Epidermal growth factor treatment of female mice that express APOE4 at an age of advanced pathology mitigates behavioral and cerebrovascular dysfunction

Zaldua, Steve; Damen, Frederick W.; Pisharody, Rohan; Thomas, Riya; Fan, Kelly; Ekkurthi, Giri K.; Scheinman, Sarah B.; Alahmadi, Sami; Marottoli, Felecia M.; Alford, Simon; Cai, Kejia; Tai, Leon M.

doi:10.1016/j.heliyon.2020.e03919

Cited by 11 publications

(13 citation statements)

References 77 publications

(139 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Therefore, E4FAD− and E4FAD+ mice were utilized to test whether candesartan modulates functions specific to the interaction of Aβ and APOE4 or were generally applicable to APOE4 . Previous research in E4FAD− and E4FAD+ mice has demonstrated that alterations in behavior and neuronal protein levels occurs earlier in female mice (∼6 months) than in male mice (∼8 months) ( Wolf et al, 2013 ; Thomas et al, 2016 , 2017 ; Tai et al, 2017 ; Zaldua et al, 2020 ). Therefore, candesartan treatments were initiated at different ages for female and male E4FAD mice to try and broadly match AD-relevant pathology at the start of treatment.…”

Section: Resultsmentioning

confidence: 96%

“…Further, although the AT1 receptor is expressed on brain endothelial cells and excessive AT1 receptor signaling has been shown to directly impair endothelial cell function ( Fleegal-DeMotta et al, 2009 ), in our study candesartan treatment did not result in changes to vascular permeability (fibrinogen) in female E4FAD− and E4FAD+ mice. Therefore, blood-brain barrier dysfunction may be too far advanced in E4FAD mice at the ages evaluated in this study ( Thomas et al, 2016 , 2017 ; Zaldua et al, 2020 ) for candesartan to have exerted a beneficial effect, or the contribution of the AT1 receptor to cerebrovascular dysfunction is minimal in E4FAD mice. For either event, the result may be that a disrupted blood-brain barrier in E4FAD mice enabled candesartan to cross into the brain.…”

Section: Discussionmentioning

confidence: 94%

“…E4FAD− mice express the human APOE4 gene under the endogenous mouse promoter, and E4FAD+ mice express the human APOE4 gene and overproduce human Aβ42 through the expression of 5xFAD autosomal dominant mutations. APOE4 is associated with age-dependent changes in behavior and neuronal function in the absence of high levels of human Aβ in vivo , including in E4FAD− mice ( Wolf et al, 2013 ; Thomas et al, 2016 , 2017 ; Zaldua et al, 2020 ). Therefore, E4FAD− and E4FAD+ mice were utilized to test whether candesartan modulates functions specific to the interaction of Aβ and APOE4 or were generally applicable to APOE4 .…”

Section: Resultsmentioning

confidence: 99%

“…Impaired memory-relevant behavior with APOE4 has been reported both in the presence and absence of Aβ in vivo ( Thomas et al, 2016 , 2017 ; Zaldua et al, 2020 ), and data are conflicting on whether ARB treatment considerably modulates memory-relevant behavior in AD-relevant mouse models ( Wang et al, 2007 ; Mogi et al, 2008 ; Takeda et al, 2009 ; Tsukuda et al, 2009 ; Danielyan et al, 2010 ; Ferrington et al, 2011 , 2012 ; Ongali et al, 2014 , 2016 ; Torika et al, 2016 , 2017 , 2018 ; Royea et al, 2017 ; Trigiani et al, 2018 ). Therefore, one of our goals was to evaluate whether candesartan treatment could modulate memory-relevant behavior in E4FAD− and E4FAD+ mice.…”

Section: Resultsmentioning

confidence: 99%

“…APOE can modulate neuronal function in the brain through a number of direct or indirect pathways both in the absence ( Wolf et al, 2013 ) and presence ( Carter, 2005 ; Ye et al, 2005 ; Tai et al, 2015 ) of Aβ. In vivo models have identified that APOE4 is associated with memory-relevant behavioral deficits ( Bour et al, 2008 ; Liu et al, 2015 ), greater neuroinflammation ( Guo et al, 2004 ), higher Aβ levels ( LaDu et al, 1994 ; Ye et al, 2005 ; Youmans et al, 2012 ; Tai et al, 2013 , 2014b ; Lewandowski et al, 2020 ), and more severe cerebrovascular dysfunction ( Thomas et al, 2016 , 2017 ; Zaldua et al, 2020 ), compared to APOE3 . As described above, these are the same functions and pathologies purported to be altered by ARB treatment in mouse models expressing familial AD (FAD) mutations.…”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

Systemic Candesartan Treatment Modulates Behavior, Synaptic Protein Levels, and Neuroinflammation in Female Mice That Express Human APOE4

et al. 2021

Self Cite

View full text Add to dashboard Cite

Evidence suggests that angiotensin receptor blockers (ARBs) could be beneficial for Alzheimer’s disease (AD) patients independent of any effects on hypertension. However, studies in rodent models directly testing the activity of ARB treatment on behavior and AD-relevent pathology including neuroinflammation, Aβ levels, and cerebrovascular function, have produced mixed results. APOE4 is a major genetic risk factor for AD and has been linked to many of the same functions as those purported to be modulated by ARB treatment. Therefore, evaluating the effects of ARB treatment on behavior and AD-relevant pathology in mice that express human APOE4 could provide important information on whether to further develop ARBs for AD therapy. In this study, we treated female and male mice that express the human APOE4 gene in the absence (E4FAD−) or presence (E4FAD+) of high Aβ levels with the ARB prodrug candesartan cilexetil for a duration of 4 months. Compared to vehicle, candesartan treatment resulted in greater memory-relevant behavior and higher hippocampal presynaptic protein levels in female, but not male, E4FAD− and E4FAD+ mice. The beneficial effects of candesartan in female E4FAD− and E4FAD+ mice occurred in tandem with lower GFAP and Iba1 levels in the hippocampus, whereas there were no effects on markers of cerebrovascular function and Aβ levels. Collectively, these data imply that the effects of ARBs on AD-relevant pathology may be modulated in part by the interaction between APOE genotype and biological sex. Thus, the further development of ARBs could provide therapeutic options for targeting neuroinflammation in female APOE4 carriers.

show abstract

Section: Resultsmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 94%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Systemic Candesartan Treatment Modulates Behavior, Synaptic Protein Levels, and Neuroinflammation in Female Mice That Express Human APOE4

et al. 2021

Self Cite

View full text Add to dashboard Cite

show abstract

Higher Neuronal Facilitation and Potentiation with APOE4 Suppressed by Angiotensin II

Scheinman,

Tseng,

Alford

et al. 2023

Mol Neurobiol

Self Cite

View full text Add to dashboard Cite

Progressive hippocampal degeneration is a key component of Alzheimer's disease (AD) progression.Therefore, identifying how hippocampal neuronal function is modulated early in AD is an important approach to eventually prevent degeneration. AD-risk factors and signaling molecules likely modulate neuronal function, including APOE genotype and angiotensin II. Compared to APOE3, APOE4 increases AD risk up to 12-fold, and high levels of angiotensin II are hypothesized to disrupt neuronal function in AD. However, the extent that APOE and angiotensin II modulates the hippocampal neuronal phenotype in AD-relevant models is unknown. To address this issue, we used electrophysiological techniques to assess the impact of APOE genotype and angiotensin II on basal synaptic transmission, presynaptic and postsynaptic activity in mice that express human APOE3 (E3FAD) or APOE4 (E4FAD) and overproduce Aβ. We found that compared to E3FAD mice, E4FAD mice had lower basal synaptic activity, but higher levels of paired pulse facilitation (PPF) and Long-Term Potentiation (LTP) in the Schaffer Collateral Commissural Pathway (SCCP) of the hippocampus. We also found that exogenous angiotensin II has a profound inhibitory effect on hippocampal LTP in both E3FAD and E4FAD mice. Collectively, our data suggests that APOE4 and Aβ are associated with a hippocampal phenotype comprised of lower basal activity and higher responses to high frequency stimulation, the latter of which is suppressed by angiotensin II. These novel data suggest a potential mechanistic link between hippocampal activity, APOE4 genotype and angiotensin II in AD.

show abstract

Apolipoprotein E polymorphisms and female fertility in a transgenic mouse model of Alzheimer’s disease

Medegan Fagla,

York,

Christensen

et al. 2024

Sci Rep

View full text Add to dashboard Cite

Apolipoprotein E (APOE) is a major cholesterol carrier responsible for lipid transport and injury repair in the brain. The human APOE gene (h-APOE) has 3 naturally occurring alleles: ε3, the common allele; ε4, which increases Alzheimer’s disease (AD) risk up to 15-fold; and ε2, the rare allele which protects against AD. Although APOE4 has negative effects on neurocognition in old age, its persistence in the population suggests a survival advantage. We investigated the relationship between APOE genotypes and fertility in EFAD mice, a transgenic mouse model expressing h-APOE. We show that APOE4 transgenic mice had the highest level of reproductive performance, followed by APOE3 and APOE2. Intriguingly, APOE3 pregnancies had more fetal resorptions and reduced fetal weights relative to APOE4 pregnancies. In conclusion, APOE genotypes impact fertility and pregnancy outcomes in female mice, in concordance with findings in human populations. These mouse models may help elucidate how h-APOE4 promotes reproductive fitness at the cost of AD in later life.

show abstract

Epidermal growth factor treatment of female mice that express APOE4 at an age of advanced pathology mitigates behavioral and cerebrovascular dysfunction

Cited by 11 publications

References 77 publications

Systemic Candesartan Treatment Modulates Behavior, Synaptic Protein Levels, and Neuroinflammation in Female Mice That Express Human APOE4

Systemic Candesartan Treatment Modulates Behavior, Synaptic Protein Levels, and Neuroinflammation in Female Mice That Express Human APOE4

Higher Neuronal Facilitation and Potentiation with APOE4 Suppressed by Angiotensin II

Apolipoprotein E polymorphisms and female fertility in a transgenic mouse model of Alzheimer’s disease

Contact Info

Product

Resources

About