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Whole-genome analysis as a diagnostic tool for patients referred for diagnosis of Silver-Russell syndrome: a real-world study

基因组印记 印记(心理学) 拷贝数变化 单亲二体 生物 Beckwith-Wiedemann综合征 基因组 医学遗传学 生物信息学 遗传学 基因 染色体 DNA甲基化 核型 基因表达
作者
Ahmed Alhendi,Derek Lim,Shane McKee,Meriel McEntagart,Katriona Tatton-Brown,I. Karen Temple,Justin H. Davies,Deborah Mackay
出处
期刊:Journal of Medical Genetics [BMJ]
卷期号:59 (6): 613-622 被引量:12
标识
DOI:10.1136/jmedgenet-2021-107699
摘要

Background Silver-Russell syndrome (SRS) is an imprinting disorder characterised by prenatal and postnatal growth restriction, but its clinical features are non-specific and its differential diagnosis is broad. Known molecular causes of SRS include imprinting disturbance, single nucleotide variant (SNV), CNV or UPD affecting several genes; however, up to 40% of individuals with a clinical diagnosis of SRS currently receive no positive molecular diagnosis. Methods To determine whether whole-genome sequencing (WGS) could uncover pathogenic variants missed by current molecular testing, we analysed data of 72 participants recruited to the 100,000 Genomes Project within the clinical category of SRS. Results In 20 participants (27% of the cohort) we identified genetic variants plausibly accounting for SRS. Coding SNVs were identified in genes including CDKN1C , IGF2 , IGF1R and ORC1 . Maternal-effect variants were found in mothers of five participants, including two participants with imprinting disturbance and one with multilocus imprinting disorder. Two regions of homozygosity were suggestive of UPD involving imprinted regions implicated in SRS and Temple syndrome, and three plausibly pathogenic CNVs were found, including a paternal deletion of PLAGL1 . In 48 participants with no plausible pathogenic variant, unbiased analysis of SNVs detected a potential association with STX4 . Conclusion WGS analysis can detect UPD, CNV and SNV and is potentially a valuable addition to diagnosis of SRS and related growth-restricting disorders.
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