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Literature DB >> 3799705

Treatment of Wilson's disease with zinc. II. Validation of oral 64copper with copper balance.

G M Hill, G J Brewer, J E Juni, A S Prasad, R D Dick.

Abstract

The efficacy of zinc as a therapeutic agent to control copper balance in Wilson's disease patients has been previously documented with balance studies. In an attempt to develop a simpler and faster tool for evaluating the adequacy of zinc therapy, a technique that measures the uptake into blood of a small oral dose of 64copper was studied in conjunction with copper balance. The mean peak 64copper uptake into blood of nine Wilson's disease patients on D-penicillamine, trien, or no medication was 6.04 +/- 2.74%, comparable with normal controls. Seven patients on zinc therapy had a markedly and significantly reduced mean uptake of 0.79 +/- 1.05% after treatment. The data demonstrate that the prevention of copper uptake into blood in Wilson's disease patients by zinc therapy can be evaluated by 64copper uptake and that peak uptakes of less than 1% occur in patients with neutral or negative copper balance.

Entities: Chemical Disease Species

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Year: 1986 PMID： 3799705 DOI： 10.1097/00000441-198612000-00002

Source DB: PubMed Journal: Am J Med Sci ISSN： 0002-9629 Impact factor: 2.378

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Cited

24 in total

1. Pharmacokinetic study of orally administered zinc in humans: evidence for an enteral recirculation.

Authors: J Nève; M Hanocq; A Peretz; F Abi Khalil; F Pelen; J P Famaey; J Fontaine
Journal: Eur J Drug Metab Pharmacokinet Date: 1991 Oct-Dec Impact factor: 2.441

Review 2. Current anti-copper therapies in management of Wilson disease.

Authors: Isabelle Mohr; Karl Heinz Weiss
Journal: Ann Transl Med Date: 2019-04

3. Copper-Induced Upregulation of MicroRNAs Directs the Suppression of Endothelial LRP1 in Alzheimer's Disease Model.

Authors: Heng-Wei Hsu; Carlos J Rodriguez-Ortiz; Siok Lam Lim; Joannee Zumkehr; Jason G Kilian; Janielle Vidal; Masashi Kitazawa
Journal: Toxicol Sci Date: 2019-07-01 Impact factor: 4.849

4. The Function of ATPase Copper Transporter ATP7B in Intestine.

Authors: Hannah Pierson; Abigael Muchenditsi; Byung-Eun Kim; Martina Ralle; Nicholas Zachos; Dominik Huster; Svetlana Lutsenko
Journal: Gastroenterology Date: 2017-09-25 Impact factor: 22.682

5. Low levels of copper disrupt brain amyloid-β homeostasis by altering its production and clearance.

Authors: Itender Singh; Abhay P Sagare; Mireia Coma; David Perlmutter; Robert Gelein; Robert D Bell; Richard J Deane; Elaine Zhong; Margaret Parisi; Joseph Ciszewski; R Tristan Kasper; Rashid Deane
Journal: Proc Natl Acad Sci U S A Date: 2013-08-19 Impact factor: 11.205

Treatment of Wilson's disease with zinc. II. Validation of oral 64copper with copper balance.

1. Pharmacokinetic study of orally administered zinc in humans: evidence for an enteral recirculation.

Review 2. Current anti-copper therapies in management of Wilson disease.

3. Copper-Induced Upregulation of MicroRNAs Directs the Suppression of Endothelial LRP1 in Alzheimer's Disease Model.

4. The Function of ATPase Copper Transporter ATP7B in Intestine.

5. Low levels of copper disrupt brain amyloid-β homeostasis by altering its production and clearance.

6. Refining the position of Wilson disease by linkage disequilibrium with polymorphic microsatellites.

7. Polymorphic microsatellites and Wilson disease (WD).

Review 8. Practical recommendations and new therapies for Wilson's disease.

9. Absorption and metabolism of oral zinc gluconate in humans in fasting state, during, and after a meal.

10. Linkage of the Wilson disease gene to chromosome 13 in North-American pedigrees.