Kawano-Matsuda Fumika, Maeda Tomoki, Kaname Tadashi, Yanagi Kumiko, Ihara Kenji
Department of Pediatrics, Oita University Faculty of Medicine, Oita, Japan.
National Center for Child Health and Development, Tokyo, Japan.
Clin Pediatr Endocrinol. 2021;30(1):61-64. doi: 10.1297/cpe.30.61. Epub 2021 Jan 5.
Many monogenetic disorders of short stature have autosomal recessive/dominant form of inheritance. However, X-linked short stature has not been well recognized. Herein, we report a case of a boy from a family with familial severe short stature and mental retardation, who displayed an X-linked recessive trait. The boy at the age of 4 yr and 6 mo presented with remarkable growth failure (height: 76.5 cm [-6.3 SD]) and mental retardation (IQ: 30) and cerebellar volume loss and without an external anomaly or microcephaly to our hospital. A careful interview to determine the family history suggested a genetic background of familial mental retardation and short stature. His mother had mild intellectual disability with normal stature and his maternal uncle had severe mental retardation with remarkably short stature. Whole-exome sequencing identified a pathogenic variant in the gene, NM_004187: exon 23: c.3874_3875del: (p.Ala1292Glnfs*7). He presented with a novel frameshift mutation. His mother was a heterozygous carrier of the variant. This case suggests that a disorder associated with the gene should be considered when patients present with remarkably short stature and X-linked mental retardation.
许多单基因矮小症疾病具有常染色体隐性/显性遗传形式。然而,X连锁矮小症尚未得到充分认识。在此,我们报告一例来自一个患有家族性严重矮小症和智力障碍家庭的男孩,他表现出X连锁隐性特征。该男孩4岁6个月时因显著生长发育迟缓(身高:76.5厘米[-6.3标准差])、智力障碍(智商:30)、小脑体积减小且无外部异常或小头畸形前来我院就诊。通过仔细询问家族史发现存在家族性智力障碍和矮小症的遗传背景。他的母亲有轻度智力残疾但身材正常,他的舅舅有严重智力障碍且身材显著矮小。全外显子测序在基因NM_004187中鉴定出一个致病变异:第23外显子:c.3874_3875del:(p.Ala1292Glnfs*7)。他出现了一个新的移码突变。他的母亲是该变异的杂合携带者。该病例表明,当患者出现显著矮小症和X连锁智力障碍时,应考虑与该基因相关的疾病。
