46,XY核型17α-羟化酶/17,20-裂解酶缺乏症:我们的经验及文献综述
17α-Hydroxylase/17,20-Lyase Deficiency in 46,XY: Our Experience and Review of Literature.
作者信息
Maheshwari Madhur, Arya Sneha, Lila Anurag Ranjan, Sarathi Vijaya, Barnabas Rohit, Rai Khushnandan, Bhandare Vishwambhar Vishnu, Memon Saba Samad, Karlekar Manjiri Pramod, Patil Virendra, Shah Nalini S, Kunwar Ambarish, Bandgar Tushar
机构信息
Department of Endocrinology, Seth G S Medical College & KEM Hospital, Mumbai 400012, India.
Department of Endocrinology, Vydehi Institute of Medical Sciences and Research Centre, Bangalore 560066, India.
出版信息
J Endocr Soc. 2022 Jan 29;6(3):bvac011. doi: 10.1210/jendso/bvac011. eCollection 2022 Mar 1.
CONTEXT
There are more than 100 pathogenic variants in that have been identified in patients with 17α-hydroxylase/17,20-lyase deficiency (17OHD).
OBJECTIVE
We aimed to describe 46,XY patients with 17OHD from our center and review the literature.
METHODS
We retrospectively analyzed genetically proven index cases of 17OHD from our 46,XY disorders of sex development cohort and reviewed similar cases from the literature (n = 150). Based on the phenotype, 17OHD probands were classified into combined severe deficiency (n = 128) and combined partial deficiency (n = 16). Additionally, patients with the apparent isolated 17,20-lyase deficiency (n = 7, from 6 families) were noted. Residual enzyme activities with the observed mutant enzymes were divided in 2 categories as < 1% and ≥ 1%, each for hydroxylase and lyase.
RESULTS
We present 4 index cases of 46,XY 17OHD with a complete spectrum of undervirilization and 2 novel variants in . In the review, the combined severe deficiency was the most common form, with more frequent female sex of rearing, hypertension, hypokalemia, suppressed renin, higher plasma corticotropin, lower serum cortisol, and androgens. Immunoassay-measured serum aldosterone was frequently (68.2%) unsuppressed (>5 ng/dL). Elevated serum progesterone had high sensitivity for diagnosis of combined 17OHD, even in combined partial deficiency (83.3%). Among patients with clinical phenotype of combined severe deficiency, 11.5% had partial 17α-hydroxylase and complete 17,20-lyase deficiency (>1%/<1%) and had significantly higher serum cortisol than those with < 1%/<1% activity.
CONCLUSION
We report the first monocentric case series of Asian Indian 46,XY patients with 17OHD. We propose that a phenotype of severe undervirilization with milder cortisol deficiency may represent a distinct subtype of combined severe 17OHD with residual 17α-hydroxylase activity but severe 17,20-lyase deficiency (>1%/<1%), which needs further validation.
背景
在17α-羟化酶/17,20-裂解酶缺乏症(17OHD)患者中已鉴定出100多种致病变体。
目的
我们旨在描述来自我们中心的46,XY 17OHD患者并回顾相关文献。
方法
我们回顾性分析了来自我们46,XY性发育障碍队列中经基因证实的17OHD索引病例,并回顾了文献中的类似病例(n = 150)。根据表型,将17OHD先证者分为联合严重缺乏型(n = 128)和联合部分缺乏型(n = 16)。此外,还记录了明显孤立的17,20-裂解酶缺乏症患者(n = 7,来自6个家系)。观察到的突变酶的残余酶活性分为<1%和≥1%两类,分别针对羟化酶和裂解酶。
结果
我们报告了4例46,XY 17OHD索引病例,具有完全的男性化不足谱以及 中的2种新变体。在综述中,联合严重缺乏是最常见的形式,抚养性别为女性、高血压、低钾血症、肾素受抑制、血浆促肾上腺皮质激素较高、血清皮质醇较低以及雄激素缺乏更为常见。免疫测定法测得的血清醛固酮经常(68.2%)未受抑制(>5 ng/dL)。血清孕酮升高对联合17OHD的诊断具有高敏感性,即使在联合部分缺乏型中也是如此(83.3%)。在具有联合严重缺乏临床表型的患者中,11.5%具有部分17α-羟化酶和完全17,20-裂解酶缺乏(>1%/<1%),并且血清皮质醇明显高于活性<1%/<1%的患者。
结论
我们报告了首例亚洲印度46,XY 17OHD患者的单中心病例系列。我们提出,男性化严重不足且皮质醇缺乏较轻的表型可能代表联合严重17OHD的一种独特亚型,具有残余的17α-羟化酶活性但严重的17,20-裂解酶缺乏(>1%/<1%),这需要进一步验证。
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