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Chromosome aberrations involving 10q22: report of three overlapping interstitial deletions and a balanced translocation disrupting C10orf11

机译:涉及10q22的染色体畸变:报告了三个重叠的间质缺失和平衡易位破坏了C10orf11

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摘要

Interstitial deletions of chromosome band 10q22 are rare. We report on the characterization of three overlapping de novo 10q22 deletions by high-resolution array comparative genomic hybridization in three unrelated patients. Patient 1 had a 7.9 Mb deletion in 10q21.3–q22.2 and suffered from severe feeding problems, facial dysmorphisms and profound mental retardation. Patients 2 and 3 had nearly identical deletions of 3.2 and 3.6 Mb, the proximal breakpoints of which were located at an identical low-copy repeat. Both patients were mentally retarded; patient 3 also suffered from growth retardation and hypotonia. We also report on the results of breakpoint analysis by array painting in a mentally retarded patient with a balanced chromosome translocation 46,XY,t(10;13)(q22;p13)dn. The breakpoint in 10q22 was found to disrupt C10orf11, a brain-expressed gene in the common deleted interval of patients 1–3. This finding suggests that haploinsufficiency of C10orf11 contributes to the cognitive defects in 10q22 deletion patients.
机译:染色体带10q22的间质性缺失很少见。我们报告了高分辨率的三个比较不相关的患者的高分辨率阵列比较基因组杂交的三个重叠的从头10q22缺失的表征。患者1在10q21.3–q22.2中的7.9 Mb缺失,并且患有严重的进食问题,面部畸形和严重的智力低下。患者2和3具有几乎相同的3.2和3.6 Mb缺失,其近端断点位于相同的低拷贝重复序列中。两名患者均为智障;患者3也患有生长迟缓和肌张力低下。我们还报告了在平衡染色体易位46,XY,t(10; 13)(q22; p13)dn的智障患者中通过阵列绘画进行断点分析的结果。发现10q22处的断点会破坏C10orf11,C10orf11是在1-3位患者的常见缺失间隔中大脑表达的基因。这一发现表明,C10orf11的单倍不足会导致10q22缺失患者的认知缺陷。

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