Iron metabolism in the hemoglobin-deficit mouse: correlation of diferric transferrin with hepcidin expression

Author:

Wilkins Sarah J.1,Frazer David M.1,Millard Kirstin N.1,McLaren Gordon D.1,Anderson Gregory J.1

Affiliation:

1. From the Iron Metabolism Laboratory, The Queensland Institute of Medical Research, Brisbane, Australia; and the VA Long Beach Healthcare System, Long Beach, and Division of Hematology/Oncology, University of California, Irvine.

Abstract

The iron requirements of the erythroid compartment modulate the expression of hepcidin in the liver, which in turn alters intestinal iron absorption and iron release from the reticuloendothelial system. We have taken advantage of an inherited anemia of the mouse (hemoglobin deficit, or hbd) to gain insights into the factors regulating hepcidin expression. hbd mice showed a significant anemia but, surprisingly, their iron absorption was not increased as it was in wild-type animals made anemic to a similar degree by dietary iron depletion. In wild-type mice hepatic hepcidin levels were decreased but in hbd animals a significant and unexpected increase was observed. The level of absorption was appropriate for the expression of hepcidin in each case, but in hbd mice did not reflect the degree of anemia. However, this apparent inappropriate regulation of hepcidin correlated with increased transferrin saturation and levels of diferric transferrin in the plasma, which in turn resulted from the reduced capacity of hbd animals to effectively use transferrin-bound iron. These data strengthen the proposal that diferric transferrin is a key indicator of body iron requirements.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

Reference45 articles.

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2. Bannerman RM, Garrick LM, Rusnak-Smalley P, Hoke JE, Edwards JA. Hemoglobin deficit: an inherited hypochromic anemia in the mouse. Proc Soc Exp Biol Med. 1986;182: 52-57.

3. Bloom ML, Simon-Stoos KL, Mabon ME. The hemoglobin-deficit mutation is located on mouse chromosome 19. Mamm Genome. 1998;9: 666-667.

4. Bloom ML, Simon-Stoos KL. The hemoglobin-deficit mouse: analysis of phenotype and hematopoiesis in the transplant model. Blood. 1997;90: 2062-2067.

5. Garrick LM, Edwards JA, Hoke JE, Bannerman RM. Diminished acquisition of iron by reticulocytes from mice with hemoglobin deficit. Exp Hematol. 1987;15: 671-675.

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