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原发性HIV感染期间的脑白质完整性

Cerebral white matter integrity during primary HIV infection.

作者信息

Wright Patrick W, Vaida Florin F, Fernández-de Thomas Ricardo J, Rutlin Jerrel, Price Richard W, Lee Evelyn, Peterson Julia, Fuchs Dietmar, Shimony Joshua S, Robertson Kevin R, Walter Rudolph, Meyerhoff Dieter J, Spudich Serena, Ances Beau M

机构信息

aDepartment of Biomedical Engineering bDepartment of Neurology, School of Medicine, St. Louis, Missouri cDepartment of Family and Preventive Medicine, UCSD, San Diego, California, USA dDepartment of Biology, University of Puerto Rico, Río Piedras, San Juan, Puerto Rico eDepartment of Psychiatry, WUSTL School of Medicine, St. Louis, Missouri fDepartment of Neurology, UCSF, San Francisco, California, USA gDivision of Biological Chemistry, Innsbruck Medical University, Innsbruck, Austria hDepartment of Radiology, WUSTL School of Medicine, St. Louis, Missouri iDepartment of Neurology, UNC, Chapel Hill, North Carolina jCenter for Imaging of Neurodegenerative Diseases, VA Medical Center, San Francisco kDepartment of Radiology and Biomedical Imaging, UCSF, San Francisco, California lDepartment of Neurology, Yale University, New Haven, Connecticut, USA. *Drs Serena S. Spudich and Beau M. Ances contributed equally to the writing of this article.

出版信息

AIDS. 2015 Feb 20;29(4):433-42. doi: 10.1097/QAD.0000000000000560.

Abstract

OBJECTIVE

Inflammation and infection within the central nervous system is initiated during primary HIV infection (PHI), but the association of these processes with the integrity of brain white matter during PHI is unknown.

DESIGN

We used diffusion tensor imaging (DTI) in this prospective cross-sectional neuroimaging study to determine the extent of white matter involvement in early HIV infection.

METHODS

Antiretroviral-naive PHI (defined as <1 year after infection, n = 62), chronic HIV infection (CHI, n = 16), and HIV-uninfected (n = 19) participants had DTI, laboratory, and neuropsychometric performance assessments. DTI metrics were examined using region of interest and whole brain voxelwise analyses. Linear mixed-effects models assessed correlations between DTI measures and laboratory and neuropsychometric performance values.

RESULTS

PHI participants were assessed at a median 4.1 months after estimated infection, and had median CD4 cell count of 573 cells/μl, and HIV-1 RNA viral load of 4.5 log10 copies/ml in plasma and 2.6 log10 copies/ml in cerebrospinal fluid (CSF). DTI metrics in PHI individuals were similar to HIV- participants and correlated with disruptions in the blood-brain barrier (indicated by CSF/plasma albumin ratio and CSF protein). CHI participants had significant loss of white matter integrity that correlated with biomarkers of infection and inflammation (blood viral load, CD4 T-cell count, and neopterin, and CSF white blood cell). Within the PHI group, DTI metrics inversely correlated with increasing days since infection.

CONCLUSION

In individuals assessed during PHI, group DTI measures suggested relative preservation of white matter microstructural integrity, but were associated with disruption of the blood-brain barrier and estimated duration of infection.

摘要

目的

中枢神经系统的炎症和感染在原发性HIV感染(PHI)期间就已开始,但这些过程与PHI期间脑白质完整性的关联尚不清楚。

设计

在这项前瞻性横断面神经影像学研究中,我们使用扩散张量成像(DTI)来确定早期HIV感染中白质受累的程度。

方法

未接受抗逆转录病毒治疗的PHI患者(定义为感染后<1年,n = 62)、慢性HIV感染(CHI,n = 16)和未感染HIV的参与者(n = 19)接受了DTI、实验室和神经心理测量性能评估。使用感兴趣区域和全脑体素分析来检查DTI指标。线性混合效应模型评估DTI测量值与实验室和神经心理测量性能值之间的相关性。

结果

PHI参与者在估计感染后的中位时间为4.1个月进行评估,中位CD4细胞计数为573个/μl,血浆中HIV-1 RNA病毒载量为4.5 log10拷贝/ml,脑脊液(CSF)中为2.6 log10拷贝/ml。PHI个体的DTI指标与未感染HIV的参与者相似,并与血脑屏障的破坏相关(由CSF/血浆白蛋白比率和CSF蛋白表示)。CHI参与者的白质完整性显著丧失,这与感染和炎症的生物标志物相关(血液病毒载量、CD4 T细胞计数、新蝶呤和CSF白细胞)。在PHI组中,DTI指标与感染后天数的增加呈负相关。

结论

在PHI期间接受评估的个体中,DTI组测量结果表明白质微观结构完整性相对保留,但与血脑屏障破坏和估计的感染持续时间相关。

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