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蛋白质生物标志物可区分皮肤利什曼病流行地区利什曼原虫主要感染个体和未感染个体。

Protein biomarkers discriminate Leishmania major-infected and non-infected individuals in areas endemic for cutaneous leishmaniasis.

作者信息

Kammoun-Rebai Wafa, Naouar Ikbel, Libri Valentina, Albert Matthew, Louzir Hechmi, Meddeb-Garnaoui Amel, Duffy Darragh

机构信息

Laboratory of Medical Parasitology, Biotechnologies and Biomolecules, Institut Pasteur de Tunis, Tunis, Tunisia.

University of Tunis El Manar, Tunis, 1068, Tunisia.

出版信息

BMC Infect Dis. 2016 Mar 24;16:138. doi: 10.1186/s12879-016-1458-6.

Abstract

BACKGROUND

A successful host immune response to infection is dependent upon both innate and adaptive immune effector mechanisms. Cutaneous leishmaniasis results in an adaptive Th1 CD4(+) T cell response that efficiently clears the parasite, but may also result in scaring. However the role of innate mechanisms during parasite clearance remains less well defined.

METHODS

We examined a unique cohort of individuals, living in a Leishmania major endemic region, that were stratified among 3 distinct clinical groups in a cross-sectional study. Specifically, patients were classified either as healed (n = 17), asymptomatic (23), or naïve to infection (18) based upon the classical Leishmanin Skin Test (LST) and the presence or absence of scars. Utilizing a multiplexed immunoassay approach we characterized the induced cytokine and chemokine response to L. major.

RESULTS

A subset of innate immune molecules was induced in all groups. By contrast, T cell-associated cytokines were largely induced in exposed groups as compared to L. major-infection naïve individuals. Two exceptions were IL-17A and IL-12p70, induced and not induced, respectively, in naïve individuals. In addition, GM-CSF was more strongly induced in healed patients as compared to the other two groups. Surprisingly an IL-13 response was the best cytokine for classifying previously infected donors.

CONCLUSIONS

Exploratory data analysis, utilizing principle component analysis (PCA), revealed distinct patient clusters of the healed and naïve groups based on the most differentially induced proteins. Asymptomatic previously infected individuals were more difficult to assign to a particular cluster based on these induced proteins. Analysis of these proteins may enable the identification of biomarkers associated with disease, leading to a better understanding of the protective mechanisms of immune response against leishmaniasis.

摘要

背景

宿主对感染的成功免疫反应依赖于先天性和适应性免疫效应机制。皮肤利什曼病会引发适应性Th1 CD4(+) T细胞反应,该反应能有效清除寄生虫,但也可能导致瘢痕形成。然而,先天性机制在寄生虫清除过程中的作用仍不太明确。

方法

我们在一项横断面研究中,对生活在利什曼原虫主要流行地区的一组独特个体进行了研究,这些个体被分为3个不同的临床组。具体而言,根据经典的利什曼原虫皮肤试验(LST)以及瘢痕的有无,将患者分为已治愈(n = 17)、无症状(23)或未感染(18)三类。我们采用多重免疫测定方法,对诱导的针对大利什曼原虫的细胞因子和趋化因子反应进行了表征。

结果

所有组均诱导了一部分先天性免疫分子。相比之下,与未感染大利什曼原虫的个体相比,暴露组中与T细胞相关的细胞因子大多被诱导产生。两个例外是IL-17A和IL-12p70,分别在未感染个体中被诱导产生和未被诱导产生。此外,与其他两组相比,GM-CSF在已治愈患者中诱导更强。令人惊讶的是,IL-13反应是区分先前感染供体的最佳细胞因子。

结论

利用主成分分析(PCA)进行的探索性数据分析显示,根据诱导差异最大的蛋白质,已治愈组和未感染组存在明显的患者聚类。基于这些诱导蛋白,无症状的先前感染个体更难被归为特定聚类。对这些蛋白质的分析可能有助于识别与疾病相关的生物标志物,从而更好地理解免疫反应对利什曼病的保护机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8dea/4806467/112d89b8f81e/12879_2016_1458_Fig1_HTML.jpg

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