Glial-restricted precursors: Patterns of expression of opioid receptors and relationship to human immunodeficiency virus-1 Tat and morphine susceptibility in vitro

Buch, Shreya; Khurdayan, Valeriya K.; Lutz, Sarah E.; Knapp, Pamela E.; El‐Hage, Nazira; Hauser, Kurt F.

doi:10.1016/j.neuroscience.2007.03.006

Cited by 24 publications

(25 citation statements)

References 76 publications

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“…Cytotoxicity after prolonged morphine or Tat exposure has been previously demonstrated in vitro in glial-restricted precursors isolated from spinal cord (Buch et al, 2007). Interestingly, Tat did not affect tolerance to the effects of morphine in the locomotor activity assay, suggesting that Tat does not interact with morphine's actions at supraspinal sites governing locomotor activity including the striatum.…”

Section: Discussionmentioning

confidence: 81%

Morphine Tolerance and Physical Dependence Are Altered in Conditional HIV-1 Tat Transgenic Mice

Fitting

Stevens

Khan

et al. 2015

Journal of Pharmacology and Experimental Therapeutics

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Despite considerable evidence that chronic opiate use selectively affects the pathophysiologic consequences of human immunodeficiency virus type 1 (HIV-1) infection in the nervous system, few studies have examined whether neuro-acquired immune deficiency syndrome (neuroAIDS) might intrinsically alter the pharmacologic responses to chronic opiate exposure. This is an important matter because HIV-1 and opiate abuse are interrelated epidemics, and HIV-1 patients are often prescribed opiates as a treatment of HIV-1-related neuropathic pain. Tolerance and physical dependence are inevitable consequences of frequent and repeated administration of morphine. In the present study, mice expressing HIV-1 Tat in a doxycycline (DOX)-inducible manner [Tat(1)], their Tat(2) controls, and control C57BL/6 mice were chronically exposed to placebo or 75-mg morphine pellets to explore the effects of Tat induction on morphine tolerance and dependence. Antinociceptive tolerance and locomotor activity tolerance were assessed using tail-flick and locomotor activity assays, respectively, and physical dependence was measured with the platform-jumping assay and recording of other withdrawal signs. We found that Tat(1) mice treated with DOX [Tat(1)/DOX] developed an increased tolerance in the tail-flick assay compared with control Tat(2)/DOX and/or C57/DOX mice. Equivalent tolerance was developed in all mice when assessed by locomotor activity. Further, Tat(1)/DOX mice expressed reduced levels of physical dependence to chronic morphine exposure after a 1-mg/kg naloxone challenge compared with control Tat(2)/DOX and/or C57/DOX mice. Assuming the results seen in Tat transgenic mice can be generalized to neuroAIDS, our findings suggest that HIV-1-infected individuals may display heightened analgesic tolerance to similar doses of opiates compared with uninfected individuals and show fewer symptoms of physical dependence.

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Section: Discussionmentioning

confidence: 81%

Morphine Tolerance and Physical Dependence Are Altered in Conditional HIV-1 Tat Transgenic Mice

Fitting

Stevens

Khan

et al. 2015

Journal of Pharmacology and Experimental Therapeutics

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“…After 5 d, cells were treated with Tat 1-86 (Clade B; 100 nM; ImmunoDiagnostics, Woburn, MA), ± morphine sulphate (500 nM; NIDA Drug Supply System, Rockville, MD), ± naloxone (1.5 μM; Sigma-Aldrich) for 12–48 h. Morphine, the major bioactive product of heroin in the brain, is a potent mu-opioid receptor (MOR) agonist; naloxone is a broad spectrum opioid receptor antagonist. These concentrations of Tat 1-86 and morphine have been established to elicit functional effects in glia and CNS progenitors in earlier studies (Buch et al 2007; El-Hage et al 2005; Hauser et al 2009; Khurdayan et al 2004). Naloxone was applied 30 min prior to other treatments, which were added simultaneously in pre-warmed medium.…”

Section: Methodsmentioning

confidence: 99%

“…Several studies suggest that CNS neural progenitor cells (NPCs), the undifferentiated precursors of both neurons and glia, are also susceptible to HIV-1 infection (Lawrence et al 2004; Rothenaigner et al 2007; Schwartz et al 2007). Even if NPCs are not readily infected, they may be affected by HIV-1 proteins directly (Buch et al 2007; Hahn et al 2010; Krathwohl and Kaiser 2004; Lee et al 2011; Mishra et al 2010; Okamoto et al 2007; Peng et al 2008), or secondarily by extracellular changes. NPCs are widely distributed in germinative zones during development.…”

Section: Introductionmentioning

confidence: 99%

“…NPCs and glial progenitors express functional opioid receptors in adult and neonatal rodent and human CNS (Buch et al 2007; Hauser et al 2009; Persson et al 2003; Reznikov et al 1999; Rius et al 1991; Tripathi et al 2008). Since co-exposure to opiate drugs of abuse enhances HIV-related CNS deficits in patients and experimental models (Anthony and Bell 2008; Bell et al 2006; Burdo et al 2006; Byrd et al 2011; Hauser et al 2007; Kopnisky et al 2007), we examined interactive opiate effects.…”

Section: Introductionmentioning

confidence: 99%

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HIV‐1 alters neural and glial progenitor cell dynamics in the central nervous system: Coordinated response to opiates during maturation

Hahn

Podhaizer

Hauser

et al. 2012

Glia

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HIV-associated neurocognitive disorders (HAND) are common sequelae of HIV infection, even when viral titers are well controlled by anti-retroviral therapy. Evidence in patients and animal models suggests that neurologic deficits are increased during chronic opiate exposure. We have hypothesized that CNS progenitor cells in both adult and developing CNS are affected by HIV infection, and that opiates exacerbate these effects. To examine this question, neural progenitors were exposed to HIV-1 Tat1-86 in the developing brain of inducible transgenic mice and in vitro. We examined whether Tat affected the proliferation or balance of progenitor populations expressing nestin, Sox2, and Olig2. Disease relevance was further tested by exposing human-derived progenitors to supernatant from HIV-1 infected monocytes. Studies concentrated on striatum, a region preferentially targeted by HIV and opiates. Results were similar among experimental paradigms. Tat or HIV exposure reduced the proliferation of undifferentiated (Sox2+) progenitors and oligodendroglial (Olig2+) progenitors. Co-exposure to morphine exacerbated the effects of Tat or HIV-1SF162 supernatant, but partially reversed HIV-1IIIB supernatant effects. Populations of Sox2+ and Olig2+ cells were also reduced by Tat exposure, although progenitor survival was unaffected. In rare instances, p24 immunolabeling was detected in viable human progenitors by confocal imaging. The vulnerability of progenitors is likely to distort the dynamic balance among neuron/glial populations as the brain matures, perhaps contributing to reports that neurologic disease is especially prevalent in pediatric HIV patients. Pediatric disease is atypical in developed regions, but remains a serious concern in resource-limited areas where infection occurs commonly at birth and through breast-feeding.

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“…Moreover, Tat-induced increases in inflammatory cytokines can intrinsically affect expression of opioid peptides and receptors in isolated astrocytes, 74 -76 leukocytes, [77][78][79] and in macrophages/microglia. 80,81 Importantly, such effects may not be restricted to Tat since gp120 and intact virions, can also alter opioid signaling through multiple mechanisms. 82 Thus, the response of the opioid system to HIV-1 infection is not restricted to a particular brain region, peptide family or receptor.…”

Section: Chronic Hiv-1 Tat Disrupts the Endogenous Opioid Systemmentioning

confidence: 99%

Interactive Comorbidity between Opioid Drug Abuse and HIV-1 Tat

Fitting

Bull

et al. 2010

The American Journal of Pathology

129

106

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HIV-1 infection predisposes the central nervous system to damage by opportunistic infections and environmental insults. Such maladaptive plasticity may underlie the exaggerated comorbidity seen with HIV-1 infection and opioid abuse. Although morphine and HIV-1 Tat synergize at high concentrations to increase neuronal death in vitro, we questioned whether chronic low Tat exposure in vivo might contribute to the spectrum of neuropathology through sublethal neuronal injury. We used a doxycycline-driven, inducible, HIV-1 Tat transgenic mouse, in which striatal neuron death was previously shown to be absent, to examine effects of differential Tat expression, alone and combined with morphine. Low constitutive Tat expression caused neurodegeneration; higher levels induced by 7 days of doxycycline significantly reduced dendritic spine numbers. Moreover, Tat expression widely disrupted the endogenous opioid system, altering and , but not ␦, opioid receptor and proopiomelanocortin, proenkephalin, and prodynorphin transcript levels in cortex, hippocampus, and striatum. In addition to markedly reducing spine density by itself, morphine amplified the effect of higher levels of Tat on spines, and also potentiated Tat-mediated dendritic pathology, thus contributing to maladaptive neuroplasticity at multiple levels. The dendritic pathology and reductions in spine density suggest that sustained Tat ؎ morphine exposure un- Exposure to HIV results in neurodegenerative alterations in the central nervous system (CNS) of a substantial proportion of patients, even in the era of highly active anti-retroviral therapy. Highly active anti-retroviral therapy does not readily cross the blood-brain barrier, making the CNS a safe-haven for infection, and permitting ongoing degenerative changes even when viral titers are quite low in the periphery. [1][2][3][4][5][6] There is considerable evidence, both in patients and in experimental models, that coexposure to abused opiate drugs can hasten the onset and worsen the outcome of HIV encephalitis and other neurodegenerative changes.7-15 A more limited number of studies show that opioids increase viral loads, and hasten disease progression and/or neuropathology in simian immunodeficiency models, 16 -19 although this has been controversial. 20 -22 Our in vitro work has consistently shown evidence for interactions between Tat or gp120 and morphine that accelerate neurodegeneration. These interactive effects appear to be orchestrated by glial cells, 23 and likely involve synergistic upregulation of proinflammatory chemokine/cytokine release and production of reactive species. 24 -26 The present work was undertaken to extend previous results suggesting that HIV-1 Tat exposure might disrupt endogenous opioid and chemokine signaling.

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Glial-restricted precursors: Patterns of expression of opioid receptors and relationship to human immunodeficiency virus-1 Tat and morphine susceptibility in vitro

Cited by 24 publications

References 76 publications

Morphine Tolerance and Physical Dependence Are Altered in Conditional HIV-1 Tat Transgenic Mice

Morphine Tolerance and Physical Dependence Are Altered in Conditional HIV-1 Tat Transgenic Mice

HIV‐1 alters neural and glial progenitor cell dynamics in the central nervous system: Coordinated response to opiates during maturation

Interactive Comorbidity between Opioid Drug Abuse and HIV-1 Tat

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