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导致德拉萨尔综合征的罕见染色体重排,伴有嵌合体 45,X 细胞系:(46,X,psu dic(X;Y)(p22.13;q11.221)/45,X/45,psu dic(X;Y)(p22.13;q11.221))。

A Rare Chromosome Rearrangement Leading to de la Chapelle Syndrome with a Mosaic 45,X Cell Line: (46,X,psu dic(X;Y)(p22.13;q11.221)/45,X/45,psu dic(X;Y)(p22.13;q11.221).

机构信息

Clément Laboratory, F-93110 Paris, France.

Department of Cytogenetics, APHP Centre, Université de Paris, Hôpital Cochin, F-75014 Paris, France.

出版信息

Genes (Basel). 2022 Dec 27;14(1):81. doi: 10.3390/genes14010081.

Abstract

Infertility affects about 15% of couples of childbearing age. About half of these cases can be attributed predominantly to a male factor, such as a quantitative or qualitative impairment in spermatogenesis. The first-line genetic screening for non-obstructive azoospermia is limited to karyotyping (to identify chromosome abnormalities) and Y chromosome microdeletions screening, with a view to explaining the spermatogenetic failure and evaluating the likelihood of sperm retrieval in a testicular biopsy. For patients with de la Chapelle syndrome (a 46,XX karyotype with the presence of (Sex determining region Y) gene) and/or Y chromosome microdeletions, or sex chromosome mosaicism, sperm retrieval is usually unsuccessful. Here, we report a patient with de la Chapelle syndrome and a short stature caused by mosaicism and a very rare chromosome rearrangement: mos 46,X,psu dic(X;Y)/45,X/45,psu dic(X;Y). This case indicates that in de la Chapelle syndrome, X- and Y-chromosome breakpoint variability is high.

摘要

不育症影响约 15%的育龄夫妇。这些病例中约有一半主要归因于男性因素,如精子发生的数量或质量受损。非阻塞性无精子症的一线遗传筛查仅限于核型分析(以识别染色体异常)和 Y 染色体微缺失筛查,旨在解释生精失败并评估睾丸活检中精子获取的可能性。对于患有 de la Chapelle 综合征(具有 (性别决定区 Y)基因的 46,XX 核型)和/或 Y 染色体微缺失或性染色体嵌合体的患者,精子获取通常不成功。在这里,我们报告了一例由嵌合体和非常罕见的染色体重排引起的 de la Chapelle 综合征和身材矮小的患者:mos 46,X,psu dic(X;Y)/45,X/45,psu dic(X;Y)。该病例表明,在 de la Chapelle 综合征中,X 染色体和 Y 染色体的断点变异性很高。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b4f0/9858770/18bfdfbabf5b/genes-14-00081-g001.jpg

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