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Human APOE isoform-dependent effects on brain beta-amyloid levels in PDAPP transgenic mice

To investigate the role of human apolipoprotein E (apoE) on Abeta deposition in vivo, we crossed PDAPP mice lacking mouse Apoe to targeted replacement mice expressing human apoE (PDAPP/TRE2, PDAPP/TRE3, or PDAPP/TRE4). We then measured the levels of apoE protein and Abeta peptides in plasma, CSF, an...

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Published in:	The Journal of neuroscience 2009-05, Vol.29 (21), p.6771-6779
Main Authors:	Bales, Kelly R, Liu, Feng, Wu, Su, Lin, Suizhen, Koger, Deanna, DeLong, Cynthia, Hansen, Jeffrey C, Sullivan, Patrick M, Paul, Steven M
Format:	Article
Language:	English
Subjects:	Age Factors Amyloid beta-Peptides - metabolism Amyloid beta-Protein Precursor - genetics Analysis of Variance Animals Apolipoproteins E - classification Apolipoproteins E - genetics Apolipoproteins E - metabolism Brain - metabolism Humans Mice Mice, Inbred C57BL Mice, Transgenic Mutation Peptide Fragments - metabolism Protein Isoforms - metabolism
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creator	Bales, Kelly R Liu, Feng Wu, Su Lin, Suizhen Koger, Deanna DeLong, Cynthia Hansen, Jeffrey C Sullivan, Patrick M Paul, Steven M
description	To investigate the role of human apolipoprotein E (apoE) on Abeta deposition in vivo, we crossed PDAPP mice lacking mouse Apoe to targeted replacement mice expressing human apoE (PDAPP/TRE2, PDAPP/TRE3, or PDAPP/TRE4). We then measured the levels of apoE protein and Abeta peptides in plasma, CSF, and brain homogenates in these mice at different ages. We also quantified the amount of brain Abeta and amyloid burden in 18-month-old mice. In young PDAPP/TRE4 mice that were analyzed at an age before brain Abeta deposition, we observed a significant decrease in the levels of apoE in CSF and brain when compared with age-matched mice expressing either human E2 or E3. The brain levels of Abeta42 in PDAPP/TRE4 mice were substantially elevated even at this very early time point. In older PDAPP/TRE4 mice, the levels of insoluble apoE protein increased in parallel to the dramatic rise in brain Abeta burden, and the majority of apoE was associated with Abeta. In TRE4 only mice, we also observed a significant decrease in the level of apoE in brain homogenates. Since the relative level of apoE mRNA was equivalent in PDAPP/TRE and TRE only mice, it appears that post-translational mechanisms influence the levels of apoE protein in brain (E4 < E3 > E3 > E2) that increase with age. Therapeutic strategies aimed at increasing the soluble levels of apoE protein, regardless of isoform, may effectively prevent and (or) treat Alzheimer's disease.
doi_str_mv	10.1523/JNEUROSCI.0887-09.2009
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We then measured the levels of apoE protein and Abeta peptides in plasma, CSF, and brain homogenates in these mice at different ages. We also quantified the amount of brain Abeta and amyloid burden in 18-month-old mice. In young PDAPP/TRE4 mice that were analyzed at an age before brain Abeta deposition, we observed a significant decrease in the levels of apoE in CSF and brain when compared with age-matched mice expressing either human E2 or E3. The brain levels of Abeta42 in PDAPP/TRE4 mice were substantially elevated even at this very early time point. In older PDAPP/TRE4 mice, the levels of insoluble apoE protein increased in parallel to the dramatic rise in brain Abeta burden, and the majority of apoE was associated with Abeta. In TRE4 only mice, we also observed a significant decrease in the level of apoE in brain homogenates. Since the relative level of apoE mRNA was equivalent in PDAPP/TRE and TRE only mice, it appears that post-translational mechanisms influence the levels of apoE protein in brain (E4 < E3 << E2), resulting in early and dramatic apoE isoform-dependent effects on brain Abeta levels (E4 >> E3 > E2) that increase with age. 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Since the relative level of apoE mRNA was equivalent in PDAPP/TRE and TRE only mice, it appears that post-translational mechanisms influence the levels of apoE protein in brain (E4 < E3 << E2), resulting in early and dramatic apoE isoform-dependent effects on brain Abeta levels (E4 >> E3 > E2) that increase with age. Therapeutic strategies aimed at increasing the soluble levels of apoE protein, regardless of isoform, may effectively prevent and (or) treat Alzheimer's disease.</description><subject>Age Factors</subject><subject>Amyloid beta-Peptides - metabolism</subject><subject>Amyloid beta-Protein Precursor - genetics</subject><subject>Analysis of Variance</subject><subject>Animals</subject><subject>Apolipoproteins E - classification</subject><subject>Apolipoproteins E - genetics</subject><subject>Apolipoproteins E - metabolism</subject><subject>Brain - metabolism</subject><subject>Humans</subject><subject>Mice</subject><subject>Mice, Inbred C57BL</subject><subject>Mice, Transgenic</subject><subject>Mutation</subject><subject>Peptide Fragments - metabolism</subject><subject>Protein Isoforms - metabolism</subject><issn>0270-6474</issn><issn>1529-2401</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2009</creationdate><recordtype>article</recordtype><recordid>eNpVkUFP3DAQha2KqizQv4B84pbt2Int-FJptWwLCHVXLVx6sSa2A0ZJvNhZJP59s2JF28uMNG_em5E-Qs4ZzJng5ZebH6v7n-tfy-s51LUqQM85gP5AZpOqC14BOyIz4AoKWanqmJzk_AQACpj6RI6ZnoYliBn5fbXrcaCLzXpFQ45tTH3h_NYPzg8j9W3r7ZhpHGiTMEzVj1hg_9rF4GjnX3yX6TTeXC42GzomHPKDH4KlfbD-jHxsscv-86Gfkrtvq7vlVXG7_n69XNwWtpTVWGBV8aZksmGuxEq2WrlG6Fpy6yQ6dFCjEJorL2wrsAYnG8eFa7BqrVVleUq-vsVud03vnZ3-TtiZbQo9plcTMZj_lSE8mof4YqSUQig9BVwcAlJ83vk8mj5k67sOBx932UjFa6aYnBbl26JNMefk2_cjDMyeinmnYvZUDGizpzIZz_998a_tgKH8A31ei6M</recordid><startdate>20090527</startdate><enddate>20090527</enddate><creator>Bales, Kelly R</creator><creator>Liu, Feng</creator><creator>Wu, Su</creator><creator>Lin, Suizhen</creator><creator>Koger, Deanna</creator><creator>DeLong, Cynthia</creator><creator>Hansen, Jeffrey C</creator><creator>Sullivan, Patrick M</creator><creator>Paul, Steven M</creator><general>Society for Neuroscience</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope><scope>5PM</scope></search><sort><creationdate>20090527</creationdate><title>Human APOE isoform-dependent effects on brain beta-amyloid levels in PDAPP transgenic mice</title><author>Bales, Kelly R ; 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subjects	Age Factors Amyloid beta-Peptides - metabolism Amyloid beta-Protein Precursor - genetics Analysis of Variance Animals Apolipoproteins E - classification Apolipoproteins E - genetics Apolipoproteins E - metabolism Brain - metabolism Humans Mice Mice, Inbred C57BL Mice, Transgenic Mutation Peptide Fragments - metabolism Protein Isoforms - metabolism
title	Human APOE isoform-dependent effects on brain beta-amyloid levels in PDAPP transgenic mice
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