Biopsychosocial phenotypes in people with HIV in the CHARTER cohort.

IF 4.1 Q1 CLINICAL NEUROLOGY Brain communications Pub Date : 2024-07-29 eCollection Date: 2024-01-01 DOI:10.1093/braincomms/fcae224
Bin Tang, Ronald J Ellis, Florin Vaida, Anya Umlauf, Donald R Franklin, Raha Dastgheyb, Leah H Rubin, Patricia K Riggs, Jennifer E Iudicello, David B Clifford, David J Moore, Robert K Heaton, Scott L Letendre
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Abstract

Neuropsychiatric complications such as neurocognitive impairment and depression are common in people with HIV despite viral suppression on antiretroviral therapy, but these conditions are heterogeneous in their clinical presentations and associated disability. Identifying novel biopsychosocial phenotypes that account for neurocognitive performance and depressive and functional symptoms will better reflect the complexities encountered in clinical practice and may have pathological and therapeutic implications. We classified 1580 people with HIV based on 17 features, including 7 cognitive domains, 4 subscales of the Beck depression inventory-II, 5 components of the patient's assessment of own functioning inventory, and dependence in instrumental and basic activities of daily living. A two-stage clustering procedure consisting of dimension reduction with self-organizing maps and Mahalanobis distance-based k-means clustering algorithms was applied to cross-sectional data. Baseline demographic and clinical characteristics were compared between the phenotypes, and their prediction on the biopsychosocial phenotypes was evaluated using multinomial logistic regression. Four distinct phenotypes were identified. Participants in Phenotype 1 overall did well in all domains. Phenotype 2 had mild-to-moderate depressive symptoms and the most substance use disorders. Phenotype 3 had mild-to-moderate cognitive impairment, moderate depressive symptoms, and the worst daily functioning; they also had the highest proportion of females and non-HIV conditions that could affect cognition. Phenotype 4 had mild-to-moderate cognitive impairment but with relatively good mood, and daily functioning. Multivariable analysis showed that demographic characteristics, medical conditions, lifetime cocaine use disorder, triglycerides, and non-antiretroviral therapy medications were important variables associated with biopsychosocial phenotype. We found complex, multidimensional biopsychosocial profiles in people with HIV that were associated with different risk patterns. Future longitudinal work should determine the stability of these phenotypes, assess factors that influence transitions from one phenotype to another, and characterize their biological associations.

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CHARTER 队列中艾滋病毒感染者的生物心理社会表型。
在接受抗逆转录病毒治疗的艾滋病病毒感染者中,尽管病毒得到了抑制,但神经认知障碍和抑郁症等神经精神并发症仍很常见,但这些症状在临床表现和相关残疾方面存在差异。确定新的生物心理社会表型以解释神经认知表现和抑郁及功能性症状,将更好地反映临床实践中遇到的复杂情况,并可能具有病理和治疗意义。我们根据 17 个特征对 1580 名艾滋病病毒感染者进行了分类,其中包括 7 个认知领域、贝克抑郁量表-II 的 4 个分量表、患者对自身功能评估量表的 5 个组成部分,以及在工具性和基本日常生活活动中的依赖性。对横截面数据进行了两阶段聚类,包括使用自组织图和基于马哈拉诺比距离的 k-means 聚类算法进行降维。比较了不同表型的基线人口学和临床特征,并使用多项式逻辑回归评估了它们对生物心理社会表型的预测。结果发现了四种不同的表型。表型 1 的参与者总体上在所有领域都表现良好。表型 2 有轻度至中度抑郁症状,药物使用障碍最多。表型 3 患有轻度至中度认知障碍、中度抑郁症状和最差的日常功能;他们中女性和可能影响认知的非艾滋病毒疾病的比例也最高。表型 4 患有轻度至中度认知障碍,但情绪和日常功能相对较好。多变量分析表明,人口统计学特征、医疗条件、终生可卡因使用障碍、甘油三酯和非抗逆转录病毒治疗药物是与生物心理社会表型相关的重要变量。我们发现,艾滋病病毒感染者的生物心理社会表型复杂而多维,与不同的风险模式相关。未来的纵向工作应确定这些表型的稳定性,评估影响从一种表型过渡到另一种表型的因素,并描述其生物学关联。
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