Schaefer Tori L, Davenport Matthew H, Erickson Craig A
Division of Child and Adolescent Psychiatry, Cincinnati Children's Hospital Medical Center, Cincinnati, OH, USA.
Appl Clin Genet. 2015 Apr 7;8:75-93. doi: 10.2147/TACG.S35673. eCollection 2015.
Fragile X syndrome (FXS) is the most common single gene cause of intellectual disability and autism spectrum disorder. Caused by a silenced fragile X mental retardation 1 gene and the subsequent deficiency in fragile X mental retardation protein, patients with FXS experience a range of physical, behavioral, and intellectual debilitations. The FXS field, as a whole, has recently met with some challenges, as several targeted clinical trials with high expectations of success have failed to elucidate significant improvements in a variety of symptom domains. As new clinical trials in FXS are planned, there has been much discussion about the use of the commonly used clinical outcome measures, as well as study design considerations, patient stratification, and optimal age range for treatment. The evidence that modification of these drug targets and use of these failed compounds would prove to be efficacious in human clinical study were rooted in years of basic and translational research. There are questions arising as to the use of the mouse models for studying FXS treatment development. This issue is twofold: many of the symptom domains and molecular and biochemical changes assessed and indicative of efficacy in mouse model study are not easily amenable to clinical trials in people with FXS because of the intolerability of the testing paradigm or a lack of noninvasive techniques (prepulse inhibition, sensory hypersensitivity, startle reactivity, or electrophysiologic, biochemical, or structural changes in the brain); and capturing subtle yet meaningful changes in symptom domains such as sociability, anxiety, and hyperactivity in human FXS clinical trials is challenging with the currently used measures (typically parent/caregiver rating scales). Clinicians, researchers, and the pharmaceutical industry have all had to take a step back and critically evaluate the way we think about how to best optimize future investigations into pharmacologic FXS treatments. As new clinical trials are coming down the drug discovery pipeline, it is clear that the field is moving in a direction that values the development of molecular biomarkers, less subjective quantitative measures of symptom improvement, and rating scales developed specifically for use in FXS in conjunction with drug safety. While summarizing preclinical evidence, where applicable, and discussing challenges in FXS treatment development, this review details both completed clinical trials for the targeted and symptomatic treatment of FXS and introduces novel projects on the cusp of clinical trial investigation.
脆性X综合征(FXS)是导致智力残疾和自闭症谱系障碍最常见的单基因病因。由沉默的脆性X智力低下1基因及随后的脆性X智力低下蛋白缺乏所致,FXS患者会经历一系列身体、行为和智力方面的损伤。总体而言,FXS领域最近遇到了一些挑战,因为几项备受期待的靶向临床试验未能在多个症状领域取得显著改善。随着FXS新临床试验的规划,人们对常用临床结局指标的使用以及研究设计考量、患者分层和最佳治疗年龄范围进行了大量讨论。这些药物靶点的修饰和这些失败化合物的使用在人体临床研究中被证明有效的证据源于多年的基础研究和转化研究。关于使用小鼠模型来研究FXS治疗进展存在一些问题。这个问题有两个方面:在小鼠模型研究中评估的许多症状领域以及指示疗效的分子和生化变化,由于测试范式不可耐受或缺乏非侵入性技术(前脉冲抑制、感觉过敏、惊吓反应或大脑中的电生理、生化或结构变化),不容易应用于FXS患者的临床试验;而在人类FXS临床试验中,使用目前的测量方法(通常是家长/照顾者评定量表)来捕捉社交能力、焦虑和多动等症状领域中细微但有意义的变化具有挑战性。临床医生、研究人员和制药行业都不得不退后一步,批判性地评估我们思考如何最好地优化未来FXS药物治疗研究的方式。随着新的临床试验进入药物研发流程,很明显该领域正朝着重视分子生物标志物的开发、症状改善的主观量化测量较少以及专门为FXS开发的与药物安全性相结合的评定量表的方向发展。在总结适用的临床前证据并讨论FXS治疗进展中的挑战时,本综述详细介绍了针对FXS的靶向和对症治疗的已完成临床试验,并介绍了即将进入临床试验研究阶段的新项目。
