Laboratorio de Biología Molecular, Subdirección de Investigación Médica, Instituto Nacional de Pediatría, Secretaría de Salud, Mexico City CP 04530, Mexico.
Facultad Mexicana de Medicina, Universidad la Salle, Mexico City CP 14070, Mexico.
Int J Mol Sci. 2023 Sep 27;24(19):14643. doi: 10.3390/ijms241914643.
Trisomy X is the most frequent sex chromosome anomaly in women, but it is often underdiagnosed postnatally because most patients do not show any clinical manifestation. It is estimated that only 10% of patients with trisomy X are diagnosed by clinical findings. Thus, it has been proposed that the clinical spectrum is not yet fully delimited, and additional uncommon or atypical clinical manifestations could be related to this entity. The present report describes a female carrying trisomy X but presenting atypical manifestations, including severe intellectual disability, short stature, thymus hypoplasia, and congenital hypothyroidism (CH). These clinical findings were initially attributed to trisomy X. However, chromosome microarray analysis (CMA) subsequently revealed that the patient also bears a heterozygous 304-kb deletion at 16p11.2. This pathogenic copy-number variant (CNV) encompasses 13 genes, including . Some authors recommend that when a phenotype differs from that described for an identified microdeletion, the presence of pathogenic variants in the non-deleted allele should be considered to assess for an autosomal recessive disorder; thus, we used a panel of 697 genes to rule out a pathogenic variant in the non-deleted allele. We discuss the possible phenotypic modifications that might be related to an additional CNV in individuals with sex chromosome aneuploidy (SCA), as seen in our patient. The presence of karyotype-demonstrated trisomy X and CMA-identified 16p11.2 deletion highlights the importance of always correlating a patient's clinical phenotype with the results of genetic studies. When the phenotype includes unusual manifestations and/or exhibits discrepancies with that described in the literature, as exemplified by our patient, a more extensive analysis should be undertaken to enable a correct diagnosis that will support proper management, genetic counseling, and medical follow-up.
三体 X 是女性最常见的性染色体异常,但由于大多数患者没有任何临床表现,通常在产后被漏诊。据估计,只有 10%的三体 X 患者通过临床发现被诊断出来。因此,有人提出该临床谱尚未完全界定,可能与该疾病相关的还有一些不常见或非典型的临床表现。本报告描述了一位携带三体 X 的女性,但表现出非典型的临床表现,包括严重智力障碍、身材矮小、胸腺发育不全和先天性甲状腺功能减退症 (CH)。这些临床表现最初归因于三体 X。然而,染色体微阵列分析 (CMA) 随后显示患者还携带 16p11.2 处的杂合性 304-kb 缺失。该致病性拷贝数变异 (CNV) 包含 13 个基因,包括. 一些作者建议,当表型与已确定的微缺失描述的表型不同时,应考虑非缺失等位基因中存在致病性变异,以评估常染色体隐性疾病;因此,我们使用了 697 个基因的小组排除了非缺失等位基因中的致病性变异。我们讨论了可能与性染色体非整倍体 (SCA) 个体中额外的 CNV 相关的表型修饰,正如我们的患者所见。核型证实的三体 X 和 CMA 鉴定的 16p11.2 缺失强调了始终将患者的临床表型与遗传研究结果相关联的重要性。当表型包括不寻常的表现和/或与文献中描述的表现存在差异时,如我们的患者所示,应进行更广泛的分析,以进行正确诊断,从而为适当的管理、遗传咨询和医疗随访提供支持。
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