Frazier Zoë J, Kilic Seyda, Osika Hailey, Mo Alisa, Quinn Meg, Ballal Sonia, Katz Tamar, Shearer A Eliot, Horlbeck Max A, Pais Lynn S, Dies Kira A, O'Donnell-Luria Anne, Kossowsky Joe, Lipton Jonathan O, Kleefstra Tjitske, Srivastava Siddharth
Rosamund Stone Zander Translational Neuroscience Center, Department of Neurology, Boston Children's Hospital, Boston, Massachusetts, USA.
School of Arts and Sciences, Tufts University, Medford, Massachusetts, USA.
Clin Genet. 2025 Jun;107(6):636-645. doi: 10.1111/cge.14697. Epub 2025 Jan 2.
Kleefstra syndrome (KLEFS) is a genetic neurodevelopmental disorder caused by haploinsufficiency of EHMT1. The full spectrum of clinical features and genotype-phenotype correlations is currently not fully understood. We performed a retrospective chart review of patients with KLEFS evaluated at the Boston Children's Hospital Kleefstra Clinic. There were 65 individuals (40 females, 25 males, mean age 9.3 years). 17% had large 9q34 deletions (≥ 1 Mb), 29% had small 9q34 deletions (< 1 Mb), and 54% had sequence variants. Global developmental delay (GDD) or intellectual disability (ID) was present in 77%. Behavioral disorders, such as autism spectrum disorder (38%), were common. Epilepsy affected 15%. Systemic health issues included structural cardiac defects (40%), hearing loss (32%), and constipation (31%). Novel features including subgroups with significant motor impairment (24%) and refractory epilepsy (9%), as well as small numbers with opsoclonus-like eye movements (n = 2), thrombocytopenia (n = 2), progressive cerebral atrophy (n = 1), and adrenal carcinoma (n = 1). 9q34 deletion subgroups had higher rates of GDD/ID (p = 0.037), significant motor impairment (p = 0.01), epilepsy (p = 0.004), and cortical visual impairment (p = 0.003) compared to the subgroup with sequence variants. This information may be used to improve clinical care as well as inform research and future therapeutic initiatives.
克莱夫斯特拉综合征(KLEFS)是一种由EHMT1基因单倍剂量不足引起的遗传性神经发育障碍。目前尚未完全了解其全部临床特征以及基因型与表型的相关性。我们对在波士顿儿童医院克莱夫斯特拉诊所接受评估的KLEFS患者进行了回顾性病历审查。共有65例个体(40名女性,25名男性,平均年龄9.3岁)。17%的患者存在9q34大片段缺失(≥1 Mb),29%的患者存在9q34小片段缺失(<1 Mb),54%的患者存在序列变异。77%的患者存在全球发育迟缓(GDD)或智力残疾(ID)。行为障碍,如自闭症谱系障碍(38%)很常见。15%的患者患有癫痫。全身健康问题包括结构性心脏缺陷(40%)、听力损失(32%)和便秘(31%)。新发现的特征包括有明显运动障碍的亚组(24%)和难治性癫痫(9%),以及少数有眼球阵挛样眼动(n = 2)、血小板减少症(n = 2)、进行性脑萎缩(n = 1)和肾上腺癌(n = 1)的患者。与序列变异亚组相比,9q34缺失亚组的GDD/ID发生率更高(p = 0.037)、明显运动障碍发生率更高(p = 0.01)、癫痫发生率更高(p = 0.004)和皮质视觉障碍发生率更高(p = 0.003)。这些信息可用于改善临床护理,并为研究和未来的治疗方案提供参考。
