儿童肥厚型心肌病中Noonan综合征基因型与临床表型

doi:10.12372/jcp.2023.21e1258

临床儿科杂志 ›› 2023, Vol. 41 ›› Issue (2): 125-129.doi: 10.12372/jcp.2023.21e1258

儿童肥厚型心肌病中Noonan综合征基因型与临床表型

朱晓丽¹, 杨倩利¹, 王博¹, 拓胜军¹, 赵雪丽¹, 李静¹, 成胜全², 刘丽文¹()

1.空军军医大学第一附属医院超声医学科，（陕西西安 710032）
2.空军军医大学第一附属医院儿科（陕西西安 710032）

收稿日期:2021-08-30 出版日期:2023-02-15 发布日期:2023-02-16
通讯作者: 刘丽文电子信箱：liuliwen@fmmu.edu.cn
基金资助:
陕西省重点研发项目(2019KW-076);国家自然科学基金项目(81901755);国家自然科学基金项目(82071932);国家自然科学基金项目(82001831);西京医院学科助推项目(XJZT19MJ01);空军军医大学临床研究资助计划(2021XD010);陕西省基金项目(2020JQ-463)

Genotypes and clinical phenotypes of Noonan syndrome in children with hypertrophic cardiomyopathy

ZHU Xiaoli¹, YANG Qianli¹, WANG Bo¹, TA Shengjun¹, ZHAO Xueli¹, LI Jing¹, CHENG Shengquan², LIU Liwen¹()

1. Department of Ultrasound, The First Affiliated Hospital of Air Force Medical University, Xi?an 710032, Shaanxi, China
2. Department of Pediatrics, The First Affiliated Hospital of Air Force Medical University, Xi'an 710032, Shaanxi, China

Received:2021-08-30 Online:2023-02-15 Published:2023-02-16

摘要/Abstract

摘要：

目的总结儿童肥厚型心肌病（HCM）中Noonan综合征的基因变异与临床特征。方法对123例儿童肥厚型心肌病先证者进行96个遗传性心肌病相关基因的二代测序及生物信息学分析，确定变异位点;筛选出11例Noonan综合征患儿，收集其临床资料及超声心动图结果。结果 11例患儿均因心肌肥厚就诊，男5例、女6例，肥厚型心肌病诊断中位年龄2岁7个月（5个月~10岁），Noonan综合征诊断中位年龄6岁9个月（7个月~16岁）。11例患儿中10例为3号染色体RAF1基因型，1例为12号染色体PTPN11基因型;7例为新发变异，其中1例RAF1基因患儿检测出同时携带与肥厚型心肌病相关的变异基因MYBPC3。11例患儿中9例具有典型Noonan综合征面部特征。11例患儿均为肥厚型心肌病，9例为梗阻性肥厚型心肌病，合并右室流出道梗阻2例，合并先天性心脏病7例。结论以肥厚型心肌病为表型的儿童Noonan综合征多为RFA1基因型，易发生左心室流出道梗阻且多合并先天性心脏病。

关键词: Noonan综合征, PTPN11基因, RAF1基因, 肥厚型心肌病, 先天性心脏病

Abstract:

Objective To retrospectively summarize the genetic variants and clinical characteristics of Noonan syndrome in children with hypertrophic cardiomyopathy (HCM). Methods A total of 123 children with HCM were enrolled in this study. Second generation sequencing and bioinformatic analysis of 96 genes associated with hypertrophic cardiomyopathy were performed in 123 probands. Eleven patients with diagnosed with Noonan syndrome, and their clinical data and echocardiographic findings were collected. Results The median age of diagnosis of HCM was 2 years and 7 months (5 months to 10 years), and the median age of diagnosis of Noonan syndrome was 6 years and 9 months (7 months to 16 years). 10 of 11 children had variants in RAF1 gene on chromosome 3, one had variant in PTPN11 gene on chromosome 12, and 7 had other novel variants. One of the patients with RAF1 was also found carrying variant in MYBPC3 which is associated with HCM. Nine out of 11 patients with HCM had typical facial features of Noonan syndrome. All 11 children had hypertrophic cardiomyopathy, 9 with obstructive hypertrophic cardiomyopathy, 2 with right ventricular outflow tract obstruction, and 7 with congenital heart disease. Conclusion RFA1 mutation is commonly seen in children with HCM in Noonan syndrome. Those patients carried with RFA1 mutation are more likely to have left ventricular outflow track obstruction and congenital heart diseases.

Key words: Noonan syndrome, PTPN11 gene, RAF1 gene, hypertrophic cardiomyopathy, congenital heart disease

朱晓丽, 杨倩利, 王博, 拓胜军, 赵雪丽, 李静, 成胜全, 刘丽文. 儿童肥厚型心肌病中Noonan综合征基因型与临床表型[J]. 临床儿科杂志, 2023, 41(2): 125-129.

ZHU Xiaoli, YANG Qianli, WANG Bo, TA Shengjun, ZHAO Xueli, LI Jing, CHENG Shengquan, LIU Liwen. Genotypes and clinical phenotypes of Noonan syndrome in children with hypertrophic cardiomyopathy[J]. Journal of Clinical Pediatrics, 2023, 41(2): 125-129.

图/表 3

表1

图1

表2

参考文献 17

[1]	刘晓亮. Noonan综合征的诊治进展[J]. 临床儿科杂志, 2016, 34(1): 64-67.
[2]	Roberts AE, Allanson JE, Tartaglia M, et al. Noonan syndrome[J]. Lancet, 2013, 381(9863): 333-342. doi: 10.1016/S0140-6736(12)61023-X pmid: 23312968
[3]	刘霞, 苏喆. Noonan综合征的诊断治疗进展[J]. 中华实用儿科临床杂志, 2014, 29(20): 1531-1533.
[4]	Ommen SR, Mital S, Burke MA, et al. 2020 AHA/ACC guideline for the diagnosis and treatment of patients with hypertrophic cardiomyopathy: executive summary: a report of the American College of Cardiology/American Heart Association Joint Committee on Clinical Practice Guidelines[J]. J Am Coll Cardiol, 2020, 76(25): 3022-3055. doi: 10.1016/j.jacc.2020.08.044
[5]	Lang RM, Badano LP, Mor-Avi V, et al. Recommendations for cardiac chamber quantification by echocardiography in adults: an update from the American Society of Echocardiography and the European Association of Cardiovascular Imaging[J]. J Am Soc Echocardiogr, 2015, 28(1): 1-39. e14. doi: 10.1016/j.echo.2014.10.003
[6]	Richards S, Aziz N, Bale S, et al. Standards and guidelines for the interpretation of sequence variants: a joint consensus recommendation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology[J]. Genet Med, 2015, 17(5): 405-424. doi: 10.1038/gim.2015.30 pmid: 25741868
[7]	罗光月, 陆韦. Noonan综合征发病机制的研究进展[J]. 疑难病杂志, 2021, 20(10): 1077-1080.
[8]	Romano AA, Allanson JE, Dahlgren J, et al. Noonan syndrome: clinical features, diagnosis, and management guidelines[J]. Pediatrics, 2010, 126(4): 746-759. doi: 10.1542/peds.2009-3207 pmid: 20876176
[9]	Wu X, Yin J, Simpson J, et al. Increased BRAF heterodimerization is the common pathogenic mechanism for Noonan syndrome-associated RAF1 mutants[J]. Mol Cell Biol, 2012, 32(19): 3872-3890. doi: 10.1128/MCB.00751-12
[10]	李辛, 王秀敏, 王剑, 等. Noonan综合征的临床实践指南[J]. 中华医学遗传学杂志, 2020, 37(3): 324-328.
[11]	Lioncino M, Monda E, Verrillo F, et al. Hypertrophic cardiomyopathy in RASopathies: diagnosis, clinical characteristics, prognostic implications, and management[J]. Heart Fail Clin, 2021, 18(1): 19-29. doi: 10.1016/j.hfc.2021.07.004
[12]	Pierpont ME, Digilio MC. Cardiovascular disease in Noonan syndrome[J]. Curr Opin Pediatr, 2018, 30(5): 601-608. doi: 10.1097/MOP.0000000000000669 pmid: 30024444
[13]	James D, April M, Bonnie A, et al. Outcomes in chlidren with Noonan syndrome and hypertrophic cardiomyopathy: a study from the pediatric cardiomyopathy registry[J]. Am Heart J, 2012, 164(3): 442-448. doi: 10.1016/j.ahj.2012.04.018
[14]	Prendiville TW, Gauvreau K, Tworog-Dube E, et al. Cardiovascular disease in Noonan syndrome[J]. Arch Dis Child, 2014, 99(7): 629-634. pmid: 24534818
[15]	Tartaglia M, Gelb BD, Zenker M. Noonan syndrome and clinically related disorders[J]. Best Pract Res Clin Endocrinol Metab, 2011, 25(1): 161-179. doi: 10.1016/j.beem.2010.09.002 pmid: 21396583
[16]	Tafazoli A, Eshraghi P, Koleti ZK, et al. Noonan syndrome - a new survey[J]. Arch Med Sci, 2017, 13(1): 215-222. doi: 10.5114/aoms.2017.64720 pmid: 28144274
[17]	Tartaglia M, Zampino G, Gelb BD. Noonan syndrome: clinical aspects and molecular pathogenesis[J]. Mol Syndromol, 2010, 1(1): 2-26. doi: 10.1159/000276766 pmid: 20648242

患儿	基因	核苷酸	氨基酸	来源	外显子	ACMG分析
例1	RAF1	c.788T>C	V263A	新发	exon7	致病性
例2	RAF1	c.781C>G	P261T	新发	exon7	致病性
例3	PTPN11	c.1528C>G	Q510E	未测	exon13	致病性
例4	RAF1	c.781C>T	P261S	新发	exon7	致病性
例4	MYBPC3	c.2684G>A	R895H	父源	exon25	临床意义未明
例5	RAF1	c.788T>C	V263A	新发	exon7	致病性
例6	RAF1	c.788T>C	V263A	新发	exon7	致病性
例7	RAF1	c.770C>T	S257L	未测	exon7	致病性
例8	RAF1	c.781C>T	P261S	未测	exon7	致病性
例9	RAF1	c.770C>T	S257L	未测	exon7	致病性
例10	RAF1	c.775T>A	S259T	新发	exon7	致病性
例11	RAF1	c.786T>A	A262L	新发	exon7	致病性

儿童肥厚型心肌病中Noonan综合征基因型与临床表型

Genotypes and clinical phenotypes of Noonan syndrome in children with hypertrophic cardiomyopathy

RichHTML

PDF (PC)

赞

可视化

摘要/Abstract

引用本文

使用本文

图/表 3

参考文献 17

相关文章 15

Metrics

本文评价

推荐阅读 0

[1]	阮雪华, 孙晶, 孙锟. 环境相关因素与先天性心脏病研究进展[J]. 临床儿科杂志, 2023, 41(3): 229-234.
[2]	陈艳华, 尹丹, 郑敏, 吕铁伟, 易岂建, 李谧, 向平. 经导管介入封堵治疗儿童动脉导管未闭合并二尖瓣反流疗效评价[J]. 临床儿科杂志, 2022, 40(7): 517-521.
[3]	刘佐嘉, 王秀敏, 唐佳丽, 等. Noonan 综合征患儿照护负担对生活质量的影响[J]. 临床儿科杂志, 2021, 39(9): 677-.
[4]	陈瑜, 徐维虹, 汪思园. 先天性心脏病患儿体外循环后发生低体温风险的列线图模型建立与评价[J]. 临床儿科杂志, 2021, 39(9): 682-.
[5]	缪文华,刘晓燕. 伴有左心室扩大的儿童肥厚型心肌病临床特征及预后[J]. 临床儿科杂志, 2021, 39(4): 241-.
[6]	陈颖慧，张琪. 调控动脉导管闭合的分子机制研究进展[J]. 临床儿科杂志, 2021, 39(11): 869-.
[7]	王桂喜,孙锟,孔令晖,等. SNParray分析技术在胎儿先天性心脏病诊断中的价值[J]. 临床儿科杂志, 2021, 39(10): 726-.
[8]	周云国，张政，许飞，等. 应用室间隔缺损封堵器治疗婴幼儿特殊形状动脉导管未闭疗效观察[J]. 临床儿科杂志, 2020, 38(9): 679-.
[9]	傅行鹏，叶菁菁，俞劲，等. 先天性心脏病合并感染性心内膜炎42 例患儿超声分析[J]. 临床儿科杂志, 2020, 38(2): 129-.
[10]	王智利，罗斯颖，易茜，等. CPAP 在先天性心脏病合并重症肺炎心功能不全患儿中的应用[J]. 临床儿科杂志, 2020, 38(1): 10-.
[11]	王野峰，胡原，杨舟，等. 儿童先天性心脏病合并心肌致密化不全的介入治疗及随访分析[J]. 临床儿科杂志, 2020, 38(1): 49-.
[12]	刘子勤，陈晓波，宋福英. Noonan 综合征7 例临床及遗传学分析[J]. 临床儿科杂志, 2019, 37(9): 661-.
[13]	徐蒙蒙，徐月娟，陈　笋，等. 内脏异位综合征患儿中DNAI1 和DNAH5 基因编码区突变分析[J]. 临床儿科杂志, 2019, 37(7): 494-.
[14]	周双,　石鑫,　陈笋,　于昱. 环境影响 DNA 甲基化及导致先天性心脏病发生的研究进展[J]. 临床儿科杂志, 2018, 36(8): 630-.
[15]	潘诚,　邹小明,　陈刚,　王涛,　江先宇,　陈建勇 . 体格检查、脉搏血氧饱和度筛查和灌注指数在新生儿先天性心脏病筛查中的作用[J]. 临床儿科杂志, 2018, 36(3): 166-.

患儿	年龄/岁	IVST/mm	LVPWT/mm	LVOT/mmHg	RVOT/mmHg	PV/cm·s^-1	PV/mmHg	EF/%	ASD	CoA
例1	2	12	4	70	5	115	5	68	-	-
例2	6	22	13	68	6	115	5	67	-	+
例3	10	13	10	62	21	130	7	72	-	-
例4	11	9	5	62	2	90	3	72	+	-
例5	1.4	7	4	10	5	319	41	61	-	-
例6	1.4	14	5	7	2	310	39	57	-	-
例7	0.7	15	4	36	60	423	72	68	+	-
例8	0.9	12	4	38	6	118	5	73	+	-
例9	12	27	10	34	60	120	6	70	+	-
例10	15	37	11	31	14	99	4	65	+	-
例11	16	21	13	42	9	130	7	68	-	-