2002
DOI: 10.1046/j.0022-3042.2002.00770.x
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Expression of human β‐secretase in the mouse brain increases the steady‐state level of β‐amyloid

Abstract: b-Site APP-cleaving enzyme (BACE) initiates the processing of the amyloid precursor protein (APP) leading to the generation of b-amyloid, the main component of Alzheimer's disease senile plaques. BACE (Asp2, memapsin 2) is a type I transmembrane aspartyl protease and is responsible for the b-secretase cleavage of APP producing different endoproteolytic fragments referred to as the carboxy-terminal C99, C89 and the soluble ectodomain sAPPb. Here we describe two transgenic mouse lines expressing human BACE in th… Show more

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Cited by 114 publications
(99 citation statements)
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“…The observation that mice with a targeted deletion of BACE1 are viable and fertile but fail to produce any A␤ indicates that BACE1 is strictly required for A␤ generation and that inhibition of BACE1 activity might be a safe and effective treatment option for AD (6,40,51,62). Because the increased BACE1 activity observed in AD patients does not seem to arise from genetic mutations or polymorphisms in BACE1 (1,42,47,51), the identification of factors that effectively regulate BACE1 activity is apparently a highly promising approach to treating AD. PAR-4 is a leucine zipper protein that was initially identified to be associated with neuronal degeneration in AD (94).…”
Section: Fig 2 Specific Interaction Between Par-4 and Bace1 In Tranmentioning
confidence: 99%
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“…The observation that mice with a targeted deletion of BACE1 are viable and fertile but fail to produce any A␤ indicates that BACE1 is strictly required for A␤ generation and that inhibition of BACE1 activity might be a safe and effective treatment option for AD (6,40,51,62). Because the increased BACE1 activity observed in AD patients does not seem to arise from genetic mutations or polymorphisms in BACE1 (1,42,47,51), the identification of factors that effectively regulate BACE1 activity is apparently a highly promising approach to treating AD. PAR-4 is a leucine zipper protein that was initially identified to be associated with neuronal degeneration in AD (94).…”
Section: Fig 2 Specific Interaction Between Par-4 and Bace1 In Tranmentioning
confidence: 99%
“…The observation that mice with a targeted deletion of BACE1 are viable and fertile but fail to produce any A␤ indicates that BACE1 is required for A␤ generation (6,40,51,62). Because neither genetic mutations nor polymorphisms in BACE1 seem to be responsible for the increased BACE1 activity observed in AD patients (1,42,47,51), the identification of factors that effectively regulate BACE1 activity is apparently a highly promising approach to treating AD.…”
mentioning
confidence: 99%
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“…With the identification of BACE1 [36,37,40], it was determined that β-secretase cleavage can be, in fact, the rate-limiting event for Aβ production. In addition, overexpression of BACE1 in APP transgenic mice results in increased β-secretase cleavage products particularly increased Aβ levels [2,4,28] as well as altered amyloid deposition pathology [4,28,38]. Specifically, we have previously reported an altered brainregional deposition profile in our double BACE1xAPP transgenic mice.…”
Section: Introductionmentioning
confidence: 53%