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外周炎症增加与病毒学控制的 HIV 感染者的结构脑变化和血流减少有关。

Increased Peripheral Inflammation Is Associated With Structural Brain Changes and Reduced Blood Flow in People With Virologically Controlled HIV.

机构信息

Department of Microbiology, Immunology, and Inflammation, Center for Neurovirology and Gene Editing, Lewis Katz School of Medicine, Temple University, Philadelphia, Pennsylvania.

Department of Neurology, Washington University in St Louis, St Louis, Missouri, USA.

出版信息

J Infect Dis. 2023 Oct 18;228(8):1071-1079. doi: 10.1093/infdis/jiad229.

Abstract

BACKGROUND

While antiretroviral therapy (ART) has improved outcomes for people with HIV (PWH), brain dysfunction is still evident. Immune activation and inflammation remain elevated in PWH receiving ART, thereby contributing to morbidity and mortality. Previous studies demonstrated reduced functional and structural changes in PWH; however, underlying mechanisms remain elusive.

METHODS

Our cohort consisted of PWH with ART adherence and viral suppression ( < 50 copies/mL; N = 173). Measurements included immune cell markers of overall immune health (CD4/CD8 T-cell ratio) and myeloid inflammation (CD16+ monocytes), plasma markers of inflammatory status (soluble CD163 and CD14), and structural and functional neuroimaging (volume and cerebral blood flow [CBF], respectively).

RESULTS

Decreased CD4/CD8 ratios correlated with reduced brain volume, and higher levels of inflammatory CD16+ monocytes were associated with reduced brain volume in total cortex and gray matter. An increase in plasma soluble CD14-a marker of acute peripheral inflammation attributed to circulating microbial products-was associated with reduced CBF within the frontal, parietal, temporal, and occipital cortices and total gray matter.

CONCLUSIONS

CD4/CD8 ratio and number of CD16+ monocytes, which are chronic immune cell markers, are associated with volumetric loss in the brain. Additionally, this study shows a potential new association between plasma soluble CD14 and CBF.

摘要

背景

虽然抗逆转录病毒疗法(ART)改善了艾滋病毒感染者(PWH)的预后,但大脑功能障碍仍然明显。接受 ART 的 PWH 中免疫激活和炎症仍然升高,从而导致发病率和死亡率增加。先前的研究表明 PWH 的功能和结构变化减少;然而,潜在的机制仍不清楚。

方法

我们的队列包括接受 ART 依从性和病毒抑制(<50 拷贝/ml;N=173)的 PWH。测量包括整体免疫健康的免疫细胞标志物(CD4/CD8 T 细胞比值)和髓样炎症(CD16+单核细胞)、炎症状态的血浆标志物(可溶性 CD163 和 CD14)以及结构和功能神经影像学(分别为体积和脑血流[CBF])。

结果

CD4/CD8 比值降低与脑体积减少相关,炎症性 CD16+单核细胞水平升高与总皮质和灰质脑体积减少相关。血浆可溶性 CD14 增加——一种归因于循环微生物产物的急性外周炎症标志物——与额、顶、颞和枕叶皮质以及总灰质内的 CBF 减少相关。

结论

慢性免疫细胞标志物 CD4/CD8 比值和 CD16+单核细胞数量与大脑体积减少有关。此外,本研究显示了血浆可溶性 CD14 和 CBF 之间的潜在新关联。

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