differential hfe gene expression is regulated by alternative splicing in human tissues微分hfe基因表达受可变剪接在人体组织.pdfVIP
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differential hfe gene expression is regulated by alternative splicing in human tissues微分hfe基因表达受可变剪接在人体组织
Differential HFE Gene Expression Is Regulated by
Alternative Splicing in Human Tissues
. .
Rute Martins , Bruno Silva , Daniela Proenc¸a, Paula Faustino*
´ ´
Departamento de Genetica, Instituto Nacional de Saude Dr. Ricardo Jorge, Lisboa, Portugal
Abstract
Background: The pathophysiology of HFE-derived Hereditary Hemochromatosis and the function of HFE protein in iron
homeostasis remain uncertain. Also, the role of alternative splicing in HFE gene expression regulation and the possible
function of the corresponding protein isoforms are still unknown. The aim of this study was to gain insights into the
physiological significance of these alternative HFE variants.
Methodology/Principal Findings: Alternatively spliced HFE transcripts in diverse human tissues were identified by RT-PCR,
cloning and sequencing. Total HFE transcripts, as well as two alternative splicing transcripts were quantified using a real-
time PCR methodology. Intracellular localization, trafficking and protein association of GFP-tagged HFE protein variants
were analysed in transiently transfected HepG2 cells by immunoprecipitation and immunofluorescence assays. Alterna-
tively spliced HFE transcripts present both level- and tissue-specificity. Concerning the exon 2 skipping and intron 4
inclusion transcripts, the liver presents the lowest relative level, while duodenum presents one of the highest amounts. The
protein resulting from exon 2 skipping transcript is unable to associate with b2M and TfR1 and reveals an ER retention.
Conversely, the intron 4 inclusion transcript gives rise to a truncated, soluble protein (sHFE) that is mostly secreted by cells
to the medium in associatio
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