Lazek Rahaf, Karoum Alaa, Fathalla Waseem
Pediatric Medicine, Sheikh Shakhbout Medical City, Abu dhabi, ARE.
Pediatric Medicine, Sheikh Shakhbout Medical City, Abu Dhabi, ARE.
Cureus. 2025 Jun 29;17(6):e86953. doi: 10.7759/cureus.86953. eCollection 2025 Jun.
Introduction Classical Rett syndrome (RTT) is a rare progressive neurodevelopmental disorder associated with mutations in the gene. This study aims to correlate the genetic mutations and phenotype characteristics of a cohort of RTT syndrome patients and evaluate their amenability to novel therapies, including Trofinetide. Methods We conducted a retrospective observational review of a case series (2000-2024) of RTT patients at Sheikh Shakhbout Medical City, Abu Dhabi, United Arab Emirates (ARE). We included patients under 16 years of age with classic RTT and a confirmed mutation. We analyzed demographic, clinical, and genetic data to determine genotype-phenotype correlations. Results Of 13 patients with RTT syndrome, 8 patients had genetic data on record and were included in the phenotype-genotype correlation analysis; the entire cohort (n=13) was included in the clinical profiling. The age at presentation was 11.2 years, and the median age was 23 months. The distribution of patients' stages at presentation was as follows: 7(53%) were in stage I, 5 (38%) were in stage II, and 1 (8%) were in stage III. Progression to Stages III and IV took place collectively in 9 (75%) of patients. Of the eight patients with genetic data, 6/8 (75%) had variants classified as pathogenic/likely pathogenic, whereas 2/8 (25%) had variants classified as variants of unknown significance (VUS) or benign, however, both met clinical diagnostic criteria for RTT and were assessed by the authors and treating team as pathogenic. These two novel variants were in two classical patients with RTT, classified as VUS (1330G>A) and benign (641C>A). The cohort revealed a high frequency of comorbidities, including epilepsy 8 (61%), behavioral disturbances 7 (53%), gastrointestinal complications 6 (46%), and scoliosis 4 (30%). 5 (43%) of patients had MRI abnormalities. As for treatment amenability, all patients in our cohort are eligible for the only currently approved treatment (Trofinetide), regardless of genotype-phenotype correlation. Conclusion This study demonstrates the clinical and genetic heterogeneity in RTT, and the value of genotyping for confirmation, assessment, and management planning. While no genotype-phenotype profile excludes treatment eligibility with Trofinetide, this correlation may inform early life response to treatment and eligibility for other emerging therapeutic options such as gene therapy. Early recognition, diagnosis, and treatment will certainly have an impact on patient outcomes.
经典型雷特综合征(RTT)是一种罕见的进行性神经发育障碍,与该基因的突变有关。本研究旨在关联一组RTT综合征患者的基因突变与表型特征,并评估他们对包括曲非尼肽在内的新型疗法的适用性。
我们对阿拉伯联合酋长国阿布扎比谢赫·沙赫布特医疗城(ARE)2000年至2024年的RTT患者病例系列进行了回顾性观察性研究。我们纳入了16岁以下患有经典型RTT且有确诊突变的患者。我们分析了人口统计学、临床和基因数据,以确定基因型与表型的相关性。
在13例RTT综合征患者中,8例有记录的基因数据并被纳入表型-基因型相关性分析;整个队列(n = 13)被纳入临床概况分析。就诊时的年龄为11.2岁,中位年龄为23个月。患者就诊时的阶段分布如下:7例(53%)处于I期,5例(38%)处于II期,1例(8%)处于III期。9例(75%)患者共同进展至III期和IV期。在有基因数据的8例患者中,6/8(75%)有被分类为致病/可能致病的变异,而2/8(25%)有被分类为意义未明的变异(VUS)或良性变异,然而,这两个变异均符合RTT的临床诊断标准,作者和治疗团队评估其为致病。这两个新变异存在于两名经典型RTT患者中,分别分类为VUS(1330G>A)和良性(641C>A)。该队列显示出高频率的合并症,包括癫痫8例(61%)、行为障碍7例(53%)、胃肠道并发症6例(46%)和脊柱侧凸4例(30%)。5例(43%)患者有MRI异常。至于治疗适用性,我们队列中的所有患者都有资格接受目前唯一批准的治疗(曲非尼肽),无论基因型与表型的相关性如何。
本研究证明了RTT的临床和基因异质性,以及基因分型在确诊、评估和管理规划中的价值。虽然没有基因型-表型特征排除曲非尼肽的治疗资格,但这种相关性可能为早期治疗反应和其他新兴治疗选择(如基因治疗)的资格提供信息。早期识别、诊断和治疗肯定会对患者的预后产生影响。
