胎儿尸检组织的全外显子组分析显示,OBL1基因存在移码突变,符合3-M综合征的诊断。
Whole-exome analysis of foetal autopsy tissue reveals a frameshift mutation in OBSL1, consistent with a diagnosis of 3-M Syndrome.
作者信息
Marshall Christian R, Farrell Sandra A, Cushing Donna, Paton Tara, Stockley Tracy L, Stavropoulos Dimitri J, Ray Peter N, Szego Michael, Lau Lynette, Pereira Sergio L, Cohn Ronald D, Wintle Richard F, Abuzenadah Adel M, Abu-Elmagd Muhammad, Scherer Stephen W
出版信息
BMC Genomics. 2015;16 Suppl 1(Suppl 1):S12. doi: 10.1186/1471-2164-16-S1-S12. Epub 2015 Jan 15.
BACKGROUND
We report a consanguineous couple that has experienced three consecutive pregnancy losses following the foetal ultrasound finding of short limbs. Post-termination examination revealed no skeletal dysplasia, but some subtle proximal limb shortening in two foetuses, and a spectrum of mildly dysmorphic features. Karyotype was normal in all three foetuses (46, XX) and comparative genomic hybridization microarray analysis detected no pathogenic copy number variants.
RESULTS
Whole-exome sequencing and genome-wide homozygosity mapping revealed a previously reported frameshift mutation in the OBSL1 gene (c.1273insA p.T425nfsX40), consistent with a diagnosis of 3-M Syndrome 2 (OMIM #612921), which had not been anticipated from the clinical findings.
CONCLUSIONS
Our study provides novel insight into the early clinical manifestations of this form of 3-M syndrome, and demonstrates the utility of whole exome sequencing as a tool for prenatal diagnosis in particular when there is a family history suggestive of a recurrent set of clinical symptoms.
背景
我们报告了一对近亲夫妇,在胎儿超声检查发现四肢短小后连续经历了三次妊娠丢失。终止妊娠后的检查未发现骨骼发育异常,但两个胎儿存在一些轻微的近端肢体缩短以及一系列轻度畸形特征。所有三个胎儿的核型均正常(46, XX),比较基因组杂交微阵列分析未检测到致病性拷贝数变异。
结果
全外显子测序和全基因组纯合性图谱分析发现OBSL1基因中一个先前报道的移码突变(c.1273insA p.T425nfsX40),符合3-M综合征2型(OMIM #612921)的诊断,而临床发现并未预期到这一结果。
结论
我们的研究为这种形式的3-M综合征的早期临床表现提供了新的见解,并证明了全外显子测序作为产前诊断工具的实用性,特别是当有家族病史提示存在一组复发性临床症状时。
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