Small supernumerary marker chromosomes derived from human chromosome 11

小附加标记染色体 单亲二体 遗传学 生物 多余的 染色体 三体 标记染色体 21号染色体 核型 基因 解剖
作者
Thomas Liehr,Monika Ziegler,Luisa Person,Stefanie Kankel,Niklas Padutsch,Anja Weise,Jörg Weimer,Heather Williams,Susana Isabel Ferreira,Joana Barbosa Melo,Isabel M. Carreira
出处
期刊:Frontiers in Genetics [Frontiers Media SA]
卷期号:14: 1293652-1293652 被引量:2
标识
DOI:10.3389/fgene.2023.1293652
摘要

Introduction: With only 39 reported cases in the literature, carriers of a small supernumerary marker chromosome (sSMC) derived from chromosome 11 represent an extremely rare cytogenomic condition. Methods: Herein, we present a review of reported sSMC(11), add 18 previously unpublished cases, and closely review eight cases classified as ‘centromere-near partial trisomy 11’ and a further four suited cases from DECIPHER. Results and discussion: Based on these data, we deduced the borders of the pericentric regions associated with clinical symptoms into a range of 2.63 and 0.96 Mb for chromosome 11 short (p) and long (q) arms, respectively. In addition, the minimal pericentric region of chromosome 11 without triplo-sensitive genes was narrowed to positions 47.68 and 60.52 Mb (GRCh37). Furthermore, there are apparent differences in the presentation of signs and symptoms in carriers of larger sSMCs derived from chromosome 11 when the partial trisomy is derived from different chromosome arms. However, the number of informative sSMC(11) cases remains low, with overlapping presentation between p- and q-arm-imbalances. In addition, uniparental disomy (UPD) of ‘normal’ chromosome 11 needs to be considered in the evaluation of sSMC(11) carriers, as imprinting may be an influencing factor, although no such cases have been reported. Comprehensively, prenatal sSMC(11) cases remain a diagnostic and prognostic challenge.

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