Value of Serum Zinc in Diagnosing and Assessing Severity of Liver Disease in Children With Wilson Disease

Wilson disease is a rare but important disorder of copper metabolism, with a failure to excrete copper appropriately into bile. It is a multisystem condition with presentations across all branches of medicine. Diagnosis can be difficult and requires a high index of suspicion. It should be considered in unexplained liver disease particularly where neuropsychiatric features are also present. Treatments are available for all stages of disease. A particularly important presentation not to overlook is acute liver failure which carries a high mortality risk and may require urgent liver transplantation. Here, we provide an overview of this complex condition.

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Exome sequencing of an adolescent with nonalcoholic fatty liver disease identifies a clinically actionable case of Wilson disease

Molecular Case Studies ◽

10.1101/mcs.a003087 ◽

2018 ◽

Vol 4 (5) ◽

pp. a003087 ◽

Cited By ~ 1

Author(s):

Julia Wattacheril ◽

Patrick R. Shea ◽

Saeed Mohammad ◽

Cynthia Behling ◽

Vimla Aggarwal ◽

...

Keyword(s):

Liver Disease ◽

Fatty Liver ◽

Nonalcoholic Fatty Liver Disease ◽

Exome Sequencing ◽

Wilson Disease ◽

Fatty Liver Disease ◽

Nonalcoholic Fatty Liver

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P.03.11 LONG TERM ZINC THERAPY IN WILSON DISEASE CHILDREN WITH MILD LIVER DISEASE

Digestive and Liver Disease ◽

10.1016/s1590-8658(12)60278-3 ◽

2012 ◽

Vol 44 ◽

pp. S102

Author(s):

G. Ranucci ◽

F. Di Dato ◽

G. Puoti ◽

D. Liccardo ◽

M. Tufano ◽

...

Keyword(s):

Liver Disease ◽

Wilson Disease

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WILSON DISEASE

The Professional Medical Journal ◽

10.29309/tpmj/2005.12.04.5098 ◽

2005 ◽

Vol 12 (04) ◽

pp. 446-450

Author(s):

HINA AYESHA ◽

AAMIR ALI CHOUDHRY ◽

MUHAMMED ASGHAR BUTT

Keyword(s):

Liver Disease ◽

Wilson Disease ◽

Neurological Disease ◽

Molecular Genetic ◽

Genotypic Differences ◽

Novel Mutations ◽

The West ◽

Medical College ◽

Genotype 2 ◽

Frequent Mutations

Objectives: 1). To study the genotypic differences, if any, betweenPakistani children suffering from Wilson’s disease from those in the west and to correlate phenotype with genotype. 2).To find out the most frequent mutations present in our patients and screen out asymptomatic siblings of the index cases.Setting: Department of Pediatrics, Allied Hospital, Punjab Medical College, Faisalabad. Duration: May 1997 to June2005. Materials and methods: 41 patients ranging from 5-18 years were diagnosed based on clinical and laboratorydata. 13 patients and 6 asymptomatic siblings along with their parents were subjected to mutation analysis. at Universityof Vienna, Austria. Results: None of the patients had His1069Gln, the commonest European mutation. R969Q andI1102T detected in our patients have previously been described. Four novel mutations were found. Asymptomaticsiblings screened were either heterozygote or normal. R969Q appears to be associated with sub-acute liver diseasewith hepatosplenomegaly. I1102T was seen in children with chronic liver disease and L1071W, C1079Y and E583R-fs(insA) with early onset of neurological disease. Conclusion: Our Patients are phenotypicaly as well as genotypicalydifferent. Different genotype could be responsible for the phenotype. Further studies are needed with a larger samplesize so that molecular genetic tests be devised for early diagnosis and family screening.

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Evaluation of Serum Zinc Status and Serum Alkaline Phosphatase Activity in Alcoholic Liver Disease Patients - A Hospital Based Study from Chennai, Tamil Nadu

Journal of Evidence Based Medicine and Healthcare ◽

10.18410/jebmh/2021/393 ◽

2021 ◽

Vol 8 (24) ◽

pp. 2100-2105

Author(s):

Uma T ◽

Nirmaladevi P ◽

Shanthi R ◽

Mahalakshmi R

Keyword(s):

Alkaline Phosphatase ◽

Liver Disease ◽

Phosphatase Activity ◽

Alcoholic Liver Disease ◽

Alkaline Phosphatase Activity ◽

Serum Zinc ◽

Meld Score ◽

Gamma Glutamyl Transferase ◽

Zinc Status ◽

Glutamyl Transferase

BACKGROUND Alcoholism remains to be the major cause of morbidity and mortality throughout the world. Consuming alcohol is the potent etiological factor for the development of alcoholic liver diseases (ALD), ranging from fatty liver to hepatocellular carcinoma with varying rates of development in both genders depending on the quality, quantity, and duration of the drink. Zinc deficiency has been documented with the progression of alcoholic liver disease. It is also a well-known fact that zinc is a co-factor for enzyme alkaline phosphatase. This study aims to assess the zinc status and alkaline phosphatase activity in patients with various stages of alcoholic liver disease, correlate zinc with alkaline phosphatase activity, albumin, gamma glutamyl transferase activity, MELD score and duration of alcohol intake and analysing the need for evaluating zinc in these patients. METHODS This comparative observational study involves group I healthy controls and group II patients diagnosed to have ethanol related decompensated liver disease with or without portal hypertension for more than three years from the Department of Medical Gastroenterology, Government Medical College Hospital. 5 ml of venous blood in fasting state was collected from both groups and assayed for serum zinc, and serum alkaline phosphatase activity. The data was statistically analysed. RESULTS The study results demonstrate that higher percentage of patients with alcoholic liver disease have low serum zinc levels than healthy controls. Zinc when compared with variables like serum albumin, duration of alcohol intake, MELD score, serum gamma glutamyl transferase and alkaline phosphatase in the case and control groups were found to be statistically significant. CONCLUSIONS There is decrease in serum zinc level and increased alkaline phosphatase activity in patients with alcoholic liver disease. The statistically significant data is a strong rationale for evaluating the zinc status and thereby supplementing zinc to patients with alcoholic liver disease. KEYWORDS Alcoholic Liver Disease, Zinc, Alkaline Phosphatase, MELD Score

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Zinc Monotherapy as an Alternative Treatment Option for Decompensated Liver Disease due to Wilson Disease?

Case Reports in Hepatology ◽

10.1155/2020/1275940 ◽

2020 ◽

Vol 2020 ◽

pp. 1-5 ◽

Cited By ~ 1

Author(s):

Hansa Haftu ◽

Mohammed Mustefa ◽

Teklu Gebrehiwot

Keyword(s):

Liver Disease ◽

Treatment Option ◽

Alternative Treatment ◽

Wilson Disease ◽

Copper Metabolism ◽

Variable Degree ◽

Decompensated Liver Disease ◽

Serum Ceruloplasmin ◽

Asymptomatic Patients ◽

Alternative Treatment Option

Background. Wilson disease is a rare metabolic disorder involving copper metabolism, and patients may present with a variable degree of hepatic, neurologic, and psychiatric manifestations. In the case of hepatic presentation, treatment is usually initiated with potentially toxic copper chelators (D-penicillamine or Trenton). Although zinc is of low toxicity and low cost for treatment of Wilson disease, it has been limited to the adjunctive as a single maintenance drug or for asymptomatic patients. The use of zinc monotherapy in patients suffering from a severe liver disease was not well studied. In our case report, we describe a pediatric patient who presented with liver failure and the use of zinc monotherapy in patients with severe hepatic manifestations. Case presentation. A 15-year-old male patient from Ethiopia presented with generalized body swelling (edema and ascites) with yellowish discoloration of his eyes and easy fatigability. He had hyperbilirubinemia, coagulopathy, hypoalbuminemia, and deranged liver enzymes. He had a Keyser–Fleischer ring visible with the naked eye, which was confirmed by slit-lamp examination. He had very low serum ceruloplasmin (<8 mg/L) and high 24-hour urine copper (150 mcg/dl). In accordance with the scoring system proposed by the 8th International Meeting on Wilson Disease and Menkes Disease, a diagnosis of Wilson disease was made. Zinc monotherapy with low copper diet was initiated for decompensated liver disease due to Wilson disease because of the inaccessibility of chelators (D-penicillamine or Trientine). After months of treatment with zinc, the patient experienced normalization of hepatic synthetic function and resolution of hypoalbuminemia and coagulopathy. The patient had also clinically stabilized (ascites, lower extremity swelling, edema, and jaundice were improved. Currently, the patient is on follow-up almost for the last four years in the gastrointestinal clinic. Conclusion. Our case shows that zinc has the potential for treatment in improving liver function. Though zinc has its own side effects, it is important and maybe an alternative treatment option in those with limited resources (not able to access chelators). This example hopefully will encourage future investigations and researches on zinc monotherapy for treating symptomatic decompensated hepatic Wilson disease.

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