Review articleThe role of APOE in transgenic mouse models of AD
-
Add time:09/02/2019 Source:sciencedirect.com
Identified in 1993, APOE4 is the greatest genetic risk factor for Alzheimer’s disease (AD), increasing risk up to 15-fold compared to the common variant APOE3. Since the mid 1990’s, transgenic (Tg) mice have been developed to model AD pathology and progression, primarily via expression of the familial AD (FAD) mutations in the presence of mouse-APOE (m-APOE). APOE4, associated with enhanced amyloid-β (Aβ) accumulation, has rarely been the focus in designing FAD-Tg mouse models. Initially, FAD-Tg mice were crossed with human (h)-APOE driven by heterologous promoters to identify an APOE genotype-specific AD phenotype. These models were later supplemented with FAD-Tg mice crossed with APOE-knockouts (APOE-/- or APOE-KO) and h-APOE-targeted replacement (h-APOE-TR) mice, originally generated to study the role of APOE genotype in peripheral lipid metabolism and atherosclerotic lesion development. Herein, we compare the m- and h-APOE multi-gene clusters, and then critically review the relevant history and approaches to developing a Tg mouse model to characterize APOE-dependent AD pathology, in combination with genetic (sex, age) and modifiable (e.g., inflammation, obesity) risk factors. Finally, we present recent data from the EFAD mice, which express 5xFAD mutations with the expression of the human apoE isoforms (E2FAD, E3FAD and E4FAD). This includes a study of 6- and 18-month-old male and female E3FAD and E4FAD, a comparison that enables examination of the interaction among the main AD risk factors: age, APOE genotype and sex. While no single transgenic mouse can capture the effects of all modifiable and genetic risk factors, going forward, a conscious effort needs to be made to include the factors that most significantly modulate AD pathology.
We also recommend Trading Suppliers and Manufacturers of AD 20 (cas 111542-07-5). Pls Click Website Link as below: cas 111542-07-5 suppliers
Prev:Temporal Certainty and Skippable In-Stream Commercials: Effects of Ad Length, Timer, and Skip-ad Button on Irritation and Skipping Behavior
Next:Full length articleExploring the effects of ad-task relevance and ad salience on ad avoidance: The moderating role of internet use motivation) - 【Back】【Close 】【Print】【Add to favorite 】
- Related Information
- New perspective on the metabolism of AD-1 in vivo: Characterization of a series of dammarane-type derivatives with novel metabolic sites and anticancer mechanisms of active oleanane-type metabolites09/10/2019
- Multi-modal AD classification via self-paced latent correlation analysis09/09/2019
- To use or not to use ad blockers? The roles of knowledge of ad blockers and attitude toward online advertising09/08/2019
- Neural responses to functional and experiential ad appeals: Explaining ad effectiveness09/07/2019
- Proteomes analysis reveals the involvement of autophagy in AD-like neuropathology induced by noise exposure and ApoE409/06/2019
- Flexible SDN control in tactical ad hoc networks09/05/2019
- Relevance-based entity selection for ad hoc retrieval09/04/2019
- Full length articleExploring the effects of ad-task relevance and ad salience on ad avoidance: The moderating role of internet use motivation09/03/2019
- Temporal Certainty and Skippable In-Stream Commercials: Effects of Ad Length, Timer, and Skip-ad Button on Irritation and Skipping Behavior09/01/2019
