首页> 外文期刊>European journal of human genetics: EJHG >Genome-wide UPD screening in patients with intellectual disability.
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Genome-wide UPD screening in patients with intellectual disability.

机译:智力障碍患者的全基因组UPD筛查。

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摘要

Uniparental disomy (UPD) describes the inheritance of a pair of chromosomes from only one parent. It may occur as isodisomy, heterodisomy or a combination of both and may involve only chromosome segments. UPD can affect each chromosome. The incidence is estimated to be around 1:3500 in live births. Some parts of chromosomes are subject to 'parent-of-origin imprinting' and the phenotypic effect in UPD syndromes is mainly due to functional imbalance of imprinted genes. Isodisomy can result in mutation homozygosity in autosomal-recessive inherited diseases. UPD causes several well-defined imprinting syndromes associated with intellectual disability (ID). Although knowledge on frequency and size of UPDs in patients with unexplained ID remains largely unknown as no efficient genome-wide screening technique was available for detection of both isodisomic and heterodisomic UPDs. SNP microarrays have been proven to be capable to detect UPDs through Mendelian errors. The correct subclassification of UPD requires child-parent trio experiments. To further elucidate the role of UPD in patients with unexplained ID, we analyzed a total of 322 child-parent trios. We were not able to detect UPDs (isodisomies and heterodisomies) within our cohort spanning whole chromosomes or chromosomal segments. We conclude that UPD is rare in patients with unexplained ID.
机译:单亲二体性(UPD)描述了仅一对亲本的一对染色体的遗传。它可能以等位切割,异种切割或两者结合出现,并且可能仅涉及染色体片段。 UPD可以影响每个染色体。据估计,活产的发病率约为1:3500。染色体的某些部分受到“祖父母印记”的影响,UPD综合征的表型效应主要归因于被印记基因的功能失衡。等染色体切割可以导致常染色体隐性遗传疾病的突变纯合性。 UPD会导致几种与智障(ID)相关的明确的烙印综合征。尽管对于无法解释的ID患者的UPD频率和大小的了解仍然未知,因为没有有效的全基因组筛选技术可用于检测等位和异位UPD。 SNP微阵列已被证明能够通过孟德尔误差检测UPD。 UPD的正确分类需要儿童-父母三重奏实验。为了进一步阐明UPD在无法解释ID的患者中的作用,我们分析了总共322个儿童-父母三重奏。我们无法检测整个队列或整个染色体段中的UPD(等位基因和异位基因)。我们得出结论,IDD不明的患者很少发生UPD。

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