2003
DOI: 10.1096/fj.03-0106fje
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C‐terminal fragments of amyloid precursor protein exert neurotoxicity by inducing glycogen synthase kinase‐3β expression

Abstract: The AICD (amyloid precursor protein [APP] intracellular domain) and C31, the caspase-cleaved C-terminal fragment of APP, have been found in the brains of patients with Alzheimer's disease (AD). Here, we demonstrate for the first time that the C-terminal fragments of APP (AICD [C57, C59] and C31) exert neurotoxicity on differentiated PC 12 cells and rat primary cortical neurons by inducing the expression of glycogen synthase kinase 3beta, forming a ternary complex with Fe65 and CP2/LSF/LBP1 in the nucleus, wher… Show more

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Cited by 251 publications
(259 citation statements)
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“…AICD-EGFP-transfected cells showed predominantly nuclear staining, whereas enhanced green fluorescent protein (EGFP) control vector-transfected cells were stained through the whole cell (see Supplemental Figure). Interestingly, transfection rates were low, and just low-level-expressing AICD-EGFP-transfected cells survived 24 h. This supports the discussed toxicity of AICD (Bertrand et al, 2001;Kim et al, 2003), which might be increased as a result of higher stability when expressed as fusion protein. FE65 immunostaining in iFA clones revealed nuclear staining of FE65 (data not shown).…”
supporting
confidence: 66%
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“…AICD-EGFP-transfected cells showed predominantly nuclear staining, whereas enhanced green fluorescent protein (EGFP) control vector-transfected cells were stained through the whole cell (see Supplemental Figure). Interestingly, transfection rates were low, and just low-level-expressing AICD-EGFP-transfected cells survived 24 h. This supports the discussed toxicity of AICD (Bertrand et al, 2001;Kim et al, 2003), which might be increased as a result of higher stability when expressed as fusion protein. FE65 immunostaining in iFA clones revealed nuclear staining of FE65 (data not shown).…”
supporting
confidence: 66%
“…Indeed, there is evidence that binding of FE65 to AICD is necessary for the nuclear translocation (Kimberly et al, 2001;Muresan and Muresan, 2004;von Rotz et al, 2004). Two different AICD transcriptionally active complexes based on the binding of AICD-FE65 to TIP60 and to CP2/ LSF/LBP1 have been suggested (Cao and Sudhof, 2001;Kim et al, 2003). TIP60 is part of a large nuclear complex with DNA binding, ATPase and DNA helicase activity (Ikura et al, 2000).…”
Section: Discussionmentioning
confidence: 99%
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“…The generation of the C-terminal fragment C31 results from the cleavage of APP at the caspase site D720 of the C-terminus by caspase 3 [165]. Once generated, C31 enhances glycogen synthase kinase-3β expression and tau protein phosphorylation [107].…”
Section: The Forkhead Transcription Factor Glycogen Synthase Kinase-mentioning
confidence: 99%