建立肌酸转运体缺乏症和胍乙酸甲基转移酶缺乏症的核心结果集

Zahra Nasseri Moghaddam, Emily K Reinhardt, Audrey Thurm, Beth K Potter, Maureen Smith, Celeste Graham, Beth H Tiller, Steven A Baker, Deborah A Bilder, Regina Bogar, Jacobus Britz, Rachel Cafferty, Daniel P Coller, Ton J DeGrauw, Vicky Hall, Gerald S Lipshutz, Nicola Longo, Saadet Mercimek-Andrews, Judith S Miller, Marzia Pasquali, Gajja S Salomons, Andreas Schulze, Celine P Wheaton, Kayla F Williams, Sarah P Young, Jasmine Li, Sofia Balog, Theresa Selucky, Sylvia Stockler-Ipsiroglu, Heidi Wallis
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引用次数: 0

摘要

肌酸转运体(CTD)和胍乙酸甲基转移酶(GAMT)缺乏症是一种罕见的肌酸代谢先天性错误,会导致脑肌酸缺乏症。患者通常表现出智力和发育障碍,经常伴有行为问题、语言发育迟缓、癫痫发作和运动障碍。CTD 目前尚无有效的治疗方法,而 GAMT 目前的治疗方法则需要终身限制蛋白质饮食和摄入大量口服营养补充剂。由于缺乏对临床和患者有意义的结果,开发有效、可持续治疗这些疾病的努力受到了限制。核心结果集(COS)可以促进就纳入研究的结果达成共识。遗憾的是,在 COS 开发过程中,患者和护理人员的观点历来被忽视,从而限制了他们对结果选择的投入。我们与护理人员和医疗专业人员合作,为 CTD 和 GAMT 建立了首个 COS。所制定的 COS 包括 CTD 和 GAMT 的七项结果(适应功能、认知功能、情绪失调、MRS 脑肌酸、癫痫发作/惊厥、表达交流和精细运动功能),以及 GAMT 的一项额外结果(血清/血浆胍基乙酸盐),这些结果对利益相关者非常重要,因此应考虑在每项临床试验中进行测量。在整个 COS 开发过程中,护理人员都是重要的合作伙伴,这提高了社区参与度,促进了护理人员的能力提升。我们希望该 COS 将确保采用以患者为中心的方法来加速 CTD 和 GAMT 的药物开发,使临床试验结果具有可比性,最大限度地减少临床试验结果选择的偏差,并促进资源的有效利用。
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Establishing a Core Outcome Set for Creatine Transporter Deficiency and Guanidinoacetate Methyltransferase Deficiency
Creatine transporter (CTD) and guanidinoacetate methyltransferase (GAMT) deficiencies are rare inborn errors of creatine metabolism, resulting in cerebral creatine deficiency. Patients commonly exhibit intellectual and developmental disabilities, often accompanied by behavior problems, delayed speech, seizures, and motor impairments. There is currently no efficacious treatment for CTD, while the current management for GAMT requires lifelong treatment with a protein restricted diet and intake of high amounts of oral supplements. Efforts to develop effective, sustainable treatments for these disorders are limited by the lack of clinical and patient-derived meaningful outcomes. A core outcome set (COS) can facilitate consensus about outcomes for inclusion in studies. Unfortunately, patient and caregiver perspectives have historically been overlooked in the COS development process, thus limiting their input into the outcome selection. We partnered with caregivers and health professionals to establish the first COS for CTD and GAMT. The COS developed includes seven outcomes (Adaptive Functioning, Cognitive Functioning, Emotional Dysregulation, MRS Brain Creatine, Seizure/Convulsions, Expressive Communication, and Fine Motor Functions) for both CTD and GAMT, and an additional outcome for GAMT (Serum/Plasma Guanidinoacetate) that are important to stakeholders and consequently should be considered for measurement in every clinical trial. Caregivers were valued partners throughout the COS development process, which increased community engagement and facilitated caregiver empowerment. We expect this COS will ensure a patient-centered approach for accelerating drug development for CTD and GAMT, make clinical trial results comparable, minimize bias in clinical trial outcome selection, and promote efficient use of resources.
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