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Am J Physiol Gastrointest Liver Physiol 286: G385-G394, 2004. First published October 30, 2003; doi:10.1152/ajpgi.00246.2003
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MUCOSAL BIOLOGY

Hepcidin regulation of ferroportin 1 expression in the liver and intestine of the rat

Kwo-yih Yeh,1,2,3 Mary Yeh,1,3 and Jonathan Glass1,3

Departments of 1Medicine and 2Molecular and Cellular Physiology and 3The Feist-Weiller Cancer Center, Louisiana State University Health Sciences Center, Shreveport, Louisiana 71130–3932

Submitted 30 May 2003 ; accepted in final form 24 October 2003

Hepcidin has been implicated as the iron stores regulator: a hepatic signaling molecule that regulates intestinal iron absorption by undefined mechanisms. The possibility that hepcidin regulates the expression of ferroportin 1 (FPT1), the basolateral iron transporter, was examined in rats after administration of LPS, an iron chelator, or His-tagged recombinant hepcidin (His-rHepc). In the liver, LPS stimulated a biphasic increase of hepcidin mRNA with peaks of mRNA at 6 and 36 h. Concurrently, hepatic FPT1 mRNA expression decreased to minimal level at 6 h and then increased with a peak at 24–36 h. LPS also induced biphasic changes in intestinal FPT1 mRNA expression, with decreased levels at 6 h and increased expression at 48 h. Whereas the initial decrease of FPT1 coincides with an LPS-induced decrease in serum iron, both intestinal and hepatic FPT1 expression recovered, whereas serum iron concentration continued to decrease for at least 24 h. Dietary iron ingestion increased intestinal ferritin protein production but did not reduce intestinal FPT1 mRNA expression. The iron chelator pyrrolidinedithiocarbamate (PDTC) stimulated hepatic hepcidin without suppressing intestinal FPT1 expression. In PDTC-treated rats, LPS stimulated no additional hepatic hepcidin expression but did increase intestinal FPT1 expression. Administration of HisrHepc induced significant reduction of intestinal FPT1 expression. Taken together, these data suggest that hepcidin mediates LPS-induced downregulation of intestinal FPT1 expression and that the hepcidin signaling pathway involves a PDTC-sensitive step.

intestinal iron absorption; lipopolysaccharide activation of hepcidin; His-tagged hepcidin; inverse relationship between hepcidin and ferroportin 1 expression



Address for reprint requests and other correspondence: K.-y. Yeh, Section of Hematology/Oncology, Dept. of Medicine, LSU Health Sciences Center, 1501 Kings Highway, Shreveport, LA 71130–3932 (E-mail: kyeh{at}lsuhsc.edu).




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