类固醇21-羟化酶缺乏相关的儿童高雄激素症的单基因和多基因模型检测。

Hormone research Pub Date : 2009-01-01 Epub Date: 2008-11-27 DOI:10.1159/000173739
B Ezquieta, M Oyarzabal, R Barrio, C Luzuriaga, F Hermoso, J L Lechuga, S Quinteiro, A Rodríguez, J I Labarta, A Gutierrez Macias, M Gallego, J M Bellón
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引用次数: 9

摘要

目的:高雄激素症,虽然主要是由于多基因相互作用,是单基因的一些酶促肾上腺素缺乏。本研究评估儿童患者单和双等位基因21-羟化酶缺乏症(21OHD)相关的高雄激素症。研究了21OHD携带者和隐型的致敏多态性和保护性多态性。方法:该研究涉及对375例非经典21OHD [NC21OHD]儿童;306名高雄激素21OHD携带者,n = 306)和170名高雄激素携带者和277名家庭成员(对照组)的多基因关联研究(CAPN10-UCSNP44、PON1-108、TNFR2-M196R、IGF2-ApaI和IRS1-G972R多态性)。代谢标记物17OH黄体酮确定缺乏程度;临床表现由儿科内分泌专家确定。结果:表现出高雄激素血症的21OHD携带者组在纯合性上富集了CAPN-UCSNP44罕见变异(4.9 vs. 0.4%, NCBI数据为一般人群;P = 0.004)。在我们的患者和对照组中,观察到这种多态性和另一种多态性TNFR2-196R的对比分布。在隐性模型中,它们的罕见变异在高表达型(p = 0.048)和低表达型(p = 0.034)中分别被检出的频率更高。结论:21odd相关的儿童高雄激素血症遵循单基因和多基因模式。CAPN-UCSNP44和TNFR2-M196R罕见变异体在临床表达方面的相反行为表明,这些变异体分别是肾上腺高雄激素症的致敏因子和保护因子。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Monogenic and polygenic models detected in steroid 21-hydroxylase deficiency-related paediatric hyperandrogenism.

Aims: Hyperandrogenism, although mostly due to polygenic interactions, is monogenic for some enzymatic adrenal deficiencies. This study evaluates mono- and biallelic 21-hydroxylase deficiency (21OHD)-related hyperandrogenism in pediatric patients. Sensitizing and protective polymorphisms were investigated in carriers and cryptic forms of 21OHD.

Methods: The study involved a monogenic analysis of CYP21A2 in patients (375 nonclassical 21OHD [NC21OHD] children; 306 hyperandrogenic 21OHD carriers, n = 306) and a polygenic association study (CAPN10-UCSNP44, PON1-108, TNFR2-M196R, IGF2-ApaI and IRS1-G972R polymorphisms) of 170 hyperandrogenic carriers plus 277 family members (control groups). The metabolic marker 17OH progesterone defined the degree of deficiency; clinical expressivity was determined by pediatric endocrinologists.

Results: The group of 21OHD carriers manifesting hyperandrogenism was enriched in the CAPN-UCSNP44 rare variant in homozygosity (4.9 vs. 0.4%, NCBI data for the general population; p = 0.004). In our patients and controls, contrasting distributions were observed for this and another polymorphism, TNFR2-196R. In a recessive model, their rare variants were more frequently detected among the forms with high (p = 0.048) and low (p = 0.034) expressivity respectively.

Conclusions: 21OHD-related pediatric hyperandrogenism follows monogenic and polygenic models. The opposite behaviors in terms of clinical expressivity detected for CAPN-UCSNP44 and TNFR2-M196R rare variants suggest these variants to be sensitizing and protective factors respectively in adrenal hyperandrogenism.

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Hormone research
Hormone research 医学-内分泌学与代谢
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