Mohd Fadley Md A, Ismail Azli, Keong Thong Meow, Yusoff Narazah Mohd, Zakaria Zubaidah
Unit of Hematology, Cancer Research Center, Institute for Medical Research, 50588 Kuala Lumpur, Malaysia.
J Med Case Rep. 2012 Jan 23;6:30. doi: 10.1186/1752-1947-6-30.
Chromosomal aberrations of chromosome 16 are uncommon and submicroscopic deletions have rarely been reported. At present, a cytogenetic or molecular abnormality can only be detected in 55% of Rubinstein-Taybi syndrome patients, leaving the diagnosis in 45% of patients to rest on clinical features only. Interestingly, this microdeletion of 16 p13.3 was found in a young child with an unexplained syndromic condition due to an indistinct etiological diagnosis. To the best of our knowledge, no evidence of a microdeletion of 16 p13.3 with contiguous gene deletion, comprising cyclic adenosine monophosphate-response element-binding protein and tumor necrosis factor receptor-associated protein 1 genes, has been described in typical Rubinstein-Taybi syndrome.
We present the case of a three-year-old Malaysian Chinese girl with a de novo microdeletion on the short arm of chromosome 16, identified by oligonucleotide array-based comparative genomic hybridization. Our patient showed mild to moderate global developmental delay, facial dysmorphism, bilateral broad thumbs and great toes, a moderate size atrial septal defect, hypotonia and feeding difficulties. A routine chromosome analysis on 20 metaphase cells showed a normal 46, XX karyotype. Further investigation by high resolution array-based comparative genomic hybridization revealed a 120 kb microdeletion on chromosomal band 16 p13.3.
A mutation or abnormality in the cyclic adenosine monophosphate-response element-binding protein has previously been determined as a cause of Rubinstein-Taybi syndrome. However, microdeletion of 16 p13.3 comprising cyclic adenosine monophosphate-response element-binding protein and tumor necrosis factor receptor-associated protein 1 genes is a rare scenario in the pathogenesis of Rubinstein-Taybi syndrome. Additionally, due to insufficient coverage of the human genome by conventional techniques, clinically significant genomic imbalances may be undetected in unexplained syndromic conditions of young children. This case report demonstrates the ability of array-based comparative genomic hybridization to offer a genome-wide analysis at high resolution and provide information directly linked to the physical and genetic maps of the human genome. This will contribute to more accurate genetic counseling and provide further insight into the syndrome.
16号染色体的染色体畸变并不常见,亚显微缺失鲜有报道。目前,仅55%的鲁宾斯坦-泰比综合征患者能检测到细胞遗传学或分子异常,45%患者的诊断仅基于临床特征。有趣的是,在一名病因不明的综合征患儿中发现了16p13.3的这种微缺失。据我们所知,典型的鲁宾斯坦-泰比综合征中,尚无包含环磷酸腺苷反应元件结合蛋白和肿瘤坏死因子受体相关蛋白1基因的16p13.3微缺失及相邻基因缺失的证据。
我们报告一例三岁马来西亚华裔女孩,通过基于寡核苷酸阵列的比较基因组杂交技术,发现其16号染色体短臂存在新生微缺失。我们的患者表现为轻度至中度的全面发育迟缓、面部畸形、双侧拇指和大脚趾宽阔、中度大小的房间隔缺损、肌张力低下和喂养困难。对20个中期细胞进行的常规染色体分析显示核型正常,为46,XX。通过基于高分辨率阵列的比较基因组杂交技术进一步检测发现,16号染色体带16p13.3存在120kb的微缺失。
先前已确定环磷酸腺苷反应元件结合蛋白的突变或异常是鲁宾斯坦-泰比综合征的病因。然而,包含环磷酸腺苷反应元件结合蛋白和肿瘤坏死因子受体相关蛋白1基因的16p13.3微缺失在鲁宾斯坦-泰比综合征的发病机制中是一种罕见情况。此外,由于传统技术对人类基因组的覆盖不足,幼儿不明原因的综合征中可能无法检测到具有临床意义的基因组失衡。本病例报告证明了基于阵列的比较基因组杂交技术能够进行高分辨率的全基因组分析,并提供与人类基因组物理图谱和遗传图谱直接相关的信息。这将有助于更准确的遗传咨询,并为该综合征提供进一步的见解。
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