Associations between brain microstructures, metabolites, and cognitive deficits during chronic HIV-1 infection of humanized mice

Boska, Michael D.; Dash, Prasanta K.; Knibbe, Jaclyn; Epstein, Adrian A.; Akhter, Sidra P.; Fields, Natasha; High, Robin; Makarov, Edward; Bonasera, Stephen J.; Gelbard, Harris A.; Poluektova, Larisa Y.; Gendelman, Howard Eliot; Gorantla, Santhi

doi:10.1186/1750-1326-9-58

Cited by 54 publications

(56 citation statements)

References 72 publications

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“…Our results also do not concur with the neuropathology seen in humanized HIV-1 mice which included robust inflammation reflected in GFAP and Iba-1 staining intensities (Boska, Dash, 2014, Dash, Gorantla, 2011, Epstein, Narayanasamy, 2013, Gorantla, Makarov, 2010). This however can be explained by the inherent differences between the two animal models as far as pathophysiology: the HIV humanized mouse is an immunodeficient model (NOD/scid-IL-2Rgamma(c)(null) mice) reconstituted with human hematopoietic CD34(+) stem cells and infected with HIV, thus reflecting human HIV-1 infection more closely, with persistent viremia, profound CD4+ T lymphocyte loss and infection of human monocyte-macrophages in the meninges/perivascular spaces of the rodent brain (Boska, Dash, 2014, Epstein, Narayanasamy, 2013).…”

Section: Discussioncontrasting

confidence: 99%

“…Engineering rodents that are permissive for HIV infection is technically demanding and only a few centers in the country have mastered the production and utilization of HIV-susceptible humanized mice (Akkina, 2013, Berges and Rowan, 2011, Boska et al, 2014, Dash et al, 2012, Dash et al, 2011, Epstein et al, 2013, Gorantla et al, 2010, Zhang and Su, 2012). Despite the usefulness of the latter, they remain technically complicated to produce and sustain (Akkina, 2013, Zhang and Su, 2012), and for our purposes of developing molecular imaging biomarkers, the small brain size of the humanized mouse poses a limitation especially when lower resolution techniques such as PET imaging are used.…”

Section: Discussionmentioning

confidence: 99%

“…This however can be explained by the inherent differences between the two animal models as far as pathophysiology: the HIV humanized mouse is an immunodeficient model (NOD/scid-IL-2Rgamma(c)(null) mice) reconstituted with human hematopoietic CD34(+) stem cells and infected with HIV, thus reflecting human HIV-1 infection more closely, with persistent viremia, profound CD4+ T lymphocyte loss and infection of human monocyte-macrophages in the meninges/perivascular spaces of the rodent brain (Boska, Dash, 2014, Epstein, Narayanasamy, 2013). The Tg rat on the other hand reflects chronic viral protein toxicity (Midde et al, 2011, Peng, Vigorito, 2010, Royal, Zhang, 2012, Vigorito et al, 2015, Wayman et al, 2015), and is closer pathologically to optimally-treated HIV+ patients than actively infected patients, as described below.…”

Section: Discussionmentioning

confidence: 99%

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Characterization of neuropathology in the HIV-1 transgenic rat at different ages

Reid

Ibrahim

Kim

et al. 2016

Journal of Neuroimmunology

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The transgenic HIV-1 rat (Tg) is a commonly used neuroHIV model with documented neurologic/behavioral deficits. Using immunofluorescent staining of the Tg brain, we found astrocytic dysfunction/damage, as well as dopaminergic neuronal loss/dysfunction, both of which worsening significantly in the striatum with age. We saw mild microglial activation in young Tg brains, but this decreased with age. There were no differences in neurogenesis potential suggesting a neurodegenerative rather than a neurodevelopmental process. Gp120 CSF levels exceeded serum gp120 levels in some animals, suggesting local viral protein production in the brain. Further probing of the pathophysiology underlying astrocytic injury in this model is warranted.

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Section: Discussioncontrasting

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Characterization of neuropathology in the HIV-1 transgenic rat at different ages

Reid

Ibrahim

Kim

et al. 2016

Journal of Neuroimmunology

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“…HIV infected mice had 2,063 HIV RNA copies/mL at two weeks post-infection and 67,400 HIV RNA copies/mL at three weeks post-infection. These data are consistent with previously published work (33–34). Two and three weeks post-HIV infection, the brains were harvested and T cells isolated by percoll gradient centrifugation.…”

Section: Resultssupporting

confidence: 94%

Migration of CD8+ T Cells into the Central Nervous System Gives Rise to Highly Potent Anti-HIV CD4dimCD8bright T Cells in a Wnt Signaling–Dependent Manner

Richards

Narasipura

Seaton

et al. 2016

The Journal of Immunology

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The role of CD8+ T cells in HIV control in the brain and the consequences of such control are unclear. Approximately 3% of peripheral CD8+ T cells dimly express CD4 on their surface. This population is known as CD4dimCD8bright T cells. We evaluated the role of CD4dimCD8bright and CD8 single positive T cells in HIV infected brain using NOD/SCID/IL-2rcγ−/− mice reconstituted with human Peripheral Blood Mononuclear Cells (PBMCs) (NSG-huPBMC). All three T cell populations (CD4 single positive, CD8 single positive, and CD4dimCD8bright) were found in NSG-huPBMC mice brain within 2 weeks of-infection. Wnts secreted from astrocytes induced CD4dimCD8bright T cells by 2-fold in vitro. Injection of highly purified CD8 single positive T cells into mouse brain induced CD4dimCD8bright T cells by 10-fold, which were proliferative and exhibited a terminally differentiated effector memory phenotype. Brain CD4dimCD8bright T cells from HIV infected mice exhibited anti-HIV specific responses, as demonstrated by induction of CD107ab post exposure to HIV-peptide loaded targets. Further, higher frequency of CD4dimCD8bright T cells (R= −0.62;p≤0.001), but not CD8 single positive T cells (R= −0.24;p≤0.27), negatively correlated with HIV-gag mRNA transcripts in HIV infected NSG-huPBMC brain. Together, these studies indicate that single positive CD8+ T cells entering the CNS during HIV infection can give rise to CD4dimCD8bright T cells, likely through a Wnt signaling-dependent manner, and that these cells are associated with potent anti-HIV control in the CNS. Thus, CD4dimCD8bright T cells are capable of HIV control in the CNS and may offer protection against HIV-Associated Neurocognitive Disorders.

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“…These human cells localize predominantly in the meninges and perivascular spaces and, to a lesser extent, in brain parenchyma 205,207 . Despite low viral burdens, chronically HIV-infected NSG-hCD34 + mice show several important characteristics of HAND, including activation of resident microglia and astrocytes in some brain regions, limited brain pathology in some mice, elevated markers of neuroinflammation, and evidence of neuronal injury and neurodegeneration, assessed with brain metabolite analysis and immunofluorescence staining 205–207 . Some of these changes were reversed by nanoparticle-based CART 208 .…”

Section: Animal Models Of Neuro-hivmentioning

confidence: 99%

HIV-associated neurocognitive disorder — pathogenesis and prospects for treatment

et al. 2016

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In the past two decades, several advancements have improved the care of HIV-infected individuals. Most importantly, the development and deployment of combination antiretroviral therapy (CART) has resulted in a dramatic decline in the rate of deaths from AIDS, so that people living with HIV today have nearly normal life expectancies if treated with CART. The term HIV-associated neurocognitive disorder (HAND) has been used to describe the spectrum of neurocognitive dysfunction associated with HIV infection. HIV can enter the CNS during early stages of infection, and persistent CNS HIV infection and inflammation probably contribute to the development of HAND. The brain can subsequently serve as a sanctuary for ongoing HIV replication, even when systemic viral suppression has been achieved. HAND can remain in patients treated with CART, and its effects on survival, quality of life and everyday functioning make it an important unresolved issue. In this Review, we describe the epidemiology of HAND, the evolving concepts of its neuropathogenesis, novel insights from animal models, and new approaches to treatment. We also discuss how inflammation is sustained in chronic HIV infection. Moreover, we suggest that adjunctive therapies -treatments targeting CNS inflammation and other metabolic processes, including glutamate homeostasis, lipid and energy metabolism -are needed to reverse or improve HAND-related neurological dysfunction. Competing interests statementThe authors declare no competing interests. HHS Public AccessAuthor manuscript Nat Rev Neurol. Author manuscript; available in PMC 2016 July 08. Author Manuscript Author ManuscriptAuthor ManuscriptAuthor Manuscript chronic infection that can be managed, is associated with a near-normal lifespan and in which opportunistic infections are rare 1 .The first major advancement was an understanding of the direct relationship between HIV replication and subsequent immunological and clinical progression. This finding emphasized the need to completely suppress HIV replication in order to control disease progression.The second major advancement was the development and deployment of combination antiretroviral therapy (CART), which can provide effective systemic suppression of HIV replication. The introduction of CART in the mid-1990s resulted in a 50% decline in the rate of death from AIDS, substantial decreases in rates of maternal-infant transmission, reduced incidence of opportunistic infections, and a 40-50% decrease in the incidence of HIVassociated dementia (HAD), which was previously common and is the most severe form of cognitive impairment associated with the infection 2 .The third major change in the care of HIV+ patients was the ability to monitor the efficacy of CART through the reliable and widespread measurement of CD4 + helper T cells, plasma HIV RNA levels and antiretroviral resistance profiles, all of which are now fully integrated into routine clinical care in the developed world and used to optimize treatment for individual patients. Plasma viral l...

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Associations between brain microstructures, metabolites, and cognitive deficits during chronic HIV-1 infection of humanized mice

Cited by 54 publications

References 72 publications

Characterization of neuropathology in the HIV-1 transgenic rat at different ages

Characterization of neuropathology in the HIV-1 transgenic rat at different ages

Migration of CD8+ T Cells into the Central Nervous System Gives Rise to Highly Potent Anti-HIV CD4dimCD8bright T Cells in a Wnt Signaling–Dependent Manner

HIV-associated neurocognitive disorder — pathogenesis and prospects for treatment

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