De Novo Balanced Translocations Disrupting the FBN1 Gene Diagnosed by Genome Sequencing: An Uncommon Cause of Marfan Syndrome Modifying Genetic Counseling.

IF 1.7 4区 生物学 Q3 GENETICS & HEREDITY
C Racine, P Callier, R Touraine, A Vitobello, N Hanna, P Arnaud, G Jondeau, C Boileau, C Thauvin-Robinet, I Creveaux, V Gatinois, M Willems, L Faivre
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Abstract

Marfan syndrome (MFS) is a well-characterized rare genetic connective tissue disorder. The features of MFS are primarily skeletal, ocular, and cardiovascular and are mainly caused by single-nucleotide variants (SNVs) in the FBN1 gene (MIM#134797) located on chromosome 15q21.1. We describe two patients, a 26-year-old male and a 10-year-old female from unrelated distinct families, with clinically diagnosed sporadic MFS. After years of unsuccessful molecular diagnosis for genetic counseling purposes, genome sequencing was performed and revealed a balanced translocation in both patients: de novo t(9;15)(p13.3;q21.1) translocation in the male patient, and de novo t(15;16)(q21.1;p13.13) translocation in the female patient, respectively, disrupting intron 40 and 45 of FBN1. The other breakpoints were not clinically relevant. These translocations were confirmed by specific fluorescence in situ hybridization probes and conventional karyotyping. In the literature, only one family has been described, leading to four cases of MFS caused by balanced translocations. Genetic counseling for balanced translocations differs from SNVs and even interstitial deletions since it is not restricted to MFS recurrence, but also involves the risk of unbalanced gametes, leading to miscarriage or unbalanced progeny. In case of clinical certainty, MFS patients should be screened for balanced translocations to ensure appropriate genetic counseling.

通过基因组测序诊断出干扰 FBN1 基因的新平衡易位:马凡综合征的一个不常见病因,改变遗传咨询。
马凡综合征(MFS)是一种特征明显的罕见遗传性结缔组织疾病。马凡综合征的特征主要是骨骼、眼部和心血管疾病,主要由位于染色体 15q21.1 上的 FBN1 基因(MIM#134797)的单核苷酸变异(SNVs)引起。我们描述了两名临床诊断为散发性 MFS 的患者,一名 26 岁男性和一名 10 岁女性,他们分别来自不同的非亲缘家庭。经过多年用于遗传咨询的分子诊断失败后,我们对这两名患者进行了基因组测序,结果显示他们都存在平衡易位:男性患者存在从头t(9;15)(p13.3;q21.1)易位,女性患者存在从头t(15;16)(q21.1;p13.13)易位,分别破坏了FBN1的内含子40和45。其他断点与临床无关。这些易位通过特异性荧光原位杂交探针和常规核型检查得到证实。文献中只描述了一个家族,导致四例由平衡易位引起的 MFS。平衡易位的遗传咨询不同于 SNV 甚至间质缺失,因为它不仅限于 MFS 复发,还涉及配子不平衡的风险,导致流产或后代不平衡。在临床确定的情况下,应对 MFS 患者进行平衡易位筛查,以确保提供适当的遗传咨询。
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来源期刊
CiteScore
3.50
自引率
5.00%
发文量
432
审稿时长
2-4 weeks
期刊介绍: The American Journal of Medical Genetics - Part A (AJMG) gives you continuous coverage of all biological and medical aspects of genetic disorders and birth defects, as well as in-depth documentation of phenotype analysis within the current context of genotype/phenotype correlations. In addition to Part A , AJMG also publishes two other parts: Part B: Neuropsychiatric Genetics , covering experimental and clinical investigations of the genetic mechanisms underlying neurologic and psychiatric disorders. Part C: Seminars in Medical Genetics , guest-edited collections of thematic reviews of topical interest to the readership of AJMG .
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