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首页> 外文期刊>Microarrays >Identification of Critical Region Responsible for Split Hand/Foot Malformation Type 3 (SHFM3) Phenotype through Systematic Review of Literature and Mapping of Breakpoints Using Microarray Data
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Identification of Critical Region Responsible for Split Hand/Foot Malformation Type 3 (SHFM3) Phenotype through Systematic Review of Literature and Mapping of Breakpoints Using Microarray Data

机译:通过文献系统回顾和使用芯片数据绘制断点图,确定负责手/足畸形3型(SHFM3)表型的关键区域

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Split hand/foot malformation (SHFM) is a limb malformation with underdeveloped or absent central digital rays, clefts of hands and feet, and variable syndactyly of the remaining digits. There are six types of SHFM. Here, we report a boy with SHFM type 3 having normal 4th and 5th digits, absent 2nd and 3rd digits, and a 4th finger flexion deformity, as well as absent 2nd, 3rd and 4th toes bilaterally. His father, two paternal uncles, and two paternal first cousins have similar phenotype. Chromosome analysis showed a normal male karyotype. A 514 kb gain at 10q24.31–q24.32 (chr10:102,962,134–103,476,346, hg19) was identified using 6.0 Single nucleotide polymorphism (SNP) microarray, resulting in the duplication of nine genes, including BTRC and FBXW4. A detailed systematic review of literature and mapping of breakpoints using microarray data from all reported cases in PubMed and DECIPHER were conducted, and exon 1 of BTRC gene was identified as the critical region responsible for the SHFM3 phenotype. The potential mechanism and future studies of this critical region causing the SHFM3 phenotype are discussed.
机译:手脚分裂畸形(SHFM)是肢体畸形,其中央数字射线欠发达或缺乏,手脚出现c裂,而其余手指则随年龄变化。 SHFM有六种类型。在这里,我们报告一个SHFM类型为3的男孩,其第四和第五手指正常,第二和第三手指缺失,第四指屈曲畸形,而第二,第三和第四趾没有双侧脚趾。他的父亲,两个父亲的叔叔和两个父亲的堂兄弟表型相似。染色体分析显示正常的男性核型。使用6.0单核苷酸多态性(SNP)微阵列鉴定出10q24.31–q24.32(chr10:102,962,134–103,476,346,hg19)的514 kb增益,导致包括BTRC和FBXW4在内的9个基因重复。使用来自PubMed和DECIPHER中所有报告病例的微阵列数据对文献进行了详尽的系统综述,并绘制了断点图,并将BTRC基因的外显子1鉴定为负责SHFM3表型的关键区域。讨论了该关键区域引起SHFM3表型的潜在机制和未来研究。

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