肝豆状核变性儿童临床表型与ATP7B基因突变谱变化研究*

doi:10.3969/j.issn.1672-5069.2024.02.015

Abstract

Abstract: Objective The aim of this study was to investigate the clinical phenotypes and blood ATP7B gene mutation profile changes in children with Wilson's disease (WD). Methods 62 children with WD including hepatic phenotype in 41 cases (clinical phenotypes in 11 cases and subclinical phenotypes in 30 cases) and neuropathy in 21 cases (clinical phenotypes in 6 cases and subclinical phenotypes in 15 cases) were admitted to our hospital between January 2020 and January 2023. The blood ATP7B gene mutation profile was obtained by gene sequencing and the results were compared in ATP7B mutation data bank. 24 hour-urine copper and serum ceruloplasmin levels were assayed by flame atomic absorption spectrometry. Results The onset age, incidence of corneal K-F ring, serum alanine aminotransferase (ALT) and 24-hour urinary copper levels in children with hepatic phenotype were(6.1±2.5)yr, 17.0%, (149.6±51.3)U/L and (157.0±25.7)μg, significantly different compared to in those with neuropathy(P<0.05); the onset age, incidence of corneal K-F ring, bile acid, serum ALT and 24-hour urinary copper levels in children with clinical phenotype of liver disease were(6.8±1.9)yr, 54.5%, (158.5±23.6)μmol/L, (279.6±17.5)U/L and (196.6±62.8)μg, significantly different compared to in those with subclinical phenotype of liver diseases (P<0.05), and the incidence of corneal K-F ring, bile acid, serum ALT and 24-hour urinary copper levels in children with clinical neuropathy were 100.0%, (26.8±5.8)μmol/L, (96.7±10.1)U/L and (376.5±48.9)μg, significantly different compared to in those with subclinical neuropathy (P<0.05); as for the ATP7B gene mutation spectrum, the c.2333G>T (Arg778Leu) was found in 41 alleles, with 33.1% of allele frequency, the c.2975G>T (Pro992Leu) was found in 10 alleles, with 8.1% of allele frequency, and the C.2621C>T (Ala874Val), c.1708-5t>g (Ala874Val) and c.994G >T (Glu332stop) were found with 4.8%, 3.2% and 3.2% allelic frequencies; 34 missense mutations, 15 insertion mutations, 8 shear mutations and 5 nonsense mutations were detected in our series and there were compound heterozygosity in 45 cases, heterozygosity mutation in 7 cases and homozygous mutation in 10 cases; there was no statistical differences as respect to the mutation frequencies of the top five pathogenic mutation genes, e.g., p.Arg778Le, p.Pro992Leu, p.Ala874Val, IvS4-5: t>g and p.Glu332stop between children with liver illness and neuropathy phenotypes (P>0.05). Conclusion The common clinical phenotype of children with WD is liver involvement, and the top five pathogenic gene variants are Arg778Leu, Pro992Leu, Ala874Val, Ala874Val and Glu332stop, which might be firstly sequenced for early diagnosis, but the gene screening probably hard to predict the clinical phenotypes.

Key words: Wilson&apos, s disease, Clinical phenotypes, ATP7B, Gene mutation profile, Children

Yan Panpan, Huang Xiaoxia, Zhu Feng, et al.. Clinical phenotypes and ATP7B gene mutation profile in children with Wilson's disease[J]. Journal of Practical Hepatology, 2024, 27(2): 218-221.

References

[1] Shribman S, Marjot T, Sharif A, et al. Investigation and management of Wilson's disease: a practical guide from the British Association for the Study of the Liver. Lancet Gastroenterol Hepatol, 2022, 7(6):560-575.
[2] Karimi A, Mohammadi S, Salehi MA, et al. Brain microstructural abnormalities in patients with Wilson's disease: A systematic review of diffusion tenor imaging studies. Brain Imaging Behav, 2022, 16(6):2809-2840.
[3] Jia S, Li X, Zhang W, et al. Laboratory and clinical evaluation of a microarray for the detection of ATP7B mutations in Wilson disease in China. J Clin Lab Anal, 2022, 36(11):e24735.
[4] Schilsky ML, Roberts EA, Bronstein JM, et al. A multidisciplinary approach to the diagnosisand management of Wilson disease: Executive summary of the 2022 Practice Guidance on Wilson disease from the American Association for the Study of Liver Diseases. Hepatology, 2023, 77(4):1428-1455.
[5] Zhang W, Yu Q, Peng H, et al. Clinical observation and risk assessment after splenectomy in hepatolenticular degeneration patients associated with hypersplenism. Front Surg, 2022, 9:972561.
[6] 纪雷, 张莹, 孔丽, 等. 83例肝豆状核变性患者的临床特征分析.临床肝胆病杂志, 2022, 38(8):1843-1846.
[7] 胡亚欣, 程卓, 丛硕, 等. 肝豆状核变性家系全基因组分析1例报告.临床肝胆病杂志, 2022, 38(7):1616-1619.
[8] Yin F, Nian M, Wang N, et al. Protective mechanism of gandou decoction in a copper-laden hepatolenticular degeneration model: In vitro pharmacology and cell metabolomics. Front Pharmacol, 2022, 13:848897.
[9] Mao H, Qin J, Kang T,et al. Wilson disease and IgA nephropathy: accidental or related? Int Urol Nephrol, 2022, 54(9):2441-2443.
[10] Wenbin Z, Yeqing H, Aiqun L, et al. A rare giant intracranial arachnoid cyst confused the diagnosis and treatment of Wilson disease. Transl Neurosci, 2022, 13(1):52-56.
[11] Bova C, de Vuono A, Ruvio M, et al. Visceral and mucosal leishmaniasis mimicking Wilson disease and oral neoplasia. IDCases, 2022, 28:e01466.
[12] 张天鹤, 毛志芹. 儿童肝豆状核变性的临床特点及基因分析(附70例报告). 中国实用儿科杂志, 2022, 37(2):135-139.
[13] Chanpong A, Dhawan A. Re-evaluation of King Wilson index in children with acutely decompensated hepatic Wilson disease. J Pediatr Gastroenterol Nutr, 2022, 74(4):510-515.
[14] Daniel-Robin T, Bénichou B, Leboucher C, et al. Epidemiology, treatment and burden of Wilson disease in France: A 10-year analysis of the national health insurance database. Clin Res Hepatol Gastroenterol, 2022, 46(10):101992.
[15] Im M, Song A, Kim J, et al. Wilson disease diagnosed incidentally by targeted gene panel sequencing in a Korean boy with severe obesity. Ann Pediatr Endocrinol Metab, 2022, 27(3):229-235.
[16] Aaraj S, Khan SA, Ali N, et al. Wilson disease in children. Chelation therapy or liver transplantation? A 10-year experience from Pakistan. Ann Transplant, 2021, 26:e932606.
[17] Kim P, Zhang C, Thoröe-Boveleth S, et al. Accurate measurement of copper overload in an experimental model of Wilson disease by laser ablation inductively coupled plasma mass spectrometry. Biomedicines, 2020, 8(9):1630-1633.
[18] Das MC, Sen Sarma M, Srivastava A, et al. Effect of chelation therapy in pediatric Wilson's disease: Liver and endoscopic outcome. J Hepatobiliary Pancreat Sci, 2021, 28(4):336-345.
[19] Koboldt DC, Hickey SE, Chaudhari BP, et al. Early-onset Wilson disease caused by ATP7B exon skipping associated with intronic variant. Cold Spring Harb Mol Case Stud, 2020, 6(3):a005306.
[20] Hashmi MA, Zubaida B, Asghar RM, et al. ATP7B mutation analysis: Wilson disease, A difficult to diagnose case. J Coll Physicians Surg Pak, 2020, 30(4):433-434.

Clinical phenotypes and ATP7B gene mutation profile in children with Wilson's disease

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