Mechanism of HIV-1 Tat Potentiation of Methamphetamine Neurotoxicity

HIV-1 Tat 增强甲基苯丙胺神经毒性的机制

基本信息

项目摘要

DESCRIPTION (provided by applicant): In the central nervous system, basal ganglia structures are highly susceptible to infection with the human immunodeficiency virus-1 (HIV). The HIV-1 protein, Tat, which is involved in viral replication, also plays an important role in the neuronal injury and recapitulates much the pathology seen in HIV-1 infection of the brain. Patients with HIV-1 infection often abuse drugs such as methamphetamine, a drug that is well known to also cause long-term structural and functional changes of the basal ganglia. Previous studies from our laboratory have demonstrated that Tat protein and methamphetamine interacted synergistically to cause profound damage to the basal ganglia dopaminergic neurotransmitter system. Although our earlier studies implicated reactive oxygen species and the cytokine TNF-1, our preliminary data strongly suggest that ceramide-induced alterations of the vesicular monoamine transporter may play a prominent role in the enhanced toxicity of MA seen after exposure to Tat. In this proposal, we will in Specific Aim 1, determine whether HIV-1 Tat alters the compartmentalization of DA in the synaptic terminal. In Specific Aim 2, we will investigate whether the production of the second messenger ceramide is involved in Tat-induced changes in dopamine compartmentalization. Lastly, in Specific Aim 3, we will determine whether ceramide mediates the synergism between Tat and methamphetamine. Both pharmacological and genetic inhibition of ceramide synthesis will be pursued. In studying these interactions, we will examine 1) vesicular mononamine transporter function, 2) dopamine release (vesicular and tissue) 3) dopamine terminal integrity and 4) behavioral measures. The results of these experiments will elucidate a novel role for ceramide signaling in dopaminergic dysfunction, not only in HIV-1, but also in the neuronal injury associated with Parkinson's disease.
描述(由申请人提供): 在中枢神经系统中,基底神经节结构对人类免疫缺陷病毒-1(HIV)的感染高度敏感。参与病毒复制的HIV-1蛋白达特在神经元损伤中也起重要作用,并再现了在HIV-1感染脑中所见的许多病理学。HIV-1感染患者经常滥用药物,如甲基苯丙胺,众所周知,这种药物也会导致基底神经节的长期结构和功能变化。本实验室先前的研究已经证明,达特蛋白和甲基苯丙胺协同作用,对基底神经节多巴胺能神经递质系统造成严重损害。虽然我们早期的研究涉及活性氧和细胞因子TNF-1,我们的初步数据强烈表明,神经酰胺诱导的囊泡单胺转运蛋白的改变可能在暴露于达特后观察到的MA毒性增强中发挥重要作用。在这个提议中,我们将在具体目标1中,确定HIV-1达特是否改变了突触末端DA的区室化。在具体目标2中,我们将研究第二信使神经酰胺的产生是否参与了Tat诱导的多巴胺区室化变化。最后,在具体目标3中,我们将确定神经酰胺是否介导达特和甲基苯丙胺之间的协同作用。神经酰胺合成的药理学和遗传学抑制将被追求。在研究这些相互作用时,我们将检查1)囊泡单胺转运蛋白功能,2)多巴胺释放(囊泡和组织)3)多巴胺末端完整性和4)行为测量。这些实验的结果将阐明神经酰胺信号在多巴胺能功能障碍中的新作用,不仅在HIV-1中,而且在与帕金森病相关的神经元损伤中。

项目成果

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William F Maragos其他文献

William F Maragos的其他文献

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{{ truncateString('William F Maragos', 18)}}的其他基金

Mechanism of HIV-1 Tat Potentiation of Methamphetamine Neurotoxicity
HIV-1 Tat 增强甲基苯丙胺神经毒性的机制
  • 批准号:
    8243903
  • 财政年份:
    2012
  • 资助金额:
    --
  • 项目类别:
Mechanism of HIV-1 Tat Potentiation of Methamphetamine Neurotoxicity
HIV-1 Tat 增强甲基苯丙胺神经毒性的机制
  • 批准号:
    8762412
  • 财政年份:
    2012
  • 资助金额:
    --
  • 项目类别:
METHAMPHETAMINE AND HIV PROTEIN-INDUCED NEUROTOXICITY
甲基苯丙胺和 HIV 蛋白引起的神经毒性
  • 批准号:
    6841603
  • 财政年份:
    2001
  • 资助金额:
    --
  • 项目类别:
Dopamine Toxicity in Models of Huntington's Disease
亨廷顿病模型中的多巴胺毒性
  • 批准号:
    6603360
  • 财政年份:
    2001
  • 资助金额:
    --
  • 项目类别:
Dopamine Toxicity in Models of Huntington's Disease
亨廷顿病模型中的多巴胺毒性
  • 批准号:
    6361950
  • 财政年份:
    2001
  • 资助金额:
    --
  • 项目类别:
METHAMPHETAMINE AND HIV PROTEIN-INDUCED NEUROTOXICITY
甲基苯丙胺和 HIV 蛋白引起的神经毒性
  • 批准号:
    6626834
  • 财政年份:
    2001
  • 资助金额:
    --
  • 项目类别:
METHAMPHETAMINE AND HIV PROTEIN-INDUCED NEUROTOXICITY
甲基苯丙胺和 HIV 蛋白引起的神经毒性
  • 批准号:
    6489495
  • 财政年份:
    2001
  • 资助金额:
    --
  • 项目类别:
Dopamine Toxicity in Models of Huntington's Disease
亨廷顿病模型中的多巴胺毒性
  • 批准号:
    6540509
  • 财政年份:
    2001
  • 资助金额:
    --
  • 项目类别:
Dopamine Toxicity in Models of Huntington's Disease
亨廷顿病模型中的多巴胺毒性
  • 批准号:
    6761866
  • 财政年份:
    2001
  • 资助金额:
    --
  • 项目类别:
METHAMPHETAMINE AND HIV PROTEIN-INDUCED NEUROTOXICITY
甲基苯丙胺和 HIV 蛋白引起的神经毒性
  • 批准号:
    6312585
  • 财政年份:
    2001
  • 资助金额:
    --
  • 项目类别:

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