Habiby R L, Boepple P, Nachtigall L, Sluss P M, Crowley W F, Jameson J L
Division of Endocrinology, Metabolism, and Molecular Medicine, Northwestern University Medical School, Chicago, Illinois 60611, USA.
J Clin Invest. 1996 Aug 15;98(4):1055-62. doi: 10.1172/JCI118866.
Adrenal hypoplasia congenita (AHC) is an X-linked disorder that typically presents with adrenal insufficiency during infancy. Hypogonadotropic hypogonadism (HHG) has been identified as a component of this disorder in affected individuals who survive into childhood. Recently, AHC was shown to be caused by mutations in DAX-1, a protein that is structurally similar in its carboxyterminal region to orphan nuclear receptors. We studied two kindreds with clinical features of AHC and HHG. DAX-1 mutations were identified in both families. In the JW kindred, a single base deletion at nucleotide 1219 was accompanied by an additional base substitution that resulted in a frameshift mutation at codon 329 followed by premature termination. In the MH kindred, a GGAT duplication at codon 418 caused a frameshift that also resulted in truncation of DAX-1. Baseline luteinizing hormone (LIT), follicle-stimulating hormone (FSH), and free-alpha-subunit (FAS) levels were determined during 24 h of frequent (q10 min) venous sampling. In patient MH, baseline LH levels were low, but FAS levels were within the normal range. In contrast, in patient JW, the mean LH and FSH were within the normal range during baseline sampling, but LH secretion was erratic rather than showing typical pulses. FAS was apulsatile for much of the day, but a surge was seen over a 3-4-h period. Pulsatile gonadotropin releasing hormone (GnRH) (25 ng/kg) was administered every 2 h for 7 d to assess pituitary responsiveness to exogenous GnRH. MH did not exhibit a gonadotropin response to pulsatile GnRH. JW exhibited a normal response to the first pulse of GnRH, but there was no increase in FAS. In contrast to the priming effect of GnRH in GnRH-deficient patients with Kallmann syndrome, GnRH pulses caused minimal secretory responses of LH and no FAS responses in patient JW. The initial LH response in patient JW implies a deficiency in hypothalamic GnRH. On the other hand, the failure to respond to pulsatile GnRH is consistent with a pituitary defect in gonadotropin production. These two cases exemplify the phenotypic heterogeneity of AHC/HHG, and suggest that DAX-1 mutations impair gonadotropin production by acting at both the hypothalamic and pituitary levels.
先天性肾上腺发育不全(AHC)是一种X连锁疾病,通常在婴儿期出现肾上腺功能不全。在存活至儿童期的受影响个体中,促性腺激素缺乏性性腺功能减退(HHG)已被确定为该疾病的一个组成部分。最近,研究表明AHC是由DAX-1基因突变引起的,DAX-1是一种蛋白质,其羧基末端区域在结构上与孤儿核受体相似。我们研究了两个具有AHC和HHG临床特征的家族。在两个家族中均发现了DAX-1基因突变。在JW家族中,核苷酸1219处的单个碱基缺失伴随着另一个碱基替换,导致第329密码子处的移码突变,随后提前终止。在MH家族中,第418密码子处的GGAT重复导致移码,也导致DAX-1截短。在24小时内通过频繁(每10分钟一次)静脉采血测定基础促黄体生成素(LH)、促卵泡生成素(FSH)和游离α亚基(FAS)水平。在患者MH中,基础LH水平较低,但FAS水平在正常范围内。相比之下,在患者JW中,基础采样期间平均LH和FSH在正常范围内,但LH分泌不稳定,未显示典型脉冲。FAS在一天中的大部分时间无脉冲,但在3 - 4小时内出现一次高峰。每2小时给予脉冲式促性腺激素释放激素(GnRH)(25 ng/kg),共7天,以评估垂体对外源性GnRH的反应性。MH对脉冲式GnRH未表现出促性腺激素反应。JW对GnRH的第一个脉冲表现出正常反应,但FAS无增加。与GnRH缺乏的卡尔曼综合征患者中GnRH的启动作用相反,GnRH脉冲在患者JW中引起LH的分泌反应最小,且无FAS反应。患者JW最初的LH反应提示下丘脑GnRH缺乏。另一方面,对脉冲式GnRH无反应与促性腺激素产生的垂体缺陷一致。这两个病例例证了AHC/HHG的表型异质性,并表明DAX-1突变通过在下丘脑和垂体水平起作用损害促性腺激素的产生。
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