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Selenoprotein P-Expression, functions, and roles in mammals

Journal

BIOCHIMICA ET BIOPHYSICA ACTA-GENERAL SUBJECTS
Volume 1790, Issue 11, Pages 1441-1447

Publisher

ELSEVIER SCIENCE BV
DOI: 10.1016/j.bbagen.2009.03.026

Keywords

Selenium transport and homeostasis; Selenium for spermatogenesis; Selenium for the brain; Selenium scavenging from glomerular filtrate; Binding of Sepp1 to the lipoprotein receptor apoER2 and megalin; Sepp1 as a marker of selenium nutritional status

Funding

  1. NIH [ES02497, DK58763]

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Selenoprotein P (Sepp1) is a secreted protein that is made up of 2 domains. The larger N-terminal domain contains 1 selenocysteine residue in a redox motif and the smaller C-terminal domain contains the other 9 selenocysteines. Sepp1 isoforms of varying lengths occur but quantitation of them has not been achieved. Hepatic synthesis of Sepp1 affects whole-body selenium content and the liver is the source of most plasma Sepp1. ApoER2, a member of the lipoprotein receptor family, binds Sepp1 and facilitates its uptake into the testis and retention of its selenium by the brain. Megalin, another lipoprotein receptor, facilitates uptake of filtered Sepp1 into proximal tubule cells of the kidney. Thus, Sepp1 serves in homeostasis and distribution of selenium. Mice with deletion of Sepp1 suffer greater morbidity and mortality from infection with Trypanosoma cangolense than do wild-type mice. Mice that express only the N-terminal domain of Sepp1 have the same severity of illness as wild-type mice, indicating that the protective function of Sepp1 against the infection resides in the N-terminal (redox) domain. Thus, Sepp1 has several functions. In addition, plasma Sepp1 concentration falls in selenium deficiency and, therefore, it can be used as an index of selenium nutritional status. (C) 2009 Elsevier B.V. All rights reserved.

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