新生儿高氨血症多中心现状调查及临床分析

doi:10.12372/jcp.2023.22e1736

摘要/Abstract

摘要：

目的通过回顾性多中心现状调查，了解新生儿高氨血症的发病率、病因分类、临床特征及预后情况。方法以2017年1月—2022年11月28家参与单位分娩并入住新生儿科治疗的血氨>100 μmol/L的新生儿作为研究对象，用描述性研究方法对确诊高氨血症新生儿的发病率、病因分类、临床特征、基因表型及预后随访等情况进行分析总结。结果观察期间28家单位总分娩量708 421例，73例符合新生儿高氨血症诊断标准，其中男44例、女29例。病因分类中先天遗传性高氨血症32.88%（24例），暂时性高氨血症15.07%（11例），继发性高氨血症16.44%（12例），另有26例原因不明（35.61%）。主要临床表现有反应差、气促、喂养困难、抽搐、意识障碍等。主要异常实验室检查为代谢性酸中毒、血乳酸增高、低血糖、电解质紊乱，血氨基酸和/或尿氨基酸异常，13例进行了基因检查的患儿中11例发现异常。治疗上除常规对症支持治疗外，主要采用了精氨酸排氨（21例）、补充肉碱（8例）、血液净化（9例）以及腹膜透析（3例）。预后方面，24例先天遗传性高氨血症患儿死亡10例，放弃治疗6例，好转出院8例；12例继发性高氨血症患儿死亡1例，放弃治疗3例，预后不详1例，治愈出院7例；11例暂时性高氨血症患儿均治愈或好转出院；而26例不明原因高氨血症病例死亡17例，放弃治疗4例，预后不详3例，好转出院2例。结论新生儿高氨血症发病率不高，但病情进展快，病死率高，尤其是先天性遗传高氨血症和不明原因高氨血症病例。提高临床医师对该病的认识，尽量做到早诊断，早治疗，可减少死亡及严重并发症。加强产前咨询，建立新生儿高氨血症筛查体系和新生儿高氨血症注册登记系统，具有积极的临床意义。

关键词: 高氨血症, 先天性遗传代谢性疾病, 新生儿

Abstract:

Objective To investigate the incidence, etiological classification, clinical features and prognosis of neonatal hyperammonemia through a retrospective multi-center status survey. Methods Neonatal patients with blood ammonia levels more than 100 μmol/L who were treated in 28 participating units between January 2017 and November 2022 made up the study population. The incidence, etiological classification, clinical traits, genetic phenotype, and prognostic follow-up of neonates with confirmed hyperammonemia were analyzed using descriptive study methodologies. Results During the observation period, the total number of deliveries in 28 units was 708421, and 73 newborns met the diagnostic criteria of neonatal hyperammonemia, including 44 boys and 29 girls. The etiological classification included congenital hyperammonemia (24 cases, 32.88%), transient hyperammonemia (11 cases, 15.07%), secondary hyperammonemia (12 cases, 16.44%), and unexplained hyperammonemia (26 cases, 35.61%). The main clinical manifestations were poor response, shortness of breath, feeding difficulties, convulsions and impaired consciousness. The main abnormal laboratory tests were metabolic acidosis, increased blood lactate, hypoglycemia, electrolyte disorders, abnormal blood and/or urine amino acids. Genetic tests were performed in 13 patients, and abnormalities were found in 11 of them. In addition to conventional symptomatic supportive treatment, arginine intravenous drip (21 cases), carnitine supplementation (8 cases), blood purification (9 cases) and peritoneal dialysis (3 cases) were mainly used. The prognosis for the 24 cases of congenital hereditary hyperammonemia was 10 deaths, 6 treatment discontinuations, and 8 discharges. Among the 12 children with secondary hyperammonemia, 1 died, 3 gave up treatment, 1 had an unknown prognosis, and 7 were cured and discharged from hospital. All 11 cases of temporary hyperammonemia were cured or improved and discharged from hospital. Among 26 cases of unknown hyperammonemia, 17 died, 4 gave up treatment, 3 had unknown prognosis, and 2 were discharged from hospital after improvement. Conclusions Neonatal hyperammonemia is uncommon, but it progresses swiftly and has a high risk of mortality, particularly in cases of congenital genetic hyperammonemia and unexplained hyperammonemia. Raising doctors' awareness of the condition and promoting early detection and treatment can reduce mortality and serious consequences. Moreover, setting up screening and registration procedures for newborn hyperammonemia as well as improving prenatal consultation are helpful for clinical outcomes.

Key words: hyperammonemia, congenital inherited metabolic diseases, neonate

深圳新生儿数据协作网. 新生儿高氨血症多中心现状调查及临床分析[J]. 临床儿科杂志, 2023, 41(4): 252-258.

Shenzhen Neonatal Data Network. A multicenter survey and clinical analysis of neonatal hyperammonemia[J]. Journal of Clinical Pediatrics, 2023, 41(4): 252-258.

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73例高氨血症患儿临床特征、实验室检查、治疗、预后及随访"

病因分类	具体疾病（原发病）	性别（例数）	胎龄/周	入院天数/d	血氨峰值 /μmol·L^-1	临床表现	常规实验室检查	治疗方式
先天遗传性代谢病	鸟氨酸氨甲酰基转移酶缺乏症	男(2)	38.78 （38.62~38.96）	1.52 （0.78~2.26）	1 590 （1 545~1 635）	发热、气促、呻吟、呕吐、抽搐、抽泣样呼吸、昏迷	血乳酸、肝酶增高，电解质紊乱	均机械通气、精氨酸静滴
	瓜氨酸血症	男(4)	39.14 （38.25~39.93）	4.5 (3.5~5.5)	867.75 （575.73~1 232.25）	同上	同上	血液净化1例，精氨酸静滴2例，左旋肉碱2例
	高鸟氨酸血症-高氨血症-高同型瓜氨酸尿症	女(1)	38.71	40	320.8	同上	不详	精氨酸静滴
	肉碱棕榈酰转移酶或移位酶	男(1) 女(2)	38.86 （38.50~39.21）	1 (0.52~1.50)	1 115 （887.0~2 247.5）	同上，心脏骤停	同上	血液净化2例，精氨酸静滴1例，纠酸3例
	甲基丙二酸血症	男(4) 女(1)	39.43 （39.00~39.89）	4 (3~6)	1 277 （257.6~1 369）	同上，心脏骤停	同上	纠酸补液、精氨酸静滴3例，血液净化2例，腹膜透析2例
	戊二酸血症II型	男(2) 女(3)	38.93 （38.43~39.43）	3 (1~3)	183 （170.1~302.4）	同上，心脏骤停	同上、低血糖	左旋肉碱4例，专用奶粉、精氨酸静滴2例，口服核黄素3例
	丙酸血症	男(2) 女(1)	38.71 （38.71~39.28）	4 （3.5~4.0）	454.1 （340.70~1 033.55）	同上	不详	精氨酸静滴1例，左旋肉碱1例，换血1例
	异戊酸血症	女(1)	38.28	14	695.3	同上	不详	精氨酸静滴
继发性高氨血症	新生儿窒息	男(2) 女(1)	39.86 （37.86~40.36）	0.04 （0.03~0.23）	107.2 （105.95~370.10）	同上	同上+脑软化	禁食、补液、机械通气
	新生儿肺炎	男(1) 女(1)	40.07 （39.61~40.54）	1.5 （0.75~2.25）	120.9 （115.35~126.45）	同上	同上	呼吸循环支持、抗感染、纠酸
	低血糖脑病	男(1)	37.85	2	234.6	同上	同上	同上
	顽固性低血糖	男(1)	40.85	0.3	1 155	同上	同上	同上
	坏死性小肠结肠炎（ⅢB）先天性胆道闭锁	男(1)	34.57	21	292.6	反复腹胀	同上+气腹+结肠细小+先天性胆道闭锁（腹部/造影和彩超）	同上
	心肌致密化不全	男(1)	38.57	34	183	气促、发绀、反应差	同上	同上
	新生儿败血症感染性休克	男(1)	40.28	1	360	同上	同上+脑梗塞	精氨酸静滴
	先天性心脏病（主动脉缩窄）	女(1)	40.42	2	408	同上	同上	呼吸循环支持、抗感染、纠酸
	糖原累积症（Ia型）	女(1)	39.42	1.3	114.8	同上、抽搐	不详	血液净化
暂时性高氨血症		男(5) 女(6)	37.7 （31.71~38.93）	1 （0.02~3.00）	139.1 （110.15~190.50）	气促、反应差、抽搐、肌张力低、皮肤黄染	代酸、高乳酸	精氨酸静滴1例，其余针对原发病治疗
不明原因高氨血症		男(16) 女(10)	37.28 (35.64~38.89)	1 （0.02~3.00）	308.90 （148~495）	反应差、喂养困难19例，发绀16例，心脏骤停8例，意识障碍8例，抽搐7例，肌张力减低3例，发热1例，肌张力增高1例	代酸、高乳酸，血糖、凝血功能、电解质紊乱	精氨酸静滴6例，血液净化3例，腹膜透析1例，左卡尼丁口服1例，余对症支持治疗

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参考文献 20

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年份	总分娩量（n）	新生儿住院数[n(%)]	高氨血症[n(×1/万)]	男[n(%)]	女[n(%)]
2017	124 970	42 261(33.81)	8(0.64)	4(50.00)	4(50.00)
2018	130 350	40 688(31.21)	18(1.38)	12(66.67)	6(33.33)
2019	135 674	46 534(34.30)	13(0.96）	6(46.15)	7(53.85)
2020	112 830	40 421(35.82)	8(0.71）	6(75.00)	2(25.00)
2021	109 153	44 247(40.53)	14(1.28)	7(50.50)	7(50.50)
2022	95 444	39 568(41.46)	12(1.26)	9(75.00)	3(25.00)
合计	708 421	253 719(35.81)	73(1.03)	44(60.27)	29(39.73）

疾病名称	基因名称	基因位点	遗传方式	变异来源
高鸟氨酸血症-高氨血症 -高同型瓜氨酸尿症（HHHS）	SLC25A15	chr13:41381512(父亲) chr13:41379324(母亲)	常染色体隐性遗传	父亲为致病性变异母亲来源临床意义未明
肉碱棕榈酰转移酶或移位酶	SLC25A20	Intron2	同上	染色体3p21.31
瓜氨酸血症	ASS1基因	chr9:13336 4791	同上	不详
瓜氨酸血症	G6PC（NM_000151.3）	exon2	同上	父母均杂合携带
戊二酸血症2A型	ETFA（NM_000126.4)	chr15:76580278变异位点c.360G>T	同上	新发
肉碱棕榈酰转移酶Ⅱ型	CPT2(NM_000098.2)	chr1：53676593	同上	新发
肉碱-酰基肉碱移位酶缺乏症	SLC25A20	chr3：48921567	同上	纯合突变
暂时性高氨血症	未发现与临床表型高度相关的基因变异	无	无	无
暂时性高氨血症	复合型氧化磷酸化缺陷症22型 21羟化酶缺乏性肾上腺皮质增生症	无	无	无
心肌致密化不全	产前诊断示NONO基因变异	无	无	无
糖原累积症	GAA基因杂合变异	c.546+5G>T和c.2051C> T(p.P684L)	常染色体隐性遗传	分别来自父母
不明原因高氨血症	正常	无	无	无
不明原因高氨血症	RYR1	c.11578G>Achr19-39026698p.E3860K c.13588C>T1chr19-39058486p.P4530S	常染色体隐性/ 显性遗传	无