常染色体显性多囊肾病
包装D1
外显率
神经纤维瘤病
孟德尔遗传
先证者
疾病
遗传学
遗传咨询
医学
马凡氏综合征
医学遗传学
生物
表型
内科学
突变
基因
作者
Stephanie A. Felker,Bruce R. Korf,Gregory S. Barsh
标识
DOI:10.1101/2025.02.26.25322940
摘要
Purpose: Research Program participants with pathogenic variation causal for three Mendelian conditions: autosomal dominant polycystic kidney disease (ADPKD), Marfan syndrome, and neurofibromatosis type 1 (NF1). Methods: . Concept terms were extracted from electronic health records to assess participant diagnosis and phenotype. Variant annotation and participant surveys were evaluated to identify biological and social factors differentiating diagnosed and undiagnosed individuals. Results: lack the associated diagnosis of NF1 (47%), Marfan syndrome (58%), or ADPKD (51%), respectively. Pathogenic variants in diagnosed individuals have greater inferred deleteriousness for NF1 and ADPKD, and undiagnosed individuals had less severe phenotypes compared to diagnosed individuals for all three conditions. Conclusion: A genotype-first ascertainment of individuals in genomic research allows for a more comprehensive assessment of Mendelian disease and removes biases that confound our understanding of the penetrance and presentation of these conditions.
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