BRAF基因变异8例临床分析

doi:10.12372/jcp.2023.22e1562

临床儿科杂志 ›› 2023, Vol. 41 ›› Issue (9): 697-702.doi: 10.12372/jcp.2023.22e1562

BRAF基因变异8例临床分析

欧跃徐, 段远辉, 曹洁(), 李洁玲

重庆医科大学附属儿童医院全科医学科儿科学重庆市实验室儿童发育疾病研究教育部重点实验室儿童发育重大疾病国家国际科技合作基地国家儿童健康与疾病临床医学研究中心（重庆 400014）

收稿日期:2022-11-22 出版日期:2023-09-15 发布日期:2023-09-05
通讯作者: 曹洁 E-mail:caojie0220@163.com

Clinical analysis of 8 children with BRAF gene variation

OU Yuexu, DUAN Yuanhui, CAO Jie(), LI Jieling

Department of Medical General Ward, Children’s Hospital of Chongqing Medical University, Ministry of Education Key Laboratory of Child Development and Disorders, National Clinical Research Center for Child Health and Disorders, China International Science and Technology Cooperation Base of Child Development and Critical Disorders, National Clinical Research Center for Child Health and Disorders, Chongqing 400014, China

Received:2022-11-22 Online:2023-09-15 Published:2023-09-05
Contact: CAO Jie E-mail:caojie0220@163.com

摘要/Abstract

摘要：

目的探讨BRAF基因变异类型及其临床特征。方法回顾性分析8例存在BRAF基因变异患儿的临床资料及基因变异类型。结果 8例患儿中4例源于生殖细胞变异，另4例源于体细胞变异。源于生殖细胞变异的4例患儿均表现为心-面-皮肤（CFC）综合征临床特征，属于极其罕见的疾病，均具有特殊面容、发育迟滞、皮肤毛发异常表现，部分患儿还存在癫痫、心脏畸形等表现，均属于BRAF基因的新发变异，但变异位点不同。源于体细胞变异的4例患儿中，2例表现为朗格罕斯细胞组织细胞增生症（LCH），另2例表现为中枢神经系统恶性肿瘤。结论 BRAF基因变异在生殖细胞时，可出现严重的发育障碍，表现为心-面-皮肤综合征的临床特征;变异在体细胞时，可出现肿瘤、LCH等。

关键词: BRAF基因, 心-面-皮肤综合征, 肿瘤

Abstract:

Objective To investigate the variants and clinical characteristics of BRAF gene. Methods The clinical data and types of gene variation in 8 cases of children with BRAF gene variation were retrospectively analyzed. Results Eight children had BRAF gene variations, four of which were derived from germ cells and the other four from somatic cells. The 4 patients with BRAF gene variations from germ cells all showed clinical features of cardio-facio-cutaneous (CFC) syndrome, which is an extremely rare disease. They all have special facial features, developmental retardation, skin and hair abnormalities, and some children also have epilepsy, heart malformation and other manifestations. They were all new variations in the BRAF gene, but the variation sites were different. Of the 4 children whose BRAF gene variations originated from somatic cells, 2 presented with Langerhans cell histiocytosis (LCH), and the other 2 presented with central nervous system malignant tumors. Conclusions When BRAF gene variation occurs in germ cells, children can develop severe developmental disorders that can present as clinical features of CFC syndrome. When BRAF gene variation occurs in somatic cells, it can cause tumors and LCH, etc.

Key words: BRAF gene, cardio-facio-cutaneous syndrome, tumor

欧跃徐, 段远辉, 曹洁, 李洁玲. BRAF基因变异8例临床分析[J]. 临床儿科杂志, 2023, 41(9): 697-702.

OU Yuexu, DUAN Yuanhui, CAO Jie, LI Jieling. Clinical analysis of 8 children with BRAF gene variation[J]. Journal of Clinical Pediatrics, 2023, 41(9): 697-702.

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参考文献 15

[1]	Ullah R, Yin Q, Snell AH, et al. RAF-MEK-ERK pathway in cancer evolution and treatment[J]. Semin Cancer Biol, 2022, 85: 123-154. doi: 10.1016/j.semcancer.2021.05.010
[2]	Hussain MR, Baig M, Mohamoud HS, et al. BRAF gene: from human cancers to developmental syndromes[J]. Saudi J Biol Sci, 2015, 22(4): 359-373. doi: 10.1016/j.sjbs.2014.10.002
[3]	Dard L, Bellance N, Lacombe D, et al. RAS signalling in energy metabolism and rare human diseases[J]. Biochim Biophys Acta Bioenerg, 2018, 1859(9): 845-867. doi: 10.1016/j.bbabio.2018.05.003
[4]	Meng P, Bedolla RG, Yun H, et al. Contextual role of E2F1 in suppression of melanoma cell motility and invasiveness[J]. Mol Carcinog, 2019, 58(9): 1701-1710. doi: 10.1002/mc.v58.9
[5]	Cao H, Alrejaye N, Klein OD, et al. A review of craniofacial and dental findings of the RASopathies[J]. Orthod Craniofac Res, 2017, 20 (Suppl 1): 32-38. doi: 10.1111/ocr.2017.20.issue-S1
[6]	Poulikakos PI, Sullivan RJ, Yaeger R, et al. Molecular pathways and mechanisms of BRAF in cancer therapy[J]. Clin Cancer Res, 2022, 28(21): 4618-4628. doi: 10.1158/1078-0432.CCR-21-2138 pmid: 35486097
[7]	Hebron KE, Hernandez ER, Yohe ME, et al. The RASopathies: from pathogenetics to therapeutics[J]. Dis Model Mech, 2022, 15(2): dmm049107. doi: 10.1242/dmm.049107
[8]	Rauen KA. The RASopathies[J]. Annu Rev Genom Hum G, 2013, 14(1): 355-369. doi: 10.1146/genom.2013.14.issue-1
[9]	Suzuki-Muromoto S, Miyabayashi T, Nagai K, et al. Leucine-485 deletion variant of BARF may exhibit the severe end of the clinical spectrum of CFC syndrome[J]. J Hum Genet, 2019, 64(5): 499-504. doi: 10.1038/s10038-019-0579-3 pmid: 30842599
[10]	Pierpont ME, Magoulas PL, Adi S, et al. Cardio-facio-cutaneous syndrome: clinical features, diagnosis, and management guidelines[J]. Pediatrics, 2014, 134(4): e1149-e1162.
[11]	陈柏谕, 尹飞, 陈施梦, 等. BRAF基因突变所致心-面-皮肤综合征1例并文献复习[J]. 中南大学学报(医学版), 2021, 46(4): 432-437.
[12]	Jhang WK, Choi JH, Lee BH, et al. Cardiac manifestations and associations with gene mutations in patients diagnosed with RASopathies[J]. Pediatr Cardiol, 2016, 37(8): 1539-1547. pmid: 27554254
[13]	Pierpont EI, Kenney-Jung DL, Shanley R, et al. Neurologic and neurodevelopmental complications in cardiofaciocutaneous syndrome are associated with genotype: a multinational cohort study[J]. Genet Med, 2022, 24(7): 1556-1566. doi: 10.1016/j.gim.2022.04.004 pmid: 35524774
[14]	Zenker M, Edouard T, Blair JC, et al. Noonan syndrome: improving recognition and diagnosis[J]. Arch Dis Child, 2022, 107(12): 1073-1078. doi: 10.1136/archdischild-2021-322858 pmid: 35246453
[15]	Feng S, Han L, Yue M, et al. Frequency detection of BRAF V600E mutation in a cohort of pediatric langerhans cell histiocytosis patients by next-generation sequencing[J]. Orphanet J Rare Dis, 2021, 16(1): 272. doi: 10.1186/s13023-021-01912-3

病人编号		例1	例2	例3	例4
就诊年龄		1岁2月	4月13天	2岁	1岁3月
性别		男	男	女	女
出生史		足月，窒息史	36⁺³周早产	34⁺³周早产	足月，窒息史
基因检测（BRAF变异位点）		ch7:140477806，exon12， c.1502A>G(p.E501G)	ch7:140453133，exon15， c.1802A>T(p.K601I)	ch7:140453133，exon6， c.722C>T(p.T241M)	chr7:140501350，exon16， c.1914T>G(P.D638E)
心脏异常		﹢/①②	﹢/①③	-	﹢/①
特殊面容		﹢	﹢	﹢	﹢
皮肤毛发异常		﹢	﹢	﹢	﹢
发育迟滞		﹢	﹢	﹢	﹢
Gesell （DQ评分）	大运动	50分	50分	31分	11分
	精细运动	36分	58分	37分	0分
	应物	30分	58分	32分	5分
	应人	33分	42分	30分	3分
	语言	31分	33分	30分	2分
癫痫		-	﹢	-	﹢
脑电图异常		﹢	﹢	﹢	﹢
头颅MRI		﹢/④	﹢/⑤	﹢/⑤⑥	﹢/⑥⑦
其他系统异常		亚临床甲减，喉软骨发育不良，枕部血管瘤，睡眠障碍，间歇性外斜视，眼球震颤	隐睾，身材矮小	睡眠障碍	喂养困难，重度营养不良
目前情况		5岁，随访中，康复训练中，未使用AEDs，脑电图无明显改善，不能说话，不能示二便及自主进食，可跑跳	6岁，随访中，左乙拉西坦治疗中，康复训练中，未再癫痫发作，脑电图无明显改善，不能说话，不能示二便及自主进食，可跑跳	7岁，随访中，丙戊酸-左乙拉西坦-丙戊酸治疗，脑电图无改善，丙戊酸减停中，不能说话，不能示二便及自主进食，可跑跳	9岁，随访中，难治性癫痫、癫痫脑病表现，奥卡西平、左乙拉西坦、托吡酯、硝西泮治疗中，仍有癫痫发作2次/d，长期卧床，重度营养不良

BRAF基因变异8例临床分析

Clinical analysis of 8 children with BRAF gene variation

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