Your search keyword '"EFAD-Tg mouse model"' showing total 3 results

1. Alzheimer's disease pathology in APOE transgenic mouse models: The Who, What, When, Where, Why, and How

Author

Cutler T. Lewandowski, Juan Maldonado Weng, and Mary Jo LaDu

Subjects

Alzheimer's Disease (AD), familial AD transgenic mice (FAD-Tg), apolipoprotein E, sex and AD risk, APOE4 and AD risk, EFAD-Tg mouse model, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The focus on amyloid plaques and neurofibrillary tangles has yielded no Alzheimer’s disease (AD) modifying treatments in the past several decades, despite successful studies in preclinical mouse models. This inconsistency has caused a renewed focus on improving the fidelity and reliability of AD mouse models, with disparate views on how this improvement can be accomplished. However, the interactive effects of the universal biological variables of AD, which include age, APOE genotype, and sex, are often overlooked. Age is the greatest risk factor for AD, while the ε4 allele of the human APOE gene, encoding apolipoprotein E, is the greatest genetic risk factor. Sex is the final universal biological variable of AD, as females develop AD at almost twice the rate of males and, importantly, female sex exacerbates the effects of APOE4 on AD risk and rate of cognitive decline. Therefore, this review evaluates the importance of context for understanding the role of APOE in preclinical mouse models. Specifically, we detail how human AD pathology is mirrored in current transgenic mouse models (“What”) and describe the critical need for introducing human APOE into these mouse models (“Who”). We next outline different methods for introducing human APOE into mice (“How”) and highlight efforts to develop temporally defined and location-specific human apoE expression models (“When” and “Where”). We conclude with the importance of choosing the human APOE mouse model relevant to the question being addressed, using the selection of transgenic models for testing apoE-targeted therapeutics as an example (“Why”).

Published

2020

2. Alzheimer's disease pathology in APOE transgenic mouse models: The Who, What, When, Where, Why, and How

Author

Mary Jo LaDu, Cutler T. Lewandowski, and Juan Maldonado Weng

Subjects

familial AD transgenic mice (FAD-Tg), 0301 basic medicine, Apolipoprotein E, Genetically modified mouse, Male, Pathology, medicine.medical_specialty, Genotype, Transgene, Apolipoprotein E4, Context (language use), Mice, Transgenic, Plaque, Amyloid, tau Proteins, Disease, Biology, Article, lcsh:RC321-571, 03 medical and health sciences, Mice, 0302 clinical medicine, Apolipoproteins E, Alzheimer Disease, medicine, Animals, Humans, Cognitive Dysfunction, Cognitive decline, Allele, Risk factor, Alzheimer's Disease (AD), lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Alleles, apolipoprotein E, Amyloid beta-Peptides, Reproducibility of Results, APOE4 and AD risk, sex and AD risk, Disease Models, Animal, 030104 developmental biology, Neurology, Female, 030217 neurology & neurosurgery, EFAD-Tg mouse model

Abstract

The focus on amyloid plaques and neurofibrillary tangles has yielded no Alzheimer’s disease (AD) modifying treatments in the past several decades, despite successful studies in preclinical mouse models. This inconsistency has caused a renewed focus on improving the fidelity and reliability of AD mouse models, with disparate views on how this improvement can be accomplished. However, the interactive effects of the universal biological variables of AD, which include age, APOE genotype, and sex, are often overlooked. Age is the greatest risk factor for AD, while the e4 allele of the human APOE gene, encoding apolipoprotein E, is the greatest genetic risk factor. Sex is the final universal biological variable of AD, as females develop AD at almost twice the rate of males and, importantly, female sex exacerbates the effects of APOE4 on AD risk and rate of cognitive decline. Therefore, this review evaluates the importance of context for understanding the role of APOE in preclinical mouse models. Specifically, we detail how human AD pathology is mirrored in current transgenic mouse models (“What”) and describe the critical need for introducing human APOE into these mouse models (“Who”). We next outline different methods for introducing human APOE into mice (“How”) and highlight efforts to develop temporally defined and location-specific human apoE expression models (“When” and “Where”). We conclude with the importance of choosing the human APOE mouse model relevant to the question being addressed, using the selection of transgenic models for testing apoE-targeted therapeutics as an example (“Why”).

Published

2019

3. Alzheimer's disease pathology in APOE transgenic mouse models: The Who, What, When, Where, Why, and How.

Author

Lewandowski, Cutler T., Maldonado Weng, Juan, and LaDu, Mary Jo

Subjects

*AMYLOID plaque, *ALZHEIMER'S disease, *TRANSGENIC mice, *PATHOLOGY, *APOLIPOPROTEIN E, *ANIMAL models in research

Abstract

The focus on amyloid plaques and neurofibrillary tangles has yielded no Alzheimer's disease (AD) modifying treatments in the past several decades, despite successful studies in preclinical mouse models. This inconsistency has caused a renewed focus on improving the fidelity and reliability of AD mouse models, with disparate views on how this improvement can be accomplished. However, the interactive effects of the universal biological variables of AD, which include age, APOE genotype, and sex, are often overlooked. Age is the greatest risk factor for AD, while the ε4 allele of the human APOE gene, encoding apolipoprotein E, is the greatest genetic risk factor. Sex is the final universal biological variable of AD, as females develop AD at almost twice the rate of males and, importantly, female sex exacerbates the effects of APOE4 on AD risk and rate of cognitive decline. Therefore, this review evaluates the importance of context for understanding the role of APOE in preclinical mouse models. Specifically, we detail how human AD pathology is mirrored in current transgenic mouse models ("What") and describe the critical need for introducing human APOE into these mouse models ("Who"). We next outline different methods for introducing human APOE into mice ("How") and highlight efforts to develop temporally defined and location-specific human apoE expression models ("When" and "Where"). We conclude with the importance of choosing the human APOE mouse model relevant to the question being addressed, using the selection of transgenic models for testing apoE-targeted therapeutics as an example ("Why"). Unlabelled Image • What: AD is uniquely human, but molecular mechanisms can be measured in Tg mice. • Who: A universal biological variable of AD, APOE is critical for preclinical models. • How: There are several strategies for developing APOE -Tg mice. • When/Where: Developmental and region-specific models probe apoE expression patterns. • Why: Therapeutic strategies targeting apoE can exploit the relevant mouse model(s). [ABSTRACT FROM AUTHOR]

Published

2020