Apolipoprotein E ε4 genotype status is not associated with neuroimaging outcomes in a large cohort of HIV+ individuals

Cooley, Sarah; Paul, Robert; Fennema-Notestine, Christine; Morgan, Erin E.; Vaida, Florin; Deng, Qinqin; Chen, Jie Ashley; Letendre, Scott; Ellis, Ronald J.; Clifford, David B.; Marra, Christina M.; Collier, Ann C.; Gelman, Benjamin B.; McArthur, Justin C.; McCutchan, J. Allen; Simpson, David M.; Morgello, Susan; Grant, Igor; Ances, Beau M.

doi:10.1007/s13365-016-0434-7

Cited by 14 publications

(10 citation statements)

References 51 publications

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“…Analysis of CHARTER and MACS participants found no association of APOE status with development of cognitive impairment, or with imaging abnormalities in either structural or metabolic brain imaging. [38–40] A major reservation about these cohort analyses is the relatively young age, which might limit the power to detect APOE4 effects. In another recent report, while APOE4 was again not associated with HAND, it was associated with abnormal CSF-abeta42 levels, consistent with increased risk of developing AD with further aging.…”

Section: Biomarkers and Handmentioning

confidence: 99%

HIV-associated neurocognitive disorder

Clifford

2017

Current Opinion in Infectious Diseases

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Purpose of review HIV associated neurocognitive disease (HAND) is the most active topic for neuroAIDS investigations at present. Although impairment is mild in patients successfully treated with modern antiviral regimens, it remains an ongoing problem for HIV patients. It is important to update the emerging research concerning HAND. Recent findings The virus enters the brain during acute infection, with evidence for abnormal functioning that may occur early and often persists. Direct relationships with ongoing viral infection continue to be monitored, but chronic inflammation, often associated with monocytes and macrophages appear to be the most likely driver of cognitive dysfunction. Appreciation for cerebrovascular disease as a significant co-morbidity that is associated with cognitive deficits is increasing. Neuroimaging is actively being developed to address detection and measurement of changes in the brain. Optimal cART therapy has vastly improved neurologic outcomes, but so far has not been demonstrated to reverse the remaining mild impairment. Inflammatory and vascular mechanisms of cerebral dysfunction may need to be addressed to achieve better outcomes. Summary Ongoing research is required to improve neurological outcomes for persons living with HIV. It is likely that interventions beyond antiviral approaches will be required to control or reverse HAND.

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Section: Biomarkers and Handmentioning

confidence: 99%

HIV-associated neurocognitive disorder

Clifford

2017

Current Opinion in Infectious Diseases

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“…Our understanding of amyloid metabolism during HIV-1 infection is further clouded by conflicting reports on the association between HAND development and Apolipoprotein E (ApoE) expression, which is a significant risk factor for abnormal amyloid deposition resulting in sporadic AD development (Kim et al, 2009;Morris et al, 2010). While some early reports demonstrate increased frequencies of HAD development in ApoE carriers, more recent studies do not find a correlation between ApoE phenotype and HAND development characterized by either neurocognitive impairments or detrimental neuroimaging outcomes (Burt et al, 2008;Cooley et al, 2016;Corder et al, 1998;Morgan et al, 2013;Valcour et al, 2004b). These differential results could be due to disparities in stages of neurocognitive impairments examined (HAD vs. milder forms of HAND) or in ages of study subjects since ApoE was shown to be an independent risk factor for HAD in HIV-infected patients who are 50 year of age and older, but not in younger subjects (Valcour et al, 2004a).…”

Section: Hiv-1 Infection Affects Cellular Metabolism In Microgliamentioning

confidence: 99%

Fate of microglia during HIV‐1 infection: From activation to senescence?

Chen

Partridge

Sell

et al. 2016

Glia

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Microglia support productive human immunodeficiency virus type 1 (HIV-1) infection and disturbed microglial function could contribute to the development of HIV-associated neurocognitive disorders (HAND). Better understanding of how HIV-1 infection and viral protein exposure modulate microglial function during the course of infection could lead to the identification of novel therapeutic targets for both the eradication of HIV-1 reservoir and treatment of neurocognitive deficits. This review first describes microglial origins and function in the normal central nervous system (CNS), and the changes that occur during aging. We then critically discuss how HIV-1 infection and exposure to viral proteins such as Tat and gp120 affect various aspects of microglial homeostasis including activation, cellular metabolism and cell cycle regulation, through pathways implicated in cellular stress responses including p38 mitogen-activated protein kinase (MAPK) and nuclear factor κB (NF-κB). We thus propose that the functions of human microglia evolve during both healthy and pathological aging. Aging-associated dysfunction of microglia comprises phenotypes resembling cellular senescence, which could contribute to cognitive impairments observed in various neurodegenerative diseases. In addition, microglia seem to develop characteristics that could be related to cellular senescence post-HIV-1 infection and after exposure to HIV-1 viral proteins. However, despite its potential role as a component of HAND and likely other neurocognitive disorders, microglia senescence has not been well characterized and should be the focus of future studies, which could have high translational relevance.

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“…One such report from the CHARTER group (mean age = 40 years, 25% over age 50 years) finds no difference in HAND prevalence between ApoE ε4 carriers and non-carriers nor did they identify neuroimaging differences by carrier status. 19,20 Similarly, investigations from the Multicenter AIDS Cohort Study (MACS, with mean ages at enrollment across groups between 30 to 40 years) do not identify an impact of ApoE ε4 on development of cognitive impairment among participants who tested normal at baseline. 21 One group carefully tested the hypothesis that age may influence the association between ApoE ε4 carrier status and cognitive outcomes using data from the National NeuroAIDS Tissue Consortium (NNTC) noting detrimental effects on HAND diagnosis, executive functioning and information processing in older age (> 50 years) but not in those of younger age.…”

Section: Introductionmentioning

confidence: 99%

ApoE ε4 Is Associated With Cognition, Brain Integrity, and Atrophy in HIV Over Age 60

Wendelken

Jahanshad

Rosen

et al. 2016

JAIDS Journal of Acquired Immune Deficiency Syndromes

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BACKGROUND There are contradicting reports on the associations between Apolipoprotein E4 (ApoE ε4) and brain outcomes in HIV with some evidence that relationships may be greatest in older age groups. METHODS We assessed cognition in 76 clinically stable HIV-infected participants over age 60 and genotyped ApoE. Sixty-one of these subjects underwent structural brain MRI and diffusion tensor imaging (DTI). RESULTS The median age of the participants was 64 years (range: 60–84) and the median estimated duration of HIV infection was 22 years. Apo ε4 carriers (n=19) were similar to non-carriers (n=57) in sex (95% vs. 96% male), and education (16.0 vs. 16.2 years) ApoE ε4 carriers demonstrated greater deficits in cognitive performance in the executive domain (p=0.045) and had reduced fractional anisotropy (FA) and increased mean diffusivity (MD) throughout large white matter tracts within the brain compared to non-carriers. Tensor Based Morphometry (TBM) analyses revealed ventricular expansion and atrophy in the posterior corpus callosum, thalamus, and brainstem among HIV-infected ApoE ε4 carriers compared to ε4-non-carriers. CONCLUSION In this sample of older HIV-infected individuals, having at least one ApoE ε4 allele was associated with decreased cognitive performance in the executive functioning domain, reduced brain white matter integrity, and brain atrophy. Brain atrophy was most prominent in the posterior corpus callosum, thalamus and brainstem. This pattern of cognitive deficit, atrophy and damage to white matter integrity was similar to that described in HIV, suggesting an exacerbation of HIV-related pathology; although emergence of other age-associated neurodegenerative disorders cannot be excluded.

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Apolipoprotein E ε4 genotype status is not associated with neuroimaging outcomes in a large cohort of HIV+ individuals

Cited by 14 publications

References 51 publications

HIV-associated neurocognitive disorder

HIV-associated neurocognitive disorder

Fate of microglia during HIV‐1 infection: From activation to senescence?

ApoE ε4 Is Associated With Cognition, Brain Integrity, and Atrophy in HIV Over Age 60

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