AI Article Synopsis
- ApoE4 in neurons may play a role in Alzheimer's disease development, and a specific splicing variant of apoE mRNA (apoE-I3) was discovered that is expressed in neurons but not in astrocytes.
- Detection methods showed that apoE-I3 is primarily found in the nucleus of neurons and doesn't lead to protein production.
- The regulation of apoE expression appears to be influenced by the presence or absence of intron-3 in the mRNA, with injury to neurons affecting the levels of apoE-I3 and mature apoE mRNA in opposite ways.
Article Abstract
Neuronal expression of apolipoprotein (apo) E4 may contribute to the pathogenesis of Alzheimer's disease (AD). In studying how apoE expression is regulated in neurons, we identified a splicing variant of apoE mRNA with intron-3 retention (apoE-I3). ApoE-I3 mRNA was detected in neuronal cell lines and primary neurons, but not in astrocytic cell lines or primary astrocytes, from humans and mice by reverse transcription (RT)-PCR. In both wild-type and human apoE knock-in mice, apoE-I3 was found predominantly in cortical and hippocampal neurons by in situ hybridization. Cell fractionation and quantitative RT-PCR revealed that over 98% of the apoE-I3 mRNA was retained in the nucleus without protein translation. In transfected primary neurons, apoE expression increased dramatically when intron-3 was deleted from a genomic DNA construct and decreased markedly when intron-3 was inserted into a cDNA construct, suggesting that intron-3 retention/splicing controls apoE expression in neurons. In response to excitotoxic challenge, the apoE-I3 mRNA was markedly increased in morphologically normal hippocampal neurons but reduced in degenerating hippocampal neurons in mice; apoE mRNA showed the opposite pattern. This apparent precursor-product relationship between apoE-I3 and apoE mRNA was supported by a transcriptional inhibition study. Thus, neuronal expression of apoE is controlled by transcription of apoE-I3 under normal conditions and by processing of apoE-I3 into mature apoE mRNA in response to injury.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6671590 | PMC |
| http://dx.doi.org/10.1523/JNEUROSCI.3253-07.2008 | DOI Listing |
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