和青少年健康状况的流行病学;临床研究也在整体上向前发展。原因之一是大多数儿科疾病也是罕见病(即符合欧盟对罕见病的定义,患病人数不超过万分之五),而事实上,在这一总标题下的大多数疾病都更为罕见,患病人数不到十万分之一。罕见儿科疾病不仅在实际开展临床试验方面,而且在计划临床试验(实际上是在激励开展临床试验所需的临床前研究和知识积累)方面都面临特殊挑战。儿科法规和孤儿法规(涵盖罕见病)的出台分别是为了解决专为儿童和罕见病患者研发药物的复杂性。这些法规相当有效,尤其是在成人和儿科疾病重叠的领域,推动了更多儿科药物的开发;然而,挑战依然存在,而且往往因疾病的罕见性而加剧。这些挑战包括有关试验规划的问题、在较小的人群中需要更多的创新方法、试验启动和招募方面的重大延误、招募问题(由于人口少和疾病的性质)、终点的缺乏以及数据稀缺。本章将讨论在儿科罕见病试验中面临的一些主要挑战,同时评估当前和未来解决这些问题的方案。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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