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首页> 外文期刊>Open Medicine Journal >Frailty Characteristics in Chronic HIV Patients are Markers of White Matter Atrophy Independently of Age and Depressive Symptoms: A Pilot Study
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Frailty Characteristics in Chronic HIV Patients are Markers of White Matter Atrophy Independently of Age and Depressive Symptoms: A Pilot Study

机译:一项初步研究表明,慢性HIV患者的虚弱特征是与年龄和抑郁症状无关的白色物质萎缩的标志

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Background:Chronic HIV disease is associated with neurocognitive impairment and age-related conditions such as frailty.Objective:To determine whether regional brain volumetric changes correlate with frailty parameters in older (≥ 40 years) HIV+ patients on stable combination antiretroviral therapy.Method:Thirty-five HIV-infected participants in the Hawaii Aging with HIV Cohort - Cardiovascular Disease study underwent T1-weighted brain magnetic resonance imaging, frailty assessment and neuropsychological testing. Five physical frailty traits were assessed: low physical activity; exhaustion; unintentional weight loss; weak hand grip strength; slow walking speed. Linear regression quantified cross-sectional relationships of 12 brain regions to walking times and hand grip strength.Results:Participants were 50.6 ± 6.8 years old and 77% had undetectable plasma viral load. One subject was frail (possessing ≥ 3 frailty traits); 23% were pre-frail (1–2 frailty traits) and had worse composite learning and memory z-scores than did non-frail individuals (p =0.06). Pre-frail or frail subjects had reduced hand grip strength relative to the non-frail group (p =0.001). Longer walking times (slower gait) related independently to lower volumes of cerebellar white matter (p <0.001, β=?0.6) and subcortical gray matter (p <0.05, β=?0.30). Reduced thalamus volume was linked to weaker grip strength (p < 0.05, β=0.4). Caudate volume was negatively associated with grip strength (p <0.01, β=?0.5).Conclusion:Volumetric changes in cerebellar white matter and subcortical gray matter, brain regions involved in motor control and cognition, may be connected to frailty development in well-controlled HIV. Gait speed is particularly sensitive to white matter alterations and should be investigated as a predictor of frailty and brain atrophy in chronically infected patients.
机译:背景:慢性HIV疾病与神经认知障碍和衰弱等与年龄相关的疾病有关。目的:确定年龄≥40岁的HIV +患者在稳定的联合抗逆转录病毒治疗下区域脑容量变化是否与衰弱参数相关。方法:三十夏威夷老龄化和艾滋病毒队列研究的5名被HIV感染的参与者进行了T1加权脑磁共振成像,脆弱性评估和神经心理学测试。评估了五个身体虚弱特征:低运动量;精疲力尽意外体重减轻;手握力弱;步行速度慢。线性回归定量分析了12个大脑区域与步行时间和握力的横断面关系。结果:参与者为50.6±6.8岁,有77%的血浆病毒载量无法检测。一名受试者身体虚弱(具有3种以上的脆弱特征); 23%的人是脆弱的前体(1-2个脆弱特征),其复合学习和记忆z得分比非脆弱者差(p = 0.06)。相对于非体弱者组,体弱者或前体力者的握力降低(p = 0.001)。较长的行走时间(步态较慢)与小脑白质(p <0.001,β=?0.6)和皮层下灰质(p <0.05,β=?0.30)的体积较小有关。丘脑体积减小与握力减弱有关(p <0.05,β= 0.4)。尾鳍体积与握力强度呈负相关( p <0.01,β=?0.5)。结论:小脑白质和皮层下灰质的体积变化,参与运动控制和认知的大脑区域可能与体弱发育有关控制得当的艾滋病毒。步态速度对白质变化特别敏感,应该作为慢性感染患者虚弱和脑萎缩的预测指标进行研究。

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