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通过单分子力谱技术展示肝素与恶性疟原虫感染的 vs. 未感染的红细胞的特异性结合。

Demonstration of specific binding of heparin to Plasmodium falciparum-infected vs. non-infected red blood cells by single-molecule force spectroscopy.

机构信息

Nanobioengineering Group, Institute for Bioengineering of Catalonia (IBEC), Baldiri Reixac 10-12, Barcelona E08028, Spain.

出版信息

Nanoscale. 2013 May 7;5(9):3673-80. doi: 10.1039/c2nr32821f. Epub 2013 Jan 10.

Abstract

Glycosaminoglycans (GAGs) play an important role in the sequestration of Plasmodium falciparum-infected red blood cells (pRBCs) in the microvascular endothelium of different tissues, as well as in the formation of small clusters (rosettes) between infected and non-infected red blood cells (RBCs). Both sequestration and rosetting have been recognized as characteristic events in severe malaria. Here we have used heparin and pRBCs infected by the 3D7 strain of P. falciparum as a model to study GAG-pRBC interactions. Fluorescence microscopy and fluorescence-assisted cell sorting assays have shown that exogenously added heparin has binding specificity for pRBCs (preferentially for those infected with late forms of the parasite) vs. RBCs. Heparin-pRBC adhesion has been probed by single-molecule force spectroscopy, obtaining an average binding force ranging between 28 and 46 pN depending on the loading rate. No significant binding of heparin to non-infected RBCs has been observed in control experiments. This work represents the first approach to quantitatively evaluate GAG-pRBC molecular interactions at the individual molecule level.

摘要

糖胺聚糖(GAGs)在疟原虫感染的红细胞(pRBC)在不同组织的微血管内皮中的隔离以及在感染和未感染的红细胞(RBC)之间形成小簇(玫瑰花结)中起着重要作用。 这两种隔离和玫瑰花结都被认为是严重疟疾的特征事件。 在这里,我们使用肝素和由恶性疟原虫 3D7 株感染的 pRBC 作为模型来研究 GAG-pRBC 相互作用。 荧光显微镜和荧光辅助细胞分选分析表明,外源性添加的肝素对 pRBC(优先对感染寄生虫晚期形式的 RBC)具有结合特异性,而对 RBC 没有特异性。 通过单分子力谱法探测肝素-pRBC 黏附,根据加载速率获得在 28 和 46 pN 之间变化的平均结合力。 在对照实验中未观察到肝素与未感染的 RBC 发生显著结合。 这项工作代表了在个体分子水平上定量评估 GAG-pRBC 分子相互作用的首次尝试。

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