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首页> 外文期刊>Clinical and vaccine immunology: CVI >Mapping Antigenic Motifs in the Trypomastigote Small Surface Antigen from Trypanosoma cruzi
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Mapping Antigenic Motifs in the Trypomastigote Small Surface Antigen from Trypanosoma cruzi

机译:从锥虫锥虫中的锥虫小表面抗原中绘制抗原序列

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摘要

The trypomastigote small surface antigen (TSSA) is a mucin-like molecule from Trypanosoma cruzi, the etiological agent of Chagas disease, which displays amino acid polymorphisms in parasite isolates. TSSA expression is restricted to the surface of infective cell-derived trypomastigotes, where it functions as an adhesin and engages surface receptors on the host cell as a prerequisite for parasite internalization. Previous results have established TSSA-CL, the isoform encoded by the CL Brener clone, as an appealing candidate for use in serology-based diagnostics for Chagas disease. Here, we used a combination of peptide-and recombinant protein-based tools to map the antigenic structure of TSSA-CL at maximal resolution. Our results indicate the presence of different partially overlapping B-cell epitopes clustering in the central portion of TSSA-CL, which contains most of the polymorphisms found in parasite isolates. Based on these results, we assessed the serodiagnostic performance of a 21-amino-acid-long peptide that spans TSSA-CL major antigenic determinants, which was similar to the performance of the previously validated glutathione S-transferase (GST)-TSSA-CL fusion molecule. Furthermore, the tools developed for the antigenic characterization of the TSSA antigen were also used to explore other potential diagnostic applications of the anti-TSSA humoral response in Chagasic patients. Overall, our present results provide additional insights into the antigenic structure of TSSA-CL and support this molecule as an excellent target for molecular intervention in Chagas disease.
机译:锥虫小表面抗原(TSSA)是Crypanosoma Cruzi的粘蛋白样分子,Cruzi是Chagas疾病的病因,它在寄生虫分离株中显示氨基酸多态性。 TSSA表达仅限于感染细胞衍生的锥虫的表面,在该表面上,它充当粘附蛋白,并在宿主细胞上接合表面受体,作为寄生虫内在化的先决条件。先前的结果已经建立了TSSA-CL,这是由CL Brener Clone编码的同工型,作为用于基于血清学的chagas疾病诊断的有吸引力的候选人。在这里,我们使用了肽和基于重组蛋白的工具的组合来绘制最大分辨率下TSSA-CL的抗原结构。我们的结果表明,在TSSA-CL的中心部分聚类的不同部分重叠的B细胞表位存在,其中包含寄生虫分离株中发现的大多数多态性。基于这些结果,我们评估了跨越TSSA-CL主要抗原决定因素的21-氨基酸长肽的血清诊断性能,该抗原剂与先前验证的谷胱甘肽S-转移酶(GST)-TSSSSSA-CL相似融合分子。此外,为TSSA抗原的抗原表征而开发的工具还用于探索抗TSSA体液反应在chagasic患者中的其他潜在诊断应用。总体而言,我们目前的结果为TSSA-CL的抗原结构提供了更多的见解,并支持该分子是chagas疾病分子干预的绝佳靶标。

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