Variable expressivity of KMT2B variants at codon 2565 in patients with dystonia and developmental disorders

肌张力障碍 表现力 遗传学 医学 心理学 生物 神经科学
作者
A. Stehr,Jan A. Fischer,Nazanin Mirza‐Schreiber,Katerina Bernardi,Joseph Porrmann,Philip Harrer,Frank J. Kaiser,Rami Abou Jamra,Juliane Winkelmann,Robert Jech,Anne Koy,Konrad Oexle,Michael Zech
出处
期刊:Parkinsonism & Related Disorders [Elsevier BV]
卷期号:133: 107319-107319
标识
DOI:10.1016/j.parkreldis.2025.107319
摘要

Variable expressivity is an emerging characteristic of KMT2B-related dystonia. However, it remains poorly understood whether variants reoccurring at specific sites of lysine-specific methlytransferase-2B (KMT2B) can drive intra- and interfamilial clinical heterogeneity. Our goal was to ascertain independent families with variants affecting residue Arg2565 of KMT2B. Whole-exome/genome sequencing, multi-site recruitment, genotype-phenotype correlations, and DNA methylation episignature analysis were performed. We report four individuals from two families harboring the variant c.7693C > G, p.Arg2565Gly. In an additional patient, a de-novo c.7693C > T, p.Arg2565Cys variant was identified. The observed phenotypic spectrum ranged from childhood-onset dystonia (N = 2) over unspecific intellectual disability syndromes (N = 2) to undiagnosed behavioral symptoms in adulthood (N = 1). Samples bearing p.Arg2565Gly had a KMT2B-typical episignature, although the effect on methylation was less pronounced than in carriers of loss-of-function KMT2B variants. We established the existence of a KMT2B missense-mutation hotspot associated with varying degrees of disease severity and expression, providing information for patient counseling and elucidation of pathomechanisms.

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