慢性HIV患者的虚弱特征是独立于年龄和抑郁症状的白质萎缩的标志:一项初步研究

K. Kallianpur, Marissa E Sakoda, L. M. Gangcuangco, L. Ndhlovu, Tracie M Umaki, D. Chow, Suwarat Wongjittraporn, C. Shikuma
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引用次数: 14

摘要

慢性艾滋病毒病与神经认知障碍和年龄相关疾病(如虚弱)有关。目的探讨接受稳定联合抗逆转录病毒治疗的老年(≥40岁)HIV阳性患者的脑容量变化是否与衰弱参数相关。方法在夏威夷老年伴HIV队列-心血管疾病研究中,35例HIV感染者接受了t1加权脑磁共振成像、虚弱评估和神经心理测试。评估了五种身体虚弱的特征:低体力活动;疲惫;意外减肥;手握力弱;缓慢的行走速度。线性回归量化了12个脑区与步行时间和握力的横截面关系。结果50.6±6.8岁,77%的患者血浆病毒载量检测不出。1名受试者体弱(具有≥3项脆弱特征);23%的人身体虚弱(1-2个脆弱特征),其综合学习和记忆z分数低于非虚弱个体(p=0.06)。体弱或体弱受试者的握力相对于非体弱组有所降低(p=0.001)。较长的步行时间(较慢的步态)与小脑白质(p<0.001, β= - 0.6)和皮层下灰质(p<0.05, β= - 0.30)的体积降低独立相关。丘脑体积减小与握力减弱相关(p < 0.05, β=0.4)。尾状核体积与握力呈负相关(p<0.01, β= - 0.5)。结论控制良好的HIV感染者小脑白质和皮层下灰质体积变化与运动控制和认知有关。步态速度对白质改变特别敏感,应作为慢性感染患者虚弱和脑萎缩的预测指标进行研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Frailty Characteristics in Chronic HIV Patients are Markers of White Matter Atrophy Independently of Age and Depressive Symptoms: A Pilot Study
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.
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