Neurophysiological markers of HAND and the impact of aging: Evidence from MEG

HAND 的神经生理学标志物和衰老的影响：来自 MEG 的证据

• 批准号: 9275016
• 负责人: Tony W Wilson
• 金额: $ 43.01万
• 依托单位: UNIVERSITY OF NEBRASKA MEDICAL CENTER
• 依托单位国家: 美国
• 财政年份: 2014
• 资助国家: 美国
• 起止时间: 2014-08-01 至 2019-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/9275016
• 关键词: AIDS Dementia Complex; Adult; Affect; Age; Aging; Aging-Related Process; Anti-Retroviral Agents; Area; Biological Markers; Brain; Brain Neoplasms; Brain imaging; Chronic; Clinical; Cognitive; Cognitive deficits; Complex; Consensus; Controlled Study; Data; Development; Diagnosis; Diagnostic tests; Disease; Disease Progression; Drug toxicity; Emerging Technologies; Encephalitis; Evaluation; Evolution; Exclusion; Exhibits; Functional disorder; Funding; General Population; Goals; HIV; HIV Infections; HIV diagnosis; HIV-associated neurocognitive disorder; High Prevalence; Human; Image; Impaired cognition; Impairment; Knowledge; Laboratories; Life Expectancy; Location; Longitudinal Studies; Magnetic Resonance Imaging; Magnetoencephalography; Malignant Neoplasms; Maps; Measures; Mental disorders; Methods; Microglia; Monitor; Motor; Motor Cortex; National Institute of Mental Health; National Institute of Neurological Disorders and Stroke; Nature; Neurologic; Neurons; Neuropsychological Tests; Neuropsychology; Opportunistic Infections; Participant; Patients; Performance; Persons; Physiology; Prefrontal Cortex; Prevalence; Protocols documentation; Recommendation; Research; Research Personnel; Research Priority; Residual state; Risk; Sensory; Series; Targeted Research; Task Performances; Terminal Disease; Testing; Time; Viral Load result; Visit; age effect; age group; antiretroviral therapy; association cortex; base; cognitive function; cognitive performance; cognitive task; density; excitotoxicity; experimental study; frontal eye fields; high risk; imaging study; macrophage; millisecond; neurocognitive disorder; neuroimaging; neurophysiology; programs; public health relevance; relating to nervous system; spatiotemporal; specific biomarkers; temporal measurement; treatment response; trend

DESCRIPTION (provided by applicant): Combination antiretroviral therapy (cART) has dramatically shifted the nature of HIV-infection from a terminal illness to a chronic manageable condition, with a life expectancy close to that of the general population. However, infected patients remain at a significantly increased risk of developing HIV-associated neurocognitive disorders (HAND), with 35-70% of all patients (treated and untreated) exhibiting at least subtle impairments in neuropsychological function. This revised R01 proposal from an early-stage investigator (ESI) will examine the neurophysiological bases of HAND, identify markers of HAND progression, and determine how chronic HIV- infection modulates the normal effects of aging on cognitive performance and brain physiology. Over the past two years, my laboratory has evaluated the impact that cART treated HIV-infection has on neural activity and neuropsychological (NP) function through a series of imaging studies using magnetoencephalography (MEG). MEG is a noninvasive and direct measure of neuronal activity with millisecond temporal resolution and good spatial precision (3-5 mm). Using MEG, we have demonstrated neurophysiological abnormalities in the frontal eye fields, dorsolateral prefrontal cortex, and other association cortices, as well as deficits in the primary motor cortex. Most commonly, we have found hyper-activation in association cortices and hypo-activation in primary sensory and motor areas of patients relative to uninfected controls. We have also shown that activation metrics in specific brain areas correlate with scores on NP tests, and that the effects of aging on neuronal activity and cognitive function follow a distinct trajectory in HIV-infected patients compared with controls. Anchored by these extensive preliminary findings, we propose that MEG imaging is uniquely sensitive to the pathophysiology and progression of HAND, and to the additive effects that HIV-infection and aging have on neuronal function. To this end, we will examine 162 adults, 81 HIV-infected patients and 81 demographically-matched controls, divided equally into three age-specific groups (i.e., 22-38, 39-55, and over 55 years). All participants will undergo high- density MEG recording during a series of cognitive tasks, complete several MRI/DTI protocols, and perform a battery of NP assessments that adheres to the recommendations of the Frascati consensus [7]. To evaluate the progression of HAND, a subset of participants (infected and uninfected) will be followed longitudinally at 1.5-year intervals. The Specific Aims of this project are to: (1) Determine the neurophysiological bases of HAND by comparing HIV-infected patients who are impaired, according to the Frascati criteria, to those who are unimpaired; (2) Identify neuronal markers of HAND progression through a short-term longitudinal study of controls and impaired patients, who will undergo repeated MEG and NP testing sessions at 1.5 year intervals; (3) Determine how aging modulates NP function and neuronal activity in patients and controls, and identify the independent effect of HIV-infection on these parameters. We expect that the cognitive and neural deficits associated with HIV-infection will be significantly exacerbated by the aging process in critical brain networks.

描述（由申请人提供）： 联合抗逆转录病毒疗法（cART）已将艾滋病毒感染的性质从绝症急剧转变为可控制的慢性疾病，预期寿命接近普通人群。然而，感染患者发展HIV相关神经认知障碍（HAND）的风险仍然显著增加，所有患者（治疗和未治疗）中有35-70%至少表现出轻微的神经心理功能障碍。这项来自早期研究者（ESI）的修订R 01提案将检查HAND的神经生理学基础，确定HAND进展的标志物，并确定慢性HIV感染如何调节衰老对认知能力和脑生理学的正常影响。在过去的两年里，我的实验室通过一系列使用脑磁图（MEG）的成像研究，评估了cART治疗HIV感染对神经活动和神经心理（NP）功能的影响。脑磁图是一种非侵入性和直接测量神经元活动的方法，具有毫秒级的时间分辨率和良好的空间精度（3-5 mm）。使用脑磁图，我们已经证明了神经生理异常的额眼领域，背外侧前额叶皮层，和其他联合皮层，以及在初级运动皮层的缺陷。最常见的是，我们发现，相对于未感染的对照组，患者的联合皮质过度激活，初级感觉和运动区激活不足。我们还表明，特定大脑区域的激活指标与NP测试的分数相关，并且与对照组相比，HIV感染患者的衰老对神经元活动和认知功能的影响遵循不同的轨迹。锚定这些广泛的初步研究结果，我们建议，脑磁图成像是唯一敏感的病理生理和进展的手，和艾滋病毒感染和老化对神经元功能的叠加效应。为此，我们将检查162名成年人，81名艾滋病毒感染者和81名人口统计学匹配的对照，平均分为三个年龄组（即，22-38岁，39-55岁，55岁以上）。所有参与者将在一系列认知任务期间接受高密度MEG记录，完成几项MRI/DTI方案，并执行一系列符合Frascati共识建议的NP评估[7]。为了评估HAND的进展，将以1.5年的间隔纵向随访一部分受试者（感染和未感染）。该项目的具体目标是：（1）通过比较根据Frascati标准受损的HIV感染患者与未受损的患者来确定HAND的神经生理学基础;（2）通过对对照组和受损患者的短期纵向研究来确定HAND进展的神经标志物，受损患者将每隔1.5年重复进行MEG和NP测试;（3）确定衰老如何调节患者和对照组的NP功能和神经元活性，并确定HIV感染对这些参数的独立影响。我们预计，与艾滋病毒感染相关的认知和神经缺陷将因关键大脑网络的老化过程而显著加剧。