Axis Shield | J Am Coll Nutr. 1998 Jun;17(3):235-8.


Active B12 Introduction What Is Active-B12 What Is The Function of Active-B12 Why Use Active-B12 Measuring Active-B12 Clinical Utility Of Active-B12 Case Studies FAQs B12 Deficiency General Diagnosis At Risk Groups Guidelines Treatment Publications Recent Abstracts Archived Abstracts Posters Recent Posters Archived Posters Presentations Downloadable Presentation News Latest News Archived News Meetings Forthcoming Meetings Meeting Reports Meeting Archive
Publications - Archived Abstracts - J Am Coll Nutr. 1998 Jun;17(3):235-8. Cobalamin (vitamin B12) and holotranscobalamin changes in plasma and liver tissue in alcoholics with liver disease. Baker H, Leevy CB, DeAngelis B, Frank O, Baker ER. Department of Preventive Medicine and Community Health, University of Medicine and Dentistry, New Jersey Medical School, Newark 07107-3001, USA. OBJECTIVE: We wanted to know if alterations in plasma cobalamin (B12) concentration and B12 carriers, e.g., holotranscobalamins (holo TC), occur in blood and liver tissue from patients with severe alcoholic liver disease. Our purpose was to test the hypothesis that liver disease may disrupt B12 distribution. METHOD: Total B12, as well as B12 bound to transcobalamin I, II, III (holo TC), were measured to determine their concentration in plasma and in liver tissue; Poteriochromonas malhamensis--a protozoan reagent served to measure only metabolically active (true) B12. Total B12 as distributed in holo TC in plasma and liver tissue of healthy subjects (controls) were compared to patients with severe alcoholic liver disease. RESULTS: Severe liver disease initiates highly elevated B12 levels in plasma and a lowered liver tissue total B12 concentration. The percent of B12 distributed to holo TC II is significantly depleted during liver disease. In contrast, holo TC I and III are elevated in plasma during liver disease and contain more B12 than controls. Total B12 and B12 distributed to TC are lower in diseased liver tissue. CONCLUSION: Severe alcoholic liver disease involves leakage of total B12 from liver tissue into the plasma. Holo TC I and III concentration increases in plasma; this preserves the high plasma B12 from being excreted. However, plasma holo TC II B12 distribution is decreased, indicating that there is a depression of exogenous B12 entering the plasma and tissues. In severe liver disease, liver tissue B12 binding and storage by TC is disrupted and causes B12 to leak out of the liver into the circulation. Eventually liver disease could produce enough severe tissue B12 deficits to cause metabolic dysfunction despite elevated plasma total B12. Elevation of plasma B12, accompanied by a lowering of holo TC II distribution, seemed to be a useful index of liver disease severity suggesting preventive treatment « Back to abstracts	News Coming Soon ! The full video recording of the Euromedlab 2007 Active B12 workshop will be available in the next few weeks, register for your copy. Live CME Web Conference on vitamin B12 deficiency, Prof. Ralph Green, Dec 13th 2007, register now. read more » Meetings 8-11 December, 2007 American Society of Hematology, Atlanta, booth 544 read more »
© Axis-Shield, 2002-2007 \| Links \| Register \| Axis Shield Website \| Disclaimer

News

Meetings