Mantero F, Palermo M, Petrelli M D, Tedde R, Stewart P M, Shackleton C H
Istituto di Medicina Interna, Cattedra di Endocrinologia, University of Ancona, Italy.
Steroids. 1996 Apr;61(4):193-6. doi: 10.1016/0039-128x(96)00012-8.
The syndrome of apparent mineralocorticoid excess (AME) is a heritable form of hypertension due to an inborn error of cortisol metabolism and is characterized by hypokalemia and low renin levels despite subnormal or normal levels of aldosterone and other known mineralocorticoids. The syndrome is attributable to congenital deficiency of the enzyme 11 beta-hydroxydehydrogenase (11 beta-HSD), which converts cortisol (F) to biologically inactive cortisone. This results in a prolonged half-life of F, which acts at the kidney level as a potent mineralocorticoid (MC). In fact, both F and aldosterone have similar affinities in vitro for type I MC receptor (MR), and 11 beta-HSD activity protects the MR in vivo from the higher circulating levels of F. The biochemical marker of this disorder is an increased ratio of tetrahydrocortisol (THF) + allo-THF/tetrahydrocortisone (THE) in the urine, which has been found in more than 20 patients described to date, together with evidence of a more general defect in steroid ring A reduction. Only a few cases (the so-called type II form) described in Italy differ from the classic form having a normal THF/THE ratio, but in both forms the ratio of free urinary F/E has recently been found to be similarly high. Dexamethasone is the treatment of choice but is often inadequate in long term control of high blood pressure. Acquired forms of AME are those consequent on abuse of licorice or carbenoxolone, which both inhibit 11 beta-HSD; the latter also inhibits the reverse 11-oxoreductase reaction leading to somewhat different abnormalities of urinary cortisol/cortisone. So far, two isoenzymes of 11 beta-HSD have been purified and cloned; 11 beta-HSD type 1 is NADP-dependent, abundant in liver, lung, and testis, and catalyzes both 11 beta-dehydrogenation and 11 beta-oxoreduction; no mutation in its gene was detected in patients with AME. A second NAD-dependent isoenzyme is present in kidney and placenta and catalyzes dehydrogenation only. Very recently (1995) two groups have independently demonstrated the presence of mutations in its gene, located in chromosome 16q22. New and co-workers found a point mutation in exon 6 of two affected siblings of an Iranian family, while White and co-workers in parallel studies showed point mutations or small deletions in both alleles in nine unrelated patients; importantly, expression studies showed minimal or absent activity for almost all the mutant sequences. No definite mutations have been so far identified in patients with AME type II. AME is thus the third single gene cause of human hypertension to be described, after glucocorticoid remediable aldosteronism in 1992 and Liddle's syndrome in 1994.
表观盐皮质激素过多综合征(AME)是一种由于皮质醇代谢先天性缺陷导致的遗传性高血压形式,其特征是尽管醛固酮和其他已知盐皮质激素水平正常或低于正常水平,但仍存在低钾血症和低肾素水平。该综合征归因于11β-羟脱氢酶(11β-HSD)先天性缺乏,该酶将皮质醇(F)转化为无生物活性的可的松。这导致F的半衰期延长,F在肾脏水平作为一种强效盐皮质激素(MC)起作用。事实上,F和醛固酮在体外对I型MC受体(MR)具有相似的亲和力,11β-HSD活性在体内可保护MR免受循环中较高水平F的影响。这种疾病的生化标志物是尿中四氢皮质醇(THF)+别-THF/四氢可的松(THE)的比值增加,在迄今描述的20多名患者中均有发现,同时有证据表明类固醇A环还原存在更普遍的缺陷。在意大利描述的少数病例(所谓的II型)与经典型不同,其THF/THE比值正常,但最近发现两种类型的尿游离F/E比值同样升高。地塞米松是首选治疗药物,但在长期控制高血压方面往往效果不佳。AME的获得性形式是由于滥用甘草或生胃酮导致的,二者均抑制11β-HSD;后者还抑制反向11-氧化还原酶反应,导致尿皮质醇/可的松出现略有不同的异常。到目前为止,已纯化并克隆了11β-HSD的两种同工酶;11β-HSD 1型依赖NADP,在肝脏、肺和睾丸中含量丰富,催化11β-脱氢和11β-氧化还原反应;AME患者中未检测到其基因突变。第二种依赖NAD的同工酶存在于肾脏和胎盘中,仅催化脱氢反应。最近(1995年),两个研究小组独立证明其基因位于16q22染色体上存在突变。New及其同事在一个伊朗家族的两名患病同胞的外显子6中发现了一个点突变,而White及其同事在平行研究中显示,9名无关患者的两个等位基因中均存在点突变或小缺失;重要的是,表达研究表明几乎所有突变序列的活性极低或无活性。到目前为止,II型AME患者中尚未确定明确的突变。因此,AME是继1992年糖皮质激素可治性醛固酮增多症和1994年Liddle综合征之后被描述的人类高血压的第三个单基因病因。
