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一种新型抗体替代生物标志物,用于监测感染克氏锥虫的患者寄生虫的持续存在。

A novel antibody surrogate biomarker to monitor parasite persistence in Trypanosoma cruzi-infected patients.

机构信息

R&D, INFYNITY BIOMARKERS SAS, Lyon, France.

Faculty of Medicine, University of Leuven (KULAK), Kortrijk, Belgium.

出版信息

PLoS Negl Trop Dis. 2018 Feb 9;12(2):e0006226. doi: 10.1371/journal.pntd.0006226. eCollection 2018 Feb.

Abstract

BACKGROUND

Trypanosoma cruzi parasite, the causative agent of Chagas disease, infects about six million individuals in more than 20 countries. Monitoring parasite persistence in infected individuals is of utmost importance to develop and evaluate treatments to control the disease. Routine screening for infected human individuals is achieved by serological assays; PCR testing to monitor spontaneous or therapy-induced parasitological cure has limitations due to the low and fluctuating parasitic load in circulating blood. The aim of the present study is to evaluate a newly developed antibody profiling assay as an indirect method to assess parasite persistence based on waning of antibodies following spontaneous or therapy-induced clearance of the infection.

METHODOLOGY/PRINCIPAL FINDINGS: We designed a multiplex serology assay, an array of fifteen optimized T. cruzi antigens, to evaluate antibody diversity in 1654 serum samples from chronic Chagas patients. One specific antibody response (antibody 3, Ab3) showed a strong correlation with T. cruzi parasite persistence as determined by T. cruzi PCR positive results. High and sustained Ab3 signal was strongly associated with PCR positivity in untreated patients, whereas significant decline in Ab3 signals was observed in BZN-treated patients who cleared parasitemia based on blood PCR results.

CONCLUSION/SIGNIFICANCE: Ab3 is a new surrogate biomarker that strongly correlates with parasite persistence in chronic and benznidazole-treated Chagas patients. We hypothesize that Ab3 is induced and maintained by incessant stimulation of the immune system by tissue-based and shed parasites that are not consistently detectable by blood based PCR techniques. Hence, a simple immunoassay measurement of Ab3 could be beneficial for monitoring the infectious status of seropositive patients.

摘要

背景

克氏锥虫寄生虫是恰加斯病的病原体,感染了 20 多个国家的约 600 万人。监测感染个体中寄生虫的持续存在对于开发和评估治疗方法以控制疾病至关重要。通过血清学检测来监测感染个体中寄生虫的持续存在;然而,PCR 检测监测自发性或治疗诱导的寄生虫学治愈存在局限性,因为循环血液中的寄生虫载量低且波动。本研究旨在评估一种新开发的抗体分析检测方法,作为一种间接方法来评估基于感染自发性或治疗诱导清除后抗体衰减的寄生虫持续存在。

方法/主要发现:我们设计了一种多重血清学检测方法,即十五种优化的克氏锥虫抗原阵列,用于评估 1654 份慢性恰加斯病患者血清样本中的抗体多样性。一种特定的抗体反应(抗体 3,Ab3)与 T. cruzi PCR 阳性结果确定的寄生虫持续存在具有很强的相关性。在未经治疗的患者中,高且持续的 Ab3 信号与 PCR 阳性强烈相关,而在根据血液 PCR 结果清除寄生虫血症的 BZN 治疗患者中,观察到 Ab3 信号显著下降。

结论/意义:Ab3 是一种新的替代生物标志物,与慢性和苯并咪唑治疗的恰加斯病患者中的寄生虫持续存在强烈相关。我们假设 Ab3 是由组织相关和脱落的寄生虫不断刺激免疫系统引起和维持的,而这些寄生虫无法通过血液 PCR 技术始终检测到。因此,Ab3 的简单免疫测定可能有益于监测血清阳性患者的感染状态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fc14/5823467/d0aca41a5ad3/pntd.0006226.g001.jpg

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