桥粒蛋白
生物
错义突变
桥粒
掌跖角化病
遗传学
普氏球蛋白
心肌病
角化病
病理
细胞生物学
表型
角化过度
内科学
信号转导
医学
心力衰竭
基因
Wnt信号通路
细胞
连环素
作者
Lynn M. Boyden,Chen Yuan Kam,Á. Hernández‐Martín,Jing Zhou,Brittany G. Craiglow,Robert Sidbury,Erin F. Mathes,Sheilagh Maguiness,Debra Crumrine,Mary L. Williams,Rong‐Hua Hu,Richard P. Lifton,Peter M. Elias,Kathleen J. Green,Keith A. Choate
摘要
Disorders of keratinization (DOK) show marked genotypic and phenotypic heterogeneity. In most cases, disease is primarily cutaneous, and further clinical evaluation is therefore rarely pursued. We have identified subjects with a novel DOK featuring erythrokeratodermia and initially-asymptomatic, progressive, potentially fatal cardiomyopathy, a finding not previously associated with erythrokeratodermia. We show that de novo missense mutations clustered tightly within a single spectrin repeat of DSP cause this novel cardio-cutaneous disorder, which we term erythrokeratodermia-cardiomyopathy (EKC) syndrome. We demonstrate that DSP mutations in our EKC syndrome subjects affect localization of desmosomal proteins and connexin 43 in the skin, and result in desmosome aggregation, widening of intercellular spaces, and lipid secretory defects. DSP encodes desmoplakin, a primary component of desmosomes, intercellular adhesion junctions most abundant in the epidermis and heart. Though mutations in DSP are known to cause other disorders, our cohort features the unique clinical finding of severe whole-body erythrokeratodermia, with distinct effects on localization of desmosomal proteins and connexin 43. These findings add a severe, previously undescribed syndrome featuring erythrokeratodermia and cardiomyopathy to the spectrum of disease caused by mutation in DSP, and identify a specific region of the protein critical to the pathobiology of EKC syndrome and to DSP function in the heart and skin.
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