Abstract

The experiments below are designed to address the relationship between the SIV and METH in the induction of alterations in CNS function. We hypothesize that METH and HIV induce convergent cellular processes in the CNS to induce neuropathogenesis. During the life and at autopsy, we have chosen measures to examine these processes and the changes they produce. Since viral load has significant consequences on the course of AIDS and likely neuroAIDS, we will assess virus in the periphery and CNS, as well as determining the CTL response, critical in controlling viral load. Since METH is known to affect neurons and monoamine neurotransmitter systems in the striatum, quantification of neurons and neurochemicals will assess our hypothesis that SIV synergizes with METH in inducing damage to the CNS.
In Aim 1, we hypothesize that METH administration surrounding the early phase of SIV infection will lead to increased damage to the CNS and effects on the crucial viral-host interaction setting the course of disease. Since the CNS itself is both infected and affected early following inoculation, changes occurring during the acute injection period may dramatically alter CNS disease. METH administration is predicted to lead to more profound, or quicker development of, SIV-induced abnormalities. During life, a longitudinal study of selected electrophysiological, physiological, behavioral, viral, monoamine metabolite and immune parameters will be performed.
This aim will model an active METH user who becomes HIV infected.
In Aim 2, we hypothesize that METH administration in the setting of chronic injection can work through numerous mechanisms to augment the CNS deficits induced by SIV infection. Among these are making the CNS more susceptible to damage through neurotoxic effects, affecting viral replication kinetics, or altering immune cell trafficking to the CNS. Here we will treat with METH for two periods following stable establishment of SIV infection. In this manner we will model an HIV-infected individual who uses METH. The first period of METH administration will allow us to determine the effects of measures of physiology, CNS function, and viral/host interactions. The second will allow the same determinations for repeat METH use, and CNS tissue analysis at the end of the second METH period will allow direct examination of the pathological consequences of recent METH use, in the setting of SIV injection and a history of METH use.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Program Projects (P01)
Project #
1P01DA012444-01A1
Application #
6359884
Study Section
Special Emphasis Panel (ZDA1-RXL-E (16))
Project Start
2000-09-30
Project End
2005-05-31
Budget Start
Budget End
Support Year
1
Fiscal Year
2000
Total Cost
$350,741
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Huitron-Resendiz, Salvador; Henriksen, Steven J; Barr, Margaret C et al. (2010) Methamphetamine and lentivirus interactions: reciprocal enhancement of central nervous system disease. J Neurovirol 16:268-78
Sanchez-Alavez, Manuel; Conti, Bruno; Moroncini, Gianluca et al. (2007) Contributions of neuronal prion protein on sleep recovery and stress response following sleep deprivation. Brain Res 1158:71-80
Persidsky, Yuri; Fox, Howard (2007) Battle of animal models. J Neuroimmune Pharmacol 2:171-7
Milner, Richard; Campbell, Iain L (2006) Increased expression of the beta4 and alpha5 integrin subunits in cerebral blood vessels of transgenic mice chronically producing the pro-inflammatory cytokines IL-6 or IFN-alpha in the central nervous system. Mol Cell Neurosci 33:429-40
Criado, Jose R; Sanchez-Alavez, Manuel; Conti, Bruno et al. (2005) Mice devoid of prion protein have cognitive deficits that are rescued by reconstitution of PrP in neurons. Neurobiol Dis 19:255-65
Madden, Lisa J; Flynn, Claudia T; Zandonatti, Michelle A et al. (2005) Modeling human methamphetamine exposure in nonhuman primates: chronic dosing in the rhesus macaque leads to behavioral and physiological abnormalities. Neuropsychopharmacology 30:350-9
Balosso, Silvia; Ravizza, Teresa; Perego, Carlo et al. (2005) Tumor necrosis factor-alpha inhibits seizures in mice via p75 receptors. Ann Neurol 57:804-12
Huitron-Resendiz, Salvador; Kristensen, Morten P; Sanchez-Alavez, Manuel et al. (2005) Urotensin II modulates rapid eye movement sleep through activation of brainstem cholinergic neurons. J Neurosci 25:5465-74
Vlkolinsky, Roman; Siggins, George R; Campbell, Iain L et al. (2004) Acute exposure to CXC chemokine ligand 10, but not its chronic astroglial production, alters synaptic plasticity in mouse hippocampal slices. J Neuroimmunol 150:37-47
Crocker, Stephen J; Pagenstecher, Axel; Campbell, Iain L (2004) The TIMPs tango with MMPs and more in the central nervous system. J Neurosci Res 75:1-11

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