2007
DOI: 10.1523/jneurosci.1153-07.2007
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Deletion of Apolipoprotein E Receptor-2 in Mice Lowers Brain Selenium and Causes Severe Neurological Dysfunction and Death When a Low-Selenium Diet Is Fed

Abstract: Selenoprotein P (Sepp1) is a plasma and extracellular protein that is rich in selenium. Deletion of Sepp1 results in sharp decreases of selenium levels in the brain and testis with dysfunction of those organs. Deletion of Sepp1 also causes increased urinary selenium excretion, leading to moderate depletion of whole-body selenium. The lipoprotein receptor apolipoprotein E receptor-2 (apoER2) binds Sepp1 and facilitates its uptake by Sertoli cells, thus providing selenium for spermatogenesis. Experiments were pe… Show more

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Cited by 159 publications
(143 citation statements)
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“…ApoER2 was shown to bind SelP and facilitate its uptake by testis and brain (35,276). Consistent with its role in Se metabolism in these tissues, ApoER2 knockout mice showed sharply decreased Se levels in testis and brain that were associated with neurological dysfunction and defective spermatogenesis similar to phenotypes observed in SelP Ϫ/Ϫ mice.…”
Section: Selenoprotein Pmentioning
confidence: 58%
“…ApoER2 was shown to bind SelP and facilitate its uptake by testis and brain (35,276). Consistent with its role in Se metabolism in these tissues, ApoER2 knockout mice showed sharply decreased Se levels in testis and brain that were associated with neurological dysfunction and defective spermatogenesis similar to phenotypes observed in SelP Ϫ/Ϫ mice.…”
Section: Selenoprotein Pmentioning
confidence: 58%
“…Apoer2 also protects against neurodegeneration through another, mechanistically distinct mechanism, which involves its role in the uptake of essential selenoproteins into the brain (Burk et al 2007). Loss of Apoer2 sensitizes the animals to low dietary selenium levels resulting in death from rapid and severe neurodegeneration.…”
Section: Apoe Receptors Protect Against Neurodegenerationmentioning
confidence: 99%
“…At the time of writing, a study by Burk et al (2007) was published that reports on slightly lower brain selenium levels in apoER2 knockout mice. Although the question as to whether apoER2 regulates GPx4 expression is still unanswered, these recent data suggest that the apoER2 -/-phenotype may also be attributed to overall altered selenoprotein expression in neurons and glial cells.…”
Section: Conclusion and Perspectivementioning
confidence: 99%