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Neuroimaging Insights Into Early Stages of HIV-Progressive Multifocal Leukoencephalopathy: A Case Report

机译:神经影像学洞察艾滋病毒培养型多焦白血病早期阶段:案例报告

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摘要

This report aims to enhance the understanding of early longitudinal neuroimaging features of progressive multifocal leukoencephalopathy (PML) in human immunodeficiency virus (HIV). Neuroimaging has become crucial in the diagnosis and early recognition of PML. Recognition of magnetic resonance imaging (MRI) features in the early stages of PML is paramount to avoid misdiagnosis and facilitate the delivery of treatments aimed at reducing disease progression. A 49-year-old white man with HIV presented with 4-month progressive left-sided weakness. Neurological examination revealed mild cognitive impairment, left-sided hemiparesis, and somatosense impairment to all modalities. Brain MRI revealed a punctate pattern with innumerable T2-FLAIR (fluid attenuated inversion recovery) hyperintensities in the cortex, brainstem, cerebellum, subcortical, and periventricular areas. Susceptibility-weighted imaging (SWI) revealed hypointensities involving subcortical U-fibers and cortical architecture. A comprehensive diagnostic evaluation was inconclusive. John Cunningham virus (JCV) PCR in cerebrospinal fluid (CSF) was indeterminate. He was started on antiretroviral therapy. Repeat brain MRI performed 1.5 months later, in the setting of further neurological decline, demonstrated progression of the T2-hyperintensities into a large confluent white matter lesion in the right frontoparietal lobe. Despite an indeterminate JCV PCR, the appearance and characteristic progression of the lesions in successive imaging in the setting of severe immunosuppression, with extensive negative infectious workup, was indicative of PML. This clinical experience illustrates unique neuroimaging features of HIV-PML in early stages and its progression over time. It especially highlights the relevance of the SWI sequence in the diagnosis and features observed with disease evolution. Short-term imaging follow-up may assist with the recognition of MRI features consistent with the biology of the infection.
机译:本报告旨在增强人类免疫缺陷病毒(HIV)中进行渐进式多焦白血病(PML)早期纵向神经影像病特征的理解。神经影像动物在诊断和早期识别PML方面变得至关重要。识别PML的早期阶段的磁共振成像(MRI)特征是至关重要的,以避免误诊,并促进旨在减少疾病进展的治疗方法。一名49岁的白人艾滋病毒患有4个月的逐步左侧弱点。神经学检查显示对所有方式的轻度认知障碍,左侧血管血管和躯体均无障碍。脑MRI在皮质,脑干,小脑,细胞系和脑室区域中揭示了一种具有无数T2-展示(流体减毒的倒置恢复)的点状模式。敏感性加权成像(SWI)揭示了涉及皮下U-纤维和皮质架构的低音。全面的诊断评估不确定。脑脊液(CSF)中的John Cunningham病毒(JCV)PCR不确定。他开始抗逆转录病毒治疗。重复脑MRI 1.5个月后,在进一步的神经系统下降的情况下,将T2高原的进展显示为右前叶中的大汇合白质病变。尽管JCV PCR不确定,但在严重免疫抑制中连续成像的情况下病变的外观和特征进展,具有广泛的阴性传染性余处,表明PML。这种临床经验说明了早期阶段中HIV-PML的独特神经影像特征及其随着时间的推移。它特别突出了SWI序列在疾病演化中观察到的诊断和特征中的相关性。短期成像随访可能有助于识别与感染生物学一致的MRI功能。

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