11p15印记中心区域1甲基化缺失是典型罗素-西尔弗综合征常见且特定的病因:临床评分系统及表观遗传学-表型相关性
11p15 imprinting center region 1 loss of methylation is a common and specific cause of typical Russell-Silver syndrome: clinical scoring system and epigenetic-phenotypic correlations.
作者信息
Netchine Irène, Rossignol Sylvie, Dufourg Marie-Noëlle, Azzi Salah, Rousseau Alexandra, Perin Laurence, Houang Muriel, Steunou Virginie, Esteva Blandine, Thibaud Nathalie, Demay Marie-Charles Raux, Danton Fabienne, Petriczko Elzbieta, Bertrand Anne-Marie, Heinrichs Claudine, Carel Jean-Claude, Loeuille Guy-André, Pinto Graziella, Jacquemont Marie-Line, Gicquel Christine, Cabrol Sylvie, Le Bouc Yves
机构信息
Hôpital Armand-Trousseau, Explorations Fonctionnelles Endocriniennes, Paris 75012, France.
出版信息
J Clin Endocrinol Metab. 2007 Aug;92(8):3148-54. doi: 10.1210/jc.2007-0354. Epub 2007 May 15.
CONTEXT
Russell-Silver syndrome (RSS), characterized by intrauterine and postnatal growth retardation, dysmorphic features, and frequent body asymmetry, spares cranial growth. Maternal uniparental disomy for chromosome 7 (mUPD7) is found in 5-10% of cases. We identified loss of methylation (LOM) of 11p15 Imprinting Center Region 1 (ICR1) domain (including IGF-II) as a mechanism leading to RSS.
OBJECTIVE
The aim was to screen for 11p15 epimutation and mUPD7 in RSS and non-RSS small-for-gestational-age (SGA) patients and identify epigenetic-phenotypic correlations. STUDIED POPULATION AND METHODS: A total of 127 SGA patients were analyzed. Clinical diagnosis of RSS was established when the criterion of being SGA was associated with at least three of five criteria: postnatal growth retardation, relative macrocephaly, prominent forehead, body asymmetry, and feeding difficulties. Serum IGF-II was evaluated for 82 patients.
RESULTS
Of the 127 SGA patients, 58 were diagnosed with RSS; 37 of these (63.8%) displayed partial LOM of the 11p15 ICR1 domain, and three (5.2%) had mUPD7. No molecular abnormalities were found in the non-RSS SGA group (n = 69). Birth weight, birth length, and postnatal body mass index (BMI) were lower in the abnormal 11p15 RSS group (ab-ICR1-RSS) than in the normal 11p15 RSS group [-3.4 vs.-2.6 SD score (SDS), -4.4 vs.-3.4 SDS, and -2.5 vs.-1.6 SDS, respectively; P < 0.05]. Among RSS patients, prominent forehead, relative macrocephaly, body asymmetry, and low BMI were significantly associated with ICR1 LOM. All ab-ICR1-RSS patients had at least four of five criteria of the scoring system. Postnatal IGF-II levels were within normal values.
CONCLUSION
The 11p15 ICR1 epimutation is a major, specific cause of RSS exhibiting failure to thrive. We propose a clinical scoring system (including a BMI < -2 SDS), highly predictive of 11p15 ICR1 LOM, for the diagnosis of RSS.
背景
罗素 - 西尔弗综合征(RSS)的特征为宫内和出生后生长迟缓、畸形特征以及频繁的身体不对称,但颅骨生长不受影响。5% - 10%的病例中可发现母源7号染色体单亲二倍体(mUPD7)。我们发现11p15印记中心区域1(ICR1)结构域(包括胰岛素样生长因子II,IGF-II)的甲基化缺失(LOM)是导致RSS的一种机制。
目的
旨在筛查RSS和非RSS的小于胎龄儿(SGA)患者中的11p15表观突变和mUPD7,并确定表观遗传与表型的相关性。研究人群与方法:共分析了127例SGA患者。当SGA标准与以下五项标准中的至少三项相关时,确立RSS的临床诊断:出生后生长迟缓、相对巨头畸形、前额突出、身体不对称和喂养困难。对82例患者评估了血清IGF-II水平。
结果
在127例SGA患者中,58例被诊断为RSS;其中37例(63.8%)表现出11p15 ICR1结构域的部分LOM,3例(5.2%)有mUPD7。非RSS的SGA组(n = 69)未发现分子异常。异常的11p15 RSS组(ab - ICR1 - RSS)的出生体重、出生身长和出生后体重指数(BMI)低于正常的11p15 RSS组[分别为 - 3.4 vs. - 2.6标准差评分(SDS), - 4.4 vs. - 3.4 SDS,以及 - 2.5 vs. - 1.6 SDS;P < 0.05]。在RSS患者中,前额突出、相对巨头畸形、身体不对称和低BMI与ICR1 LOM显著相关。所有ab - ICR1 - RSS患者在评分系统的五项标准中至少有四项符合。出生后IGF-II水平在正常范围内。
结论
11p15 ICR1表观突变是RSS出现生长发育不良的主要特定原因。我们提出了一种临床评分系统(包括BMI < - 2 SDS),对诊断RSS具有高度预测11p15 ICR1 LOM的能力。
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