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首页> 外文期刊>Journal of neuroinflammation >Mass-spectrometric profiling of cerebrospinal fluid reveals metabolite biomarkers for CNS involvement in varicella zoster virus reactivation
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Mass-spectrometric profiling of cerebrospinal fluid reveals metabolite biomarkers for CNS involvement in varicella zoster virus reactivation

机译:脑脊液的质谱分析揭示了中枢神经系统参与水痘带状疱疹病毒激活的代谢物生物标志物

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BackgroundVaricella zoster virus (VZV) reactivation spans the spectrum from uncomplicated segmental herpes zoster to life-threatening disseminated CNS infection. Moreover, in the absence of a small animal model for this human pathogen, studies of pathogenesis at the organismal level depend on analysis of human biosamples. Changes in cerebrospinal fluid (CSF) metabolites may reflect critical aspects of host responses and end-organ damage in neuroinfection and neuroinflammation. We therefore applied a targeted metabolomics screen of CSF to three clinically distinct forms of VZV reactivation and infectious and non-infectious disease controls in order to identify biomarkers for CNS involvement in VZV reactivation. MethodsMetabolite profiles were determined by targeted liquid chromatography-mass spectrometry in CSF from patients with segmental zoster (shingles, n =?14), facial nerve zoster ( n =?16), VZV meningitis/encephalitis ( n =?15), enteroviral meningitis ( n =?10), idiopathic Bell’s palsy ( n =?11), and normal pressure hydrocephalus ( n =?15). ResultsConcentrations of 88 metabolites passing quality assessment clearly separated the three VZV reactivation forms from each other and from the non-infected samples. Internal cross-validation identified four metabolites (SM C16:1, glycine, lysoPC a C26:1, PC ae C34:0) that were particularly associated with VZV meningoencephalitis. SM(OH) C14:1 accurately distinguished facial nerve zoster from Bell’s palsy. Random forest construction revealed even more accurate classifiers (signatures comprising 2–4 metabolites) for most comparisons. Some of the most accurate biomarkers correlated only weakly with CSF leukocyte count, indicating that they do not merely reflect recruitment of inflammatory cells but, rather, specific pathophysiological mechanisms. Across all samples, only the sum of hexoses and the amino acids arginine, serine, and tryptophan correlated negatively with leukocyte count. Increased expression of the metabolites associated with VZV meningoencephalitis could be linked to processes relating to neuroinflammation/immune activation, neuronal signaling, and cell stress, turnover, and death (e.g., autophagy and apoptosis), suggesting that these metabolites might sense processes relating to end-organ damage. ConclusionsThe results provide proof-of-concept for the value of CSF metabolites as (1) disease-associated signatures suggesting pathophysiological mechanisms, (2) degree and nature of neuroinflammation, and (3) biomarkers for diagnosis and risk stratification of VZV reactivation and, likely, neuroinfections due to other pathogens. Trial registrationNot applicable (non-interventional study).
机译:背景水痘带状疱疹病毒(VZV)的激活范围从简单的节段性带状疱疹到威胁生命的弥漫性中枢神经系统感染。此外,在没有针对这种人类病原体的小动物模型的情况下,在生物水平上对发病机理的研究取决于对人类生物样品的分析。脑脊液(CSF)代谢产物的变化可能反映了宿主反应的关键方面以及神经感染和神经炎症中的终末器官损害。因此,我们将有针对性的CSF代谢组学筛查应用于三种临床上不同形式的VZV激活以及感染性和非感染性疾病对照,以便确定CNS参与VZV激活的生物标记。方法采用靶向液相色谱-质谱法测定脑带状节段性带状疱疹(带状疱疹,n = 14),面神经带状疱疹(n = 16),VZV脑膜炎/脑炎(n = 15),肠病毒性脑膜炎的代谢物谱(n = 10),特发性贝尔麻痹(n = 11)和正常压力脑积水(n = 15)。结果通过质量评估的88种代谢物的浓度清楚地将三种VZV活化形式彼此分离,并与未感染的样品分离。内部交叉验证确定了四种与VZV脑膜脑炎特别相关的代谢产物(SM C16:1,甘氨酸,lysoPC a C26:1,PC ae C34:0)。 SM(OH)C14:1准确地将面神经带状疱疹与贝尔的麻痹区分开。对于大多数比较而言,随机森林建设显示出甚至更准确的分类器(包含2-4种代谢物的签名)。一些最准确的生物标志物与脑脊液白细胞计数的相关性很弱,表明它们不仅反映了炎症细胞的募集,而且反映了特定的病理生理机制。在所有样品中,只有己糖和氨基酸的精氨酸,丝氨酸和色氨酸之和与白细胞计数呈负相关。与VZV脑膜脑炎相关的代谢物表达增加可能与神经炎症/免疫激活,神经元信号转导以及细胞应激,周转和死亡(例如自噬和凋亡)有关,这表明这些代谢物可能感觉到与终末有关的过程。 -器官损伤。结论结果为CSF代谢物的价值提供了概念验证,因为(1)与疾病相关的特征提示病理生理机制,(2)神经炎​​症的程度和性质,以及(3)诊断和诊断VZV活化的危险分层的生物标志物,以及可能是由于其他病原体引起的神经感染。试用注册不适用(非干预性研究)。

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