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Alanine Aminotransferase as the First Test Parameter for Wilson’s Disease

  • Hisao Hayashi*,1,
  • Kazumasa Watanabe2,
  • Ayano Inui3,
  • Ayako Kato1,
  • Yasuaki Tatsumi1,
  • Akihiko Okumura2,
  • Tomoo Fujisawa3 and
  • Koichi Kato1
Journal of Clinical and Translational Hepatology   2019;7(4):293-296

doi: 10.14218/JCTH.2019.00042

Received:

Revised:

Accepted:

Published online:

 Author information

Citation: Hayashi H, Watanabe K, Inui A, Kato A, Tatsumi Y, Okumura A, et al. Alanine Aminotransferase as the First Test Parameter for Wilson’s Disease. J Clin Transl Hepatol. 2019;7(4):293-296. doi: 10.14218/JCTH.2019.00042.

Abstract

Background and Aims: The liver is the first organ affected by toxic copper in the classical and severe hepatic forms of Wilson’s disease (WD). Because their associated chronic liver damage is mostly asymptomatic, an intervention using a special test including serum alanine aminotransferase (ALT) activity is needed for detecting WD.

Methods: Using the modified international criteria for the diagnosis of WD, 45 patients were selected from the collective databases of our institutions, and 7 infants were reviewed from the literature. Two patients had the severe hepatic form, with normoceruloplasminemia and no mutations in ATP7B. The rapid ALT change during hemolytic anemia was adjusted for a baseline. The diagnostic potential of the ALT test was assessed from the age-dependent natural course of the liver damage of WD.

Results: The natural course had three stages. ALTs were still low in some infants younger than 4 years-old. They were high in all children between the ages of 4 and 8 years-old; then, they reduced to low levels in some patients over 9 years of age. The high ALT stage represents chronic active hepatitis, and the subsequent low ALT stage is due to silent cirrhosis. The hepatic copper content is a reliable but invasive test, while urinary copper secretion is an alternative, non-invasive test for copper toxicosis of WD. The serum ceruloplasmin and ATP7B analyses are subtype tests of WD. The response to anti-copper regimens is the final test result.

Conclusions: ALT could be the first parameter to test to detect WD in children between the ages of 4 and 8 years.

Keywords

Alanine aminotransferase, ATP7B, Ceruloplasmin, Chronic active hepatitis, Wilson’s disease

Introduction

New terminology proposed by Tatsumi et al.1 may facilitate a better understanding of the primary copper toxicosis of Wilson’s disease (WD) and a simple approach to diagnose asymptomatic liver damage in the early stage of WD. The classical form is a primary copper-induced liver disease, which may be complicated by lenticular degeneration at a later stage, and which was initially described by SAK Wilson in 1912.1–3 In addition to increased hepatic copper of 250 μg/g dry liver or more, two mutant alleles in the ATP7B gene and reduced serum levels of ceruloplasmin (CP) are found in typical cases.1,3 Other subtype tests include detection of Kayser Fleischer rings, neuropsychiatric signs, and Coombs-negative hemolytic anemia.1,3 The severe hepatic form is another copper-induced liver disease, the former name of which was idiopathic copper toxicosis, proposed by Scheinberg and Sternlieb in 1994.1,4–6 There are currently no tests for the severe hepatic form, other than detection of increased hepatic copper and urinary copper secretion,1,6 and the new subtype tests proposed by Tatsumi et al.1 are combined results of normal CP levels and no mutations in ATP7B.

Another recommendation that Tatsumi et al.1 propose is a treatment for the copper toxicosis of WD. Every patient with WD should receive a short-term treatment trial involving anti-copper regimens, followed by life-long maintenance treatment. For the former, a poor response to anti-copper regimens indicates non-WD. Some patients with WD, especially the severe hepatic form, suddenly present with hepatic failure and require a liver transplantation without the liver biopsy essential for diagnosing WD. In such cases, the postoperative diagnosis of WD should be confirmed by the increased copper content of the removed liver.

It is now an urgent task to establish liver tests for patients with asymptomatic liver damage of WD. Aspartate aminotransferase (AST) and alanine aminotransferase (ALT) are favorable liver tests, but they are hampered by the following problems in WD patients: (1) rapid falls of AST and ALT during Coombs-negative hemolytic anemia;7 (2) natural courses of the first increasing and second decreasing stages of AST and ALT;8 and (3) AST having an erythrocyte fraction in WD, where it is significantly affected by copper-induced hemolysis.7,9 When the serum levels of AST and ALT are introduced as tests for the primary liver damage of WD, all problems should be overcome to minimize misdiagnosis.

In this study, we evaluated the potential of serum levels of ALT as representative of age-dependent liver disease activity of WD and determined the optimal age for the ALT test in WD patients.

Methods

Patients

International proposals were used for the diagnosis of WD, with minor modifications.3 The original scoring system for the diagnosis consists of Kayser-Fleischer rings (2 points), neuropsychiatric symptoms (2), Coombs-negative hemolytic anemia (1), urinary copper (max. increase: 2), hepatic copper quantitative (max. increase: 2), serum CP level (max. decrease: 2),10 and ATP7B mutation (2 alleles: 4, one allele: 1). Diagnostic WD is assigned with a score of 4 or more points. Probable WD is assigned with score of 2–3 points. Unlikely WD is assigned with score of 0–1 points. In the patients saved by liver transplantation, the copper content of the removed liver should receive a maximum of 2 points (>250 μg/g dry liver weight). In patients with 2–3 points (probable WD), the diagnosis was retrospectively confirmed by giving an additional 2 points for a good response to anti-copper regimens. A removed liver with copper less than 250 μg/g dry liver and a poor response to anti-copper regimens were set as exclusion criteria. WD cases complicated with either chronic cholestasis or other chronic liver disease, including chronic viral hepatitis, nonalcoholic steatohepatitis, etc., were also excluded from the study.

A total of 52 patients with primary copper toxicosis of WD were enrolled in the study. Forty-five Japanese patients were selected from the databases of three institutes (Aichi Gakuin University School of Pharmacy, Kainan Hospital, and Saiseikai Yokohama Toub Hospital), and 7 infant patients were cited based on a literature review of PubMed to identify relevant papers written in English since 1993.11–16 Clinical data of two Japanese patients were analyzed twice because they were followed for years without anti-copper regimens.

Based on ATP7B analysis and serum levels of CP, the primary copper toxicosis of WD in the studied patients was subtyped into two forms — classical and severe hepatic WD (Table 1).1 Forty-five patients had typical features of the classical form, with two mutant alleles in ATP7B and low levels of serum CP (<20 mg/dL); two other patients had the severe hepatic form, with no mutation in ATP7B and normal levels of serum CP. Five patients had atypical classical forms, with one mutant allele of ATP7B.

Table 1.

Fifty-two patients with WD and their subtypes using ATP7B analysis and serum CP levels

Group of patientsATP7BSerum CP (>20 mg/dL)Patient numberMajor subtype
Literature, n = 7Two mutant allelesLow7Classical
Normal0Classical
Patient databases, n = 45Two mutant allelesLow38Classical
Normal1Classical
One mutant alleleLow4Classical
Normal0?
No mutant alleleLow0?
Normal2Severe hepatic

Methods

The study protocol was approved by the ethics committees of 3 institutes (Aichi Gakuin University School of Pharmacy, Kainan Hospital, and Saiseikai Yokohama Toub Hospital). Serum levels of ALT were determined by one point at entry in all patients with WD, except for those with Coombs-negative hemolytic anemia and complicated acute diseases. The baseline ALT levels of hemolysis patients were obtained at the stage of pre-hemolytic anemia or recovery from anemia.7 In the patients whose WD was found after acute diseases, such as fever episodes and gastrointestinal problems, the baseline ALT was obtained at the recovery stage. Using the serum levels of ALT and onset ages of 52 patients aged between 0.7 and 47 years, a virtual image was made for the natural course of WD. The diagnostic potential of the age-dependent ALT levels was assessed for the primary liver damage of WD.

Results

Virtual images of the natural course of WD using serum ALT levels representative of primary liver disease activities and entry ages of patients are presented in Fig. 1. There are three ALT stages associated with the onset ages of patients. In the first stage, some infants younger than 4 years-old showed low ALT levels. In the second stage, all of the 10 children aged between 4 and 8 years showed high ALT levels (>150 IU/L). In the third stage, patients over the age of 9 years showed a wide range of ALT levels; fifteen of thirty-five patients showed pathologically high ALT levels, while 20 patients had levels that were near-normal. Especially, all seven patients aged 35 years or older showed ALT levels below 50 IU/L.

Natural course of WD represented by serum ALT levels adjusted for the baseline liver disease and onset ages of patients.
Fig. 1.  Natural course of WD represented by serum ALT levels adjusted for the baseline liver disease and onset ages of patients.

Rapid ALT changes during Coombs-negative hemolytic anemia of WD were adjusted to a baseline at either the prehemolytic anemia or postrecovery stage. In the patients whose WD was found after acute diseases, such as fever episodes and gastrointestinal problems, the baseline ALT was obtained at the recovery stage. Three ALT stages of WD associated with the ages of patients are shown. The first stage includes 7 infants with development of WD before 4 years old; ALT levels are low in 4 and high in 3 infants. The second stage consists of 10 patients aged between 4 and 8 years whose ALT levels are all high, over 150 IU/L. The third stage includes 35 patients with a wide range of ALT levels; fifteen patients have pathologically high ALT levels, while 20 patients have near-normal levels. Especially, all 7 patients aged 35 years or older show ALT levels below 50 IU/L. The ALT test is reliable for detecting WD at the high ALT stage of children aged between 4 and 8 years. ALT, alanine aminotransferase; WD, Wilson’s disease. ●: Classical form of Japanese patients; ▴: Severe hepatic form (non-ATP7B) of Japanese patients; ○: Infants with the ATP7B classical form cited from the international literature.11–16

Discussion

Our observations strongly suggest that a standard liver test — ALT — has the potential to detect most WD patients between the ages of 4 and 8 years-old. Serum ALT levels higher than 150 IU/L are representative of active chronic hepatitis of WD.17,18 Underlying mechanisms of the low ALT levels are different in the first and third stages. The former means that there is no active liver damage in some patients as yet, due to a small amount of toxic copper in the liver,8 while the latter involves silent cirrhosis in some patients. It is well known that, in chronic viral hepatitis, histological progression from chronic hepatitis to cirrhosis is associated with declining inflammation in the liver. Such transformation is of special importance in WD. A large amount of copper is mostly stored in hepatocyte lysosomes of cirrhosis as detoxified cuprothioneins.19,20 Age-dependent copper accumulation in the central nervous system is also associated with silent cirrhosis formation in classical WD.8 As a result, ALT tests partially lose the potential to detect copper-induced liver diseases in patients over 9 years-old.

Based on the natural disease course presented in this study, we can postulate that most patients aged over 9 years had asymptomatically experienced the high ALT stage when between the ages of 4 and 8 years-old. Therefore, children aged between 4 and 8 years may be suitable candidates for special intervention to detect asymptomatic but biochemically active liver damage of WD, as summarized in Table 2.

Table 2.

Recommended diagnostic approach to the primary liver disorders of WD

WD
Classical FormSevere Hepatic Form
1Liver testSerum ALT test: > 150 IU/L in children aged 4 – 8 yrs
2Copper testsHepatic copper more than 250 μg/g dry liver
Increased urinary copper secretion (basic and post-penicillamine)
3Subtype testsHypoceruloplasminemiaNormoceruloplasminemia and no ATP7B mutation
Mutations in ATP7B
4Anti-copper testsGood responses on ALT reduction

Increased hepatic copper and urinary copper secretion are reliable tests for the copper toxicosis of WD favored by the international proposal.3 Hypoceruloplasminemia1,10 and ATP7B mutations1,3 strongly support the classical form. In contrast, their respective absence does not exclude WD; the negative combination of the two major subtyping tests for the classical form may be transient subtype tests for the severe hepatic form that has no definitive subtype tests, including gene analysis.1,6

A final diagnosis of WD should be confirmed in all children with WD, by anti-copper regimens. A recent study on young patients under 10 years of age revealed that zinc monotherapy reduced serum ALT levels ranging from 243 ± 151 to 70 ± 29 IU/L in 1 month.23 It is also important that copper-overload conditions secondary to chronic cholestasis24 or chronic liver diseases other than WD25,26 could be differentiated by the short-term treatment test.

Because neuropsychiatric symptoms of classical WD appear at a late cirrhotic stage associated with low ALT levels,8 an intentional ALT test for children at the high ALT stage is prophylactic for neuropsychiatric complications. A smaller number of children with WD may have been affected by Coombs-negative hemolytic anemia before such a scheduled ALT test.8 A similar episode in a 7-year-old girl among the 10 patients in the high ALT stage was self-limiting, and she recovered from anemia without any sequelae. ALT intervention specialized to detect asymptomatic WD should be confirmed in a large number of patients.

Conclusions

There are two subtypes of classical and severe hepatic forms in the primary copper toxicosis of WD. A standard liver test of ALT is highly recommended for children between the ages of 4 and 8 years-old to detect asymptomatic WD. The selection criterion is a serum ALT level over 150 IU/L. Increased hepatic copper is an etiological test. Serum CP level and ATP7B analyses are subtype tests. A marked reduction of ALT with anti-copper regimens is diagnostic for WD.

Abbreviations

ALT: 

alanine aminotransferase

AST: 

aspartate aminotransferase

CP: 

ceruloplasmin

WD: 

Wilson’s disease

Declarations

Conflict of interest

The authors have no conflict of interests related to this publication.

Authors’ contributions

Conception of study objective and design (HH, AI, TF), collection of patient data (KW, AO, KK), gene analysis (AK, YT).

References

  1. Tatsumi Y, Kato A, Kato K, Hayashi H. The interactions between iron and copper in genetic iron overload syndromes and primary copper toxicoses in Japan. Hepatol Res 2018;48:679-691 View Article PubMed/NCBI
  2. Compston A. Progressive lenticular degeneration: a familial nervous disease associated with cirrhosis of the liver, by S. A. Kinnier Wilson, (From the National Hospital, and the Laboratory of the National Hospital, Queen Square, London) Brain 1912: 34; 295–509. Brain 2009;132:1997-2001 View Article PubMed/NCBI
  3. Ferenci P, Caca K, Loudianos G, Mieli-Vergani G, Tanner S, Sternlieb I. Diagnosis and phenotypic classification of Wilson disease. Liver Int 2003;23:139-142 View Article PubMed/NCBI
  4. Scheinberg IH, Sternlieb I. Is non-Indian childhood cirrhosis caused by excess dietary copper?. Lancet 1994;344:1002-1004 View Article PubMed/NCBI
  5. Müller T, Müller W, Feichtinger H. Idiopathic copper toxicosis. Am J Clin Nutr 1998;67:1082S-1086S View Article PubMed/NCBI
  6. Fujisawa T, Inui A, Kawakami M. Pediatric clinical hepatology. Tokyo: Tokyo Igakusha; 2017 View Article PubMed/NCBI
  7. Hayashi H, Tatsumi Y, Yahata S, Hayashi H, Momose K, Isaji R. Acute hepatic phenotype of Wilson disease: Clinical features of acute episodes and chronic lesions remaining in survivors. J Clin Transl Hepatol 2015;3:239-245 View Article PubMed/NCBI
  8. Katano Y, Hayashi K, Hattori A, Tatsumi Y, Ueyama J, Wakusawa S. Biochemical staging of the chronic hepatic lesions of Wilson disease. Nagoya J Med Sci 2014;76:139-148 View Article PubMed/NCBI
  9. Lippi G, Salvagno GL, Montagnana M, Brocco G, Guidi GC. Influence of hemolysis on routine clinical chemistry testing. Clin Chem Lab Med 2006;44:311-316 View Article PubMed/NCBI
  10. Scheinberg IH, Gitlin D. Deficiency of ceruloplasmin in patients with hepatolenticular degeneration (Wilson’s disease). Science 1952;116:484-485 View Article PubMed/NCBI
  11. Shimizu N, Nakazono H, Watanabe A, Yamaguci Y, Hemmi H, Aoki T. Molecular diagnosis of Wilson’s disease. Lancet 1997;349:1811-1812 View Article PubMed/NCBI
  12. Abuduxikuer K, Li LT, Qiu YL, Wang NL, Wang JS. Wilson disease with hepatic presentation in an eight-month-old boy. World J Gastroenterol 2015;21:8981-8984 View Article PubMed/NCBI
  13. Kim JW, Kim JH, Seo JK, Ko JS, Chang JY, Yang HR. Genetically confirmed Wilson disease in a 9-month old boy with elevations of aminotransferases. World J Hepatol 2013;5:156-159 View Article PubMed/NCBI
  14. Usta J, Wehbeh A, Rida K, El-Rifai O, Estiphan TA, Majarian T. Phenotype-genotype correlation in Wilson disease in a large Lebanese family: association of c.2299insC with hepatic and of p. Ala1003Thr with neurologic phenotype. PLoS One 2014;9:e109727 View Article PubMed/NCBI
  15. Ohura T, Abukawa D, Shiraishi H, Yamaguchi A, Arashima S, Hiyamuta S. Pilot study of screening for Wilson disease using dried blood spots obtained from children seen at outpatient clinics. J Inherit Metab Dis 1999;22:74-80 View Article PubMed/NCBI
  16. Yuan ZF, Wu W, Yu YL, Shen J, Mao SS, Gao F. Novel mutations of the ATP7B gene in Han Chinese families with pre-symptomatic Wilson’s disease. World J Pediatr 2015;11:255-260 View Article PubMed/NCBI
  17. Sternlieb I, Scheinberg IH. Chronic hepatitis as a first manifestation of Wilson’s disease. Ann Intern Med 1972;76:59-64 View Article PubMed/NCBI
  18. Stromeyer FW, Ishak KG. Histology of the liver in Wilson’s disease: a study of 34 cases. Am J Clin Pathol 1980;73:12-24 View Article PubMed/NCBI
  19. Goldfischer S, Sternlieb I. Changes in the distribution of hepatic copper in relation to the progression of Wilson’s disease (hepatolenticular degeneration). Am J Pathol 1968;53:883-901 View Article PubMed/NCBI
  20. Hanaichi T, Kidokoro R, Hayashi H, Sakamoto N. Electron probe X-ray analysis on human hepatocellular lysosomes with copper deposits: copper binding to a thiol-protein in lysosomes. Lab Invest 1984;51:592-597 View Article PubMed/NCBI
  21. Walshe JM. Serum ‘free’ copper in Wilson disease. QJM 2012;105:419-423 View Article PubMed/NCBI
  22. Squitti R, Ghidoni R, Simonelli I, Ivanova ID, Colabufo NA, Zuin M. Copper dyshomeostasis in Wilson disease and Alzheimer’s disease as shown by serum and urine copper indicators. J Trace Elem Med Biol 2018;45:181-188 View Article PubMed/NCBI
  23. Eda K, Mizuochi T, Iwama I, Inui A, Etani Y, Araki M. Zinc monotherapy for young children with presymptomatic Wilson disease: A multicenter study in Japan. J Gastroenterol Hepatol 2018;33:264-269 View Article PubMed/NCBI
  24. Ramraj R, Finegold MJ, Karpen SJ. Progressive familial intrahepatic cholestasis type 3: overlapping presentation with Wilson disease. Clin Pediatr (Phila) 2012;51:689-691 View Article PubMed/NCBI
  25. Piekuse L, Kreile M, Zarina A, Steinberga Z, Sondore V, Keiss J. Association between inherited monogenic liver disorders and chronic hepatitis C. World J Hepatol 2014;6:92-97 View Article PubMed/NCBI
  26. Tahir A, Malik FR, Ahmad I, Akhtar P. Aetiological factors of chronic liver disease in children. J Ayub Med Coll Abbottabad 2011;23:12-14 View Article PubMed/NCBI