First case of two supernumerary markers derived from chromosome 5 and chromosome 8.

IF 1.3 4区 生物学 Q4 GENETICS & HEREDITY Molecular Cytogenetics Pub Date : 2022-06-27 DOI:10.1186/s13039-022-00601-5
Roberta Giansante, Chiara Palka Bayard De Volo, Melissa Alfonsi, Elisena Morizio, Paolo Guanciali Franchi
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Abstract

Background: Small supernumerary marker chromosomes (sSMC) are additional centric chromosome fragments too small to be identified by banding cytogenetics alone. A sSMC can originate from any chromosome and it is estimated that 70% of sSMC are de novo, while 30% are inherited. Cases of sSMC derived from chromosome 5 (sSMC5) are rare, accounting for1.4% of all reported sSMC cases. In these patients, the most common reported features are macrocephaly, dysmorphic facial features, heart defects, growth retardation, hypotonia, and intellectual disability. Also sSMC derived from chromosome 8 are very rare and the phenotype of patients with sSMC8 is very variable. Common clinical features of the patients include developmental delay, mental retardation, intellectual disability, hypotonia, hypospadias, attention deficit hyperactivity disorders (ADHD), skeletal anomalies, dysmorphic facial features, and renal dysplasia. To the best of our knowledge, in literature there are no cases with coexistence of sSMC5 and sSMC8, so we reviewed the literature to compare cases with SMC5 and those with SMC8 separately. This study is aimed to highlight the unique findings of a patient with the coexistence of sSMC5 and sSMC8.

Case presentation: We describe a female patient with two supernumerary markers derived from chromosome 5 (SMC5) and chromosome 8 (SMC8). The patient was born prematurely at 30 weeks with respiratory distress and bronchodysplasia. On physical examination she presented dysmorphic features, respiratory issues, congenital heart defect, developmental delay, and intellectual disability. The G-banded chromosome analysis on cultured lymphocytes revealed in all the analyzed cells a female karyotype with the presence of two supernumerary chromosomal markers and the array-CGH highlighted the region and the size of these two duplications. We also used the fluorescent in situ hybridization analysis (FISH) using painting of chromosomes 5 and 8 to confirm the origin of the two sSMC. So, the karyotype of the patient was: 48, XX, +mar1, +mar2.

Conclusions: This is the first case with two markers: one from chromosome 5 and one from chromosome 8. Based on the data reported, we can affirm that the phenotype of our patient is probably caused mainly by the presence of the sSMC.

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第5号染色体和第8号染色体首次发现两个多余标记。
背景:小多余标记染色体(Small superary marker chromosome, sSMC)是额外的中心染色体片段,它们太小而无法单独通过带带细胞遗传学来识别。sSMC可以起源于任何染色体,估计70%的sSMC是新生的,而30%是遗传的。来自5号染色体(sSMC5)的sSMC病例很少,占所有报道的sSMC病例的1.4%。在这些患者中,最常见的报道特征是大头畸形、面部畸形、心脏缺陷、生长迟缓、张力低下和智力残疾。此外,来自8号染色体的sSMC非常罕见,并且sSMC8患者的表型非常多变。患者的常见临床特征包括发育迟缓、智力低下、智力障碍、尿道下裂、注意缺陷多动障碍(ADHD)、骨骼异常、面部特征畸形和肾脏发育不良。据我们所知,文献中没有sSMC5和sSMC8同时存在的病例,所以我们复习文献,分别比较SMC5和SMC8的病例。本研究旨在突出sSMC5和sSMC8共存患者的独特发现。病例介绍:我们描述了一个女性患者的两个多余的标记来自染色体5 (SMC5)和染色体8 (SMC8)。患者在30周时早产,伴有呼吸窘迫和支气管发育不良。在体格检查中,她表现出畸形、呼吸问题、先天性心脏缺陷、发育迟缓和智力残疾。对培养的淋巴细胞进行g带染色体分析,发现所有细胞均为女性核型,存在两个额外的染色体标记,阵列- cgh突出了这两个重复的区域和大小。我们还利用荧光原位杂交分析(FISH)对5号和8号染色体进行了染色,以确定两个sSMC的起源。因此,患者的核型为:48,XX, +mar1, +mar2。结论:本例为第1例具有5号染色体和8号染色体两种标记物的病例。根据报告的数据,我们可以肯定,我们患者的表型可能主要是由sSMC的存在引起的。
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来源期刊
Molecular Cytogenetics
Molecular Cytogenetics GENETICS & HEREDITY-
CiteScore
2.60
自引率
7.70%
发文量
49
审稿时长
>12 weeks
期刊介绍: Molecular Cytogenetics encompasses all aspects of chromosome biology and the application of molecular cytogenetic techniques in all areas of biology and medicine, including structural and functional organization of the chromosome and nucleus, genome variation, expression and evolution, chromosome abnormalities and genomic variations in medical genetics and tumor genetics. Molecular Cytogenetics primarily defines a large set of the techniques that operate either with the entire genome or with specific targeted DNA sequences. Topical areas include, but are not limited to: -Structural and functional organization of chromosome and nucleus- Genome variation, expression and evolution- Animal and plant molecular cytogenetics and genomics- Chromosome abnormalities and genomic variations in clinical genetics- Applications in preimplantation, pre- and post-natal diagnosis- Applications in the central nervous system, cancer and haematology research- Previously unreported applications of molecular cytogenetic techniques- Development of new techniques or significant enhancements to established techniques. This journal is a source for numerous scientists all over the world, who wish to improve or introduce molecular cytogenetic techniques into their practice.
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