Volume 1, Issue 3, Pages (March 2005)

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Volume 1, Issue 3, Pages 191-200 (March 2005) The iron exporter ferroportin/Slc40a1 is essential for iron homeostasis  Adriana Donovan, Christine A. Lima, Jack L. Pinkus, Geraldine S. Pinkus, Leonard I. Zon, Sylvie Robine, Nancy C. Andrews  Cell Metabolism  Volume 1, Issue 3, Pages 191-200 (March 2005) DOI: 10.1016/j.cmet.2005.01.003 Copyright © 2005 Elsevier Inc. Terms and Conditions

Figure 1 Embryonic expression of ferroportin protein Immunohistochemical staining for ferroportin in a wild-type E7.0 embryo (A). The brown staining indicates the expression of ferroportin in the extraembryonic visceral endoderm (arrow). At higher power ([A], inset), it is evident that these cells are a polarized epithelium with ferroportin expressed on the basolateral surface, as it is in duodenal enterocytes of the intestine. A littermate of the embryo in (A) that appears significantly smaller and has no detectable ferroportin protein by immunohistochemistry (B). The arrow points to the extraembryonic visceral endoderm. Cell Metabolism 2005 1, 191-200DOI: (10.1016/j.cmet.2005.01.003) Copyright © 2005 Elsevier Inc. Terms and Conditions

Figure 2 Conditional deletion of ferroportin by Meox2-Cre causes iron deficiency anemia The 10-day-old Meox2-cre;Fpn1flox/flox pup ([A], bottom) is small and pale compared to a wild-type littermate ([A], top). Peripheral blood smear of a 12-day-old wild-type animal stained with Wright-Giemsa (B). Peripheral blood smear of a 12-day-old Meox2-Cre;Fpn1flox/flox animal stained with Wright-Giemsa (C). Cell Metabolism 2005 1, 191-200DOI: (10.1016/j.cmet.2005.01.003) Copyright © 2005 Elsevier Inc. Terms and Conditions

Figure 3 Meox2-Cre;Fpn mutant mice accumulate iron in enterocytes, macrophages, and hepatocytes Perls Prussian blue stain for iron in crosssections of duodenal villi of 12-day-old mice (A and B). Blue staining shows iron accumulated in enterocytes. DAB-enhanced Perls stain for iron in liver sections from 12-day-old mice (C and D). Brown staining shows iron accumulated in cells. The asterix (*) marks a Kupffer cell, and the arrow points to hepatocytes that are loaded with iron. DAB-enhanced Perls stain for iron in spleen sections of 12-day-old mice (E and F). The genotypes of the mice are the following: Fpnflox/flox (A, C, and E) and Meox2-Cre;Fpnflox/flox (B, D, and F). Cell Metabolism 2005 1, 191-200DOI: (10.1016/j.cmet.2005.01.003) Copyright © 2005 Elsevier Inc. Terms and Conditions

Figure 4 Meox2-Cre;Fpn mutant mice have abnormal nonheme iron levels in liver and spleen Box plot depicting the measurement of nonheme iron levels (μg Fe/g wet weight) in liver and spleen of wild-type controls (pink boxes) and Meox2-Cre;Fpn mutants (white boxes). The genotypes of the Meox2-Cre;Fpn mutant mice were Meox2-Cre;Fpnflox/flox and Meox2-Cre;Fpnflox/null. The genotypes of the wild-type controls were Fpnflox/flox, Fpnflox/+, and Fpnflox/null. We analyzed animals at two different ages: (1) 10- to 12-day-old mice (wild-type n = 6 and mutant n = 7) and (2) 18- to 22-day-old mice (wild-type n = 13 and mutant n = 11). This data was collected from both male and female animals. p values were calculated using Student’s T-test. The box plot was drawn using Statview 5.0.1 (SAS Institute, Inc.) The middle bar of the box represents the median. The top of the box is the 75th percentile of the data set, and the bottom of the box is the 25th percentile. The top whisker represents the 90th percentile of the data, and the bottom whisker represents the 10th percentile of the data. The circles represent data points that lie outside of the 10th and 90th percentiles. Cell Metabolism 2005 1, 191-200DOI: (10.1016/j.cmet.2005.01.003) Copyright © 2005 Elsevier Inc. Terms and Conditions

Figure 5 Conditional deletion of ferroportin in enterocytes by vil-Cre-ERT2 PCR analysis of tissue DNA from a vil-Cre-ERT2;Fpnflox/flox mouse that was injected with tamoxifen (A). Tail (T), liver (L), spleen (S), kidney (K), lung (Lu), pancreas (P), heart (H), intestine (I). The marker is a 100 bp ladder. The floxed allele is 522 bp, and the full deletion allele is 398 bp. Immunohistochemistry for ferroportin protein in a wild-type animal (B) and a vil-Cre-ERT2;Fpnflox/flox mouse injected with tamoxifen (C). Brown staining represents ferroportin expression in duodenal enterocytes. Higher magnification images show basolateral localization of ferroportin in the wild-type animals ([B], inset) and absence of ferroportin expression in the vil-Cre-ERT2;Fpnflox/flox mouse ([C], inset). Cell Metabolism 2005 1, 191-200DOI: (10.1016/j.cmet.2005.01.003) Copyright © 2005 Elsevier Inc. Terms and Conditions

Figure 6 Ferroportin is critical for intestinal iron absorption Wright-Giemsa-stained peripheral blood smears of tamoxifen-injected Fpnflox/flox (A) and vil-Cre-ERT2;Fpnflox/flox (B) animals. Perls stain for nonheme iron in the duodenum of tamoxifen injected Fpnflox/flox (C) and vil-Cre-ERT2;Fpnflox/flox (D) animals. Blue staining represents nonheme iron accumulation in duodenal enterocytes. Cell Metabolism 2005 1, 191-200DOI: (10.1016/j.cmet.2005.01.003) Copyright © 2005 Elsevier Inc. Terms and Conditions