异戊酸血症患儿临床特征、基因型及随访分析

doi:10.12372/jcp.2024.23e1218

Abstract

Abstract:

Objective To explore the clinical features, gene variation and follow-up results of children with isovaleric acidemia (IVA), and to provide evidence for early recognition, diagnosis and treatment of IVA. Methods The clinical data of children diagnosed with IVA in the Department of Pediatric Endocrinology from April 2012 to October 2023 were retrospectively analyzed. Results Of the 34 children with IVA (22 boys and 12 girls), 15 had acute neonatal type, 3 had chronic intermittent type, and 16 had asymptomatic type confirmed by neonatal screening. Compared with asymptomatic group, blood isovalerylcarnitine (C5) level, C5/ acetylcarnitine (C2) ratio, C5/ propionylcarnitine (C3) ratio and urine isovalerylglycine level in the group with clinical symptoms (including acute neonatal type and chronic intermittent type) were significantly increased, with statistical significance (P<0.05). A total of 40 mutations were identified in 34 patients, most of which were missense mutations (30/40, 75.0%) and c.1208A>G (n=8) was the most frequent variant. There was no significant correlation between clinical manifestation and type of gene variation. Four patients, all of whom belonged to the acute neonatal type, died during follow-up. Thirty surviving children had considerably lower urinary isovalerylglycine levels at the most recent follow-up, with a statistically significant difference from before therapy (P<0.05). Conclusions Clinical manifestations of IVA lack specificity. Elevated C5, C5/C2 ratio and C5/C3 ratio in plasm and isovalerylglycine in urine are typical hallmarks of IVA. Newborn screening is pivotal for early diagnosis, treatment, and prognosis.

Key words: isovaleric academia, IVD gene, tandem mass spectrometry, newborn screening

SUN Yuning, LIANG Lili, DING Si, LIU Yuchao, CHEN Ting, GONG Zhuwen, QIU Wenjuan, ZHANG Huiwen, GU Xuefan, HAN Lianshu. Clinical characteristics, genotypes and follow-up analysis of children with isovaleric academia[J].Journal of Clinical Pediatrics, 2024, 42(3): 224-229.

Figures/Tables 3

References 27

[1]	Tanaka K, Budd MA, Efron ML, et al. Isovaleric acidemia: a new genetic defect of leucine metabolism[J]. Proc Natl Acad Sci U S A, 1966, 56(1): 236-242. doi: 10.1073/pnas.56.1.236
[2]	Ensenauer R, Fingerhut R, Maier EM, et al. Newborn screening for isovaleric acidemia using tandem mass spectrometry: data from 1.6 million newborns[J]. Clin Chem, 2011, 57(4): 623-626. doi: 10.1373/clinchem.2010.151134 pmid: 21335445
[3]	Schulze A, Lindner M, Kohlmüller D, et al. Expanded newborn screening for inborn errors of metabolism by electrospray ionization-tandem mass spectrometry: results, outcome, and implications[J]. Pediatrics, 2003, 111(6 Pt 1):1399-1406. doi: 10.1542/peds.111.6.1399 pmid: 12777559
[4]	Lin WD, Wang CH, Lee CC, et al. Genetic mutation profile of isovaleric acidemia patients in Taiwan[J]. Mol Genet Metab, 2007, 90(2): 134-139. doi: 10.1016/j.ymgme.2006.08.011
[5]	胡真真, 杨建滨, 胡凌微, 等. 浙江省新生儿异戊酸血症筛查及临床分析[J]. 浙江大学学报(医学版), 2020, 49(5): 556-564.
[6]	郑泉志, 傅清流, 彭维林, 等. 新生儿异戊酸血症串联质谱法与相关基因突变检测的价值研究[J]. 现代检验医学杂志, 2022, 37(5): 61-64.
[7]	顾学范, 韩连书, 余永国. 中国新生儿遗传代谢病筛查现状及展望[J]. 罕见病研究, 2022, 1(1): 13-19.
[8]	Dercksen M, Duran M, Ijlst L, et al. Clinical variability of isovaleric acidemia in a genetically homogeneous population[J]. J Inherit Metab Dis, 2012, 35(6): 1021-1029. doi: 10.1007/s10545-012-9457-2 pmid: 22350545
[9]	邱文娟, 顾学范, 叶军, 等. 异戊酸血症一例临床及异戊酰辅酶A脱氢酶基因突变研究[J]. 中华儿科杂志, 2008, 46(7): 526-530.
[10]	顾学范. 临床遗传代谢病[M]. 北京: 人民卫生出版社, 2015.
[11]	赵云飞, 祝莎莎, 黄新文. 异戊酸血症的研究进展[J]. 中华医学遗传学杂志, 2022, 39(1): 88-91.
[12]	韩连书, 高晓岚, 叶军, 等. 串联质谱分析干血滤纸片酰基肉碱方法的建立[J]. 中华检验医学杂志, 2005, 28(1): 245-248.
[13]	罗小平, 王慕逖, 魏虹, 等. 尿滤纸片法气相色谱-质谱分析技术在遗传性代谢病高危筛查诊断中的应用[J]. 中华儿科杂志, 2003, 41(4): 245-248.
[14]	唐雅楠, 叶贤涛, 顾学范, 等. Menke-Hennekam综合征表型及基因型分析[J]. 临床儿科杂志, 2023, 41(8): 613-617.
[15]	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
[16]	Ribeiro CA, Balestro F, Grando V, et al. Isovaleric acid reduces Na⁺, K⁺-ATPase activity in synaptic membranes from cerebral cortex of young rats[J]. Cell Mol Neurobiol, 2007, 27(4): 529-540. doi: 10.1007/s10571-007-9143-3 pmid: 17394058
[17]	Grünert SC, Wendel U, Lindner M, et al. Clinical and neurocognitive outcome in symptomatic isovaleric acidemia[J]. Orphanet J Rare Dis, 2012, 7: 9. doi: 10.1186/1750-1172-7-9 pmid: 22277694
[18]	Shibata N, Hasegawa Y, Yamada K, et al. Diversity in the incidence and spectrum of organic acidemias, fatty acid oxidation disorders, and amino acid disorders in Asian countries: selective screening vs. expanded newborn screening[J]. Mol Genet Metab Rep, 2018, 16: 5-10. doi: 10.1016/j.ymgmr.2018.05.003 pmid: 29946514
[19]	宋燕红, 张琪, 容翠环, 等. 串联质谱技术测定C5酰基肉碱水平在新生儿短链酰基辅酶A脱氢酶缺乏症筛查中的应用[J]. 广东医学院学报, 2021, 39(6): 729-731.
[20]	Couce ML, Aldamiz-Echevarría L, Bueno MA, et al. Genotype and phenotype characterization in a Spanish cohort with isovaleric acidemia[J]. J Hum Genet, 2017, 62(3): 355-360. doi: 10.1038/jhg.2016.144 pmid: 27904153
[21]	Chinen Y, Nakamura S, Tamashiro K, et al. Isovaleric acidemia: therapeutic response to supplementation with glycine, l-carnitine, or both in combination and a 10-year follow-up case study[J]. Mol Genet Metab Rep, 2017, 11: 2-5. doi: 10.1016/j.ymgmr.2017.03.002 pmid: 30547004
[22]	Li Y, Shen M, Jin Y, et al. Eight novel mutations detected from eight Chinese patients with isovaleric acidemia[J]. Clin Chim Acta, 2019, 498: 116-121. doi: S0009-8981(19)32014-5 pmid: 31442447
[23]	Lee YW, Lee DH, Vockley J, et al. Different spectrum of mutations of isovaleryl-CoA dehydrogenase (IVD) gene in Korean patients with isovaleric acidemia[J]. Mol Genet Metab, 2007, 92(1-2): 71-77. doi: 10.1016/j.ymgme.2007.05.003
[24]	Vatanavicharn N, Liammongkolkul S, Sakamoto O, et al. Phenotypic and mutation spectrums of Thai patients with isovaleric acidemia[J]. Pediatr Int, 2011, 53(6): 990-994. doi: 10.1111/j.1442-200X.2011.03488.x pmid: 22004070
[25]	李溪远, 华瑛, 丁圆, 等. 3例非典型异戊酸尿症患儿临床及基因型研究[J]. 临床儿科杂志, 2014, 32(12): 1107-1111.
[26]	Tan J, Chen D, Chang R, et al. Tandem mass spectrometry screening for inborn errors of metabolism in newborns and high-risk infants in Southern China: disease spectrum and genetic characteristics in a Chinese population[J]. Front Genet, 2021, 12: 631-688.
[27]	Wiley V, Webster D, Loeber G. Screening pathways through China, the Asia Pacific region, the world[J]. Int J Neonatal Screen, 2019, 5(3): 26. doi: 10.3390/ijns5030026 pmid: 33072985

组别	例数	血				尿
组别	例数	C5/μmol·L^-1	C0/μmol·L^-1	C5/C2	C5/C3	异戊酰甘氨酸/ mmol·mol肌酐^-1
有临床症状组	18	7.57(4.09~10.07)	29.86(13.36~40.60)	0.45(0.28~0.66)	8.05(4.87~17.14)	366.89(90.43~894.26)
无症状型组	16	1.41(0.75~5.47)	28.62(21.37~37.56)	0.15(0.05~0.43)	1.74(0.58~6.78)	18.14(2.23~152.30)
Z值		3.10	0.13	2.70	2.92	3.30
P		0.002	0.895	0.007	0.003	0.001

患儿	分型	测试时患儿年龄	动作能DQ（粗）	动作能DQ（细）	应物能DQ	言语能DQ	应人能DQ
例2	急性新生儿型	11月龄	80	74	74	70	44
例5	急性新生儿型	1岁1个月	56	54	25	25	87
例10	急性新生儿型	2岁2个月	93	97	91	77	98
例11	急性新生儿型	1岁6个月	94	96	72	46	86
例12	急性新生儿型	3岁7个月	80	72	56	52	81
例13	急性新生儿型	4岁2个月	126	111	80	76	89
例15	急性新生儿型	5岁2个月	98	81	62	67	83
例17	慢性间歇型	5岁6个月	42	44	82	77	75
例18	慢性间歇型	4岁3个月	110	102	73	72	65
例19	慢性间歇型	3岁3个月	113	106	71	74	73

时间	血				尿
时间	C5/μmol·L^-1	C0/μmol·L^-1	C5/C2	C5/C3	异戊酰甘氨酸/mmol·mol肌酐^-1
治疗前	4.20(1.25~9.23)	26.31(16.14~40.91)	0.27(0.10~0.57)	6.31 (1.69~13.03)	198.19(8.07~355.22)
最后1次随访时	5.41(1.12~9.21)	33.63(25.44~42.11)	0.30(0.07~0.49)	6.60(1.06~8.49)	16.17(1.57~169.14)
Z值	0.97	0.76	0.26	0.97	3.40
P	0.330	0.446	0.794	0.332	0.001

Clinical characteristics, genotypes and follow-up analysis of children with isovaleric academia

RichHTML

PDF (PC)

Like

Knowledge

Abstract

Cite this article

share this article

Figures/Tables 3

References 27

Related Articles 14

Metrics

Comments

Recommended 0

[1]	HUANG Cidan, XU Haizhu, WEN Yingmei, LIU Xiulian. Analysis of the results of newborn screening for fatty acid oxidative metabolic diseases in ethnic minority areas of Hainan Province [J]. Journal of Clinical Pediatrics, 2024, 42(2): 133-138.
[2]	ZHAO Zhengyan. The forty-three year development of newborn screening in china: starting with Chen Ruiguan [J]. Journal of Clinical Pediatrics, 2024, 42(2): 89-92.
[3]	HAN Lianshu. Detection technology and application selection of genetic metabolic diseases [J]. Journal of Clinical Pediatrics, 2023, 41(2): 81-85.
[4]	LIANG Lili. Genetic classification, diagnosis, and treatment of hyperphenylalaninemia [J]. Journal of Clinical Pediatrics, 2023, 41(2): 92-97.
[5]	LU Xiaoyan, CHEN Shaohong, CHEN Yingying, ZHOU Wenjun, ZHOU Chan, SONG Yan, LI Luquan, TANG Wenyan. Related factors affecting delayed thyroid stimulating hormone elevation in preterm infants with gestational age <34 weeks [J]. Journal of Clinical Pediatrics, 2023, 41(10): 675-679.
[6]	HU Haili, LI Weidong, WANG Yan, SONG Wangsheng, MA Qingqing. Neonatal screening and gene variation analysis of primary carnitine deficiency in Hefei City [J]. Journal of Clinical Pediatrics, 2023, 41(10): 680-684.
[7]	ZHANG Wanqiao, YAN Lei, ZHU Lina, MA Xiuwei. Metabolic and genetic analysis of abnormal 3-hydroxyisovalerylcarnitine in children from northern China [J]. Journal of Clinical Pediatrics, 2023, 41(10): 692-696.
[8]	WANG Yanyun, SUN Yun, JIANG Tao. 10q22.3-q23.2 deletion syndrome combined with hypermethioninemia: a case report and literature review [J]. Journal of Clinical Pediatrics, 2021, 39(9): 660-.
[9]	WANG Yanyun, SUN Yun, CHENG Wei, et al. Clinical characteristics of hyperprolinemia [J]. Journal of Clinical Pediatrics, 2020, 38(1): 40-.
[10]	CUI Qingyang, SUN Weiwei, LU Jun. Clinical feature and genetic variation analysis of glutaric aciduria type I in a child [J]. Journal of Clinical Pediatrics, 2019, 37(7): 545-.
[11]	ZHANG Zhilei, SUN Yun, Wang Yanyun, et al. Clinical analysis of methionine adenosyltransferase Ⅰ / Ⅲ deficiency in 5 confirmed cases in neonatal screening [J]. Journal of Clinical Pediatrics, 2019, 37(12): 889-.
[12]	ZHAN Xia, HAN Lianshu, YE Jun, QIU Wenjuan, GU Xuefan . Preparation and evaluation of dried blood spots control materials for steroids [J]. , 2017, 35(12): 941-.
[13]	HU Yuhui, CUI Dong, LIU Lin, CHEN Shuli. Mitochondrial acetoacetyl-CoA thiolase deficiency: report of three cases in a family and literature review [J]. , 2016, 34(4): 282-.
[14]	YAO Yingzi, JIANG Ling, ZHANG Cuimei, HUANG Xiang, LIANG Rui, HIANG Lianhong, WAN Z hidan, YAN Xueqin . The pilot study of combined detection of thyroid stimulating hormone and free thyroxine in screening for congenital hypothyroidism in neonates [J]. , 2014, 32(7): 649-.