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在人类免疫缺陷病毒 1 型感染中,高活性抗逆转录病毒治疗中断期间的认知功能。

Cognitive functioning during highly active antiretroviral therapy interruption in human immunodeficiency virus type 1 infection.

机构信息

Department of Neurosciences, University of California at San Diego, San Diego, California 92103, USA.

出版信息

J Neurovirol. 2008 Nov;14(6):550-7. doi: 10.1080/13550280802372313.

DOI:10.1080/13550280802372313
PMID:19016380
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4692591/
Abstract

Although no longer considered therapeutically beneficial, antiretroviral treatment interruptions (TIs) still occur frequently among patients with human immunodeficiency virus (HIV) infection for a variety of reasons. TIs typically result in viral rebound and worsening immunosuppression, which in turn are risk factors for neurocognitive decline and dementia. We sought to determine the extent of neurocognitive risk with TIs and subsequent reintroduction of highly active antiretroviral therapy (HAART) by using a comprehensive, sensitive neuropsychological assessment and by concurrently determining changes in plasma and cerebrospinal fluid (CSF) viral load and CD4 counts. Prospective, serial, clinical evaluations including neuropsychological (NP) testing and measurement of plasma HIV RNA and CD4 count and mood state were performed on HIV-1-infected individuals (N=11) at three time points: (1) prior to a TI, while on HAART; (2) after TIs averaging 6 months; and (3) after reinitiating HAART therapy. During TI, plasma HIV RNA increased and CD4 counts declined significantly, but NP performance did not change. Following reinitiation of HAART, viral loads fell below pre-TI levels, and CD4 counts rose. Improved viral suppression and immune restoration with reinitiation of HAART resulted in significant improvement in neurocognitive performance. No changes on comprehensive questionnaires of mood state were observed in relation to TI.NP performance and mood state remained stable during TIs despite worsened viral loads and CD4 counts. Because "practice effects" are generally greatest between the first and second NP testing sessions, improvement at the third, post-TI time point was unlikely to be accounted for by practice. TIs of up to 6 months appear to be neurocognitively and psychiatrically safe for most patients.

摘要

尽管不再被认为具有治疗益处,但由于各种原因,艾滋病毒(HIV)感染者中断抗逆转录病毒治疗(TI)的情况仍经常发生。TI 通常会导致病毒反弹和免疫抑制恶化,这反过来又成为神经认知能力下降和痴呆的危险因素。我们试图通过使用全面、敏感的神经心理学评估,并同时确定血浆和脑脊液(CSF)病毒载量和 CD4 计数的变化,来确定 TI 及其随后重新引入高效抗逆转录病毒治疗(HAART)的神经认知风险程度。前瞻性、连续的临床评估包括神经心理学(NP)测试以及血浆 HIV RNA 和 CD4 计数和情绪状态的测量,对 11 名 HIV-1 感染者在三个时间点进行:(1)在 TI 之前,同时进行 HAART;(2)TI 平均 6 个月后;(3)重新开始 HAART 治疗后。在 TI 期间,血浆 HIV RNA 增加,CD4 计数显著下降,但 NP 表现没有变化。重新开始 HAART 后,病毒载量降至 TI 前水平以下,CD4 计数上升。随着 HAART 的重新启动,病毒抑制和免疫恢复得到改善,导致神经认知表现显著改善。在 TI 期间,与 TI 相关的情绪状态综合问卷没有观察到变化。尽管病毒载量和 CD4 计数恶化,但 NP 表现和情绪状态在 TI 期间保持稳定。由于“练习效应”通常在第一次和第二次 NP 测试之间最大,因此在第三次(TI 后)时间点的改善不太可能归因于练习。长达 6 个月的 TI 似乎对大多数患者在神经认知和精神上都是安全的。

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