Endocrinology Unit, Hospital Geral Alberto Rassi, Goiânia, Brazil.
Department of Medicine, Division of Endocrinology, Escola Paulista de Medicina, Laboratory of Molecular and Translational Endocrinology, Universidade Federal de São Paulo, Rua Pedro de Toledo 669, Sao Paulo, SP, 04039-032, Brazil.
BMC Endocr Disord. 2020 Feb 6;20(1):21. doi: 10.1186/s12902-020-0500-2.
Adrenal hypoplasia congenita (AHC) is an X-linked disorder that affects the adrenal cortex and hypothalamus-pituitary-gonadal axis (HPG), leading to primary adrenocortical insufficiency (PAI) and hypogonadotropic hypogonadism. AHC is caused by a mutation in the DAX-1 gene (NR0B1). More commonly, this disease is characterized by early-onset PAI, with symptoms in the first months of life. However, a less severe phenotype termed late-onset AHC has been described, as PAI signs and symptoms may begin in adolescence and adulthood. Here we describe a family report of a novel mutation within NR0B1 gene and variable reproductive phenotypes, including spontaneous fertility, in a very late-onset X-linked AHC kindred.
Three affected maternal male relatives had confirmed PAI diagnosis between 30 y and at late 64 y. The X-linked pattern has made the endocrinology team to AHC suspicion. Regarding the HPG axis, all males presented a distinct degree of testosterone deficiency and fertility phenotypes, varying from a variable degree of hypogonadism, oligoasthenoteratozoospermia to spontaneous fertility. Interestingly, the other five maternal male relatives unexpectedly died during early adulthood, most likely due to undiagnosed PAI/adrenal crisis as the probable cause of their premature deaths. Sequencing analysis of the NR0B1 gene has shown a novel NR0B1 mutation (p.Tyr378Cys) that segregated in three AHC family members.
NR0B1 p.Tyr378Cys segregates in an AHC family with a variable degree of adrenal and gonadal phenotypes, and its hemizygous trait explains the disease in affected family members. We recommend that NR0B1 mutation carriers, even those that are allegedly asymptomatic, be carefully monitored while reinforcing education to prevent PAI and consider early sperm banking when spermatogenesis still viable.
先天性肾上腺发育不全(AHC)是一种 X 连锁疾病,影响肾上腺皮质和下丘脑-垂体-性腺轴(HPG),导致原发性肾上腺皮质功能不全(PAI)和促性腺激素低下性性腺功能减退症。AHC 是由 DAX-1 基因(NR0B1)突变引起的。更常见的是,这种疾病的特征是早发性 PAI,症状出现在生命的头几个月。然而,已经描述了一种较轻的表型,称为迟发性 AHC,其 PAI 迹象和症状可能在青春期和成年期开始。在这里,我们描述了一个 NR0B1 基因内新突变和可变生殖表型的家族报告,包括非常迟发性 X 连锁 AHC 家族中的自发性生育。
三名受影响的母系男性亲属在 30 岁至 64 岁之间被确诊为 PAI。X 连锁模式使内分泌团队怀疑 AHC。关于 HPG 轴,所有男性均表现出不同程度的睾酮缺乏和生育表型,从不同程度的性腺功能减退症、少精症到自发性生育不等。有趣的是,其他五名母系男性亲属在年轻时意外死亡,很可能是由于未诊断的 PAI/肾上腺危象导致他们过早死亡。NR0B1 基因测序分析显示了一种新的 NR0B1 突变(p.Tyr378Cys),该突变在三个 AHC 家族成员中发生了遗传。
NR0B1 p.Tyr378Cys 在具有不同程度肾上腺和性腺表型的 AHC 家族中遗传,其半合子特征解释了受影响家族成员的疾病。我们建议 NR0B1 突变携带者,即使那些据称无症状,也应仔细监测,同时加强教育以预防 PAI,并在精子发生仍然可行时考虑早期精子库存储。
