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血清抗性相关蛋白在布氏罗得西亚锥虫和转基因布氏布氏锥虫中的定位

Localization of serum resistance-associated protein in Trypanosoma brucei rhodesiense and transgenic Trypanosoma brucei brucei.

作者信息

Bart Jean-Mathieu, Cordon-Obras Carlos, Vidal Isabel, Reed Jennifer, Perez-Pastrana Esperanza, Cuevas Laureano, Field Mark C, Carrington Mark, Navarro Miguel

机构信息

Instituto de Parasitología y Biomedicina 'López-Neyra', Consejo Superior de Investigaciones Científicas, Granada, Spain.

Centro Nacional de Medicina Tropical, Instituto de Salud Carlos III, Madrid, Spain.

出版信息

Cell Microbiol. 2015 Oct;17(10):1523-35. doi: 10.1111/cmi.12454. Epub 2015 Jun 26.

Abstract

African trypanosomes infect a broad range of mammals, but humans and some higher primates are protected by serum trypanosome lytic factors that contain apolipoprotein L1 (ApoL1). In the human-infective subspecies of Trypanosoma brucei, Trypanosoma brucei rhodesiense, a gene product derived from the variant surface glycoprotein gene family member, serum resistance-associated protein (SRA protein), protects against ApoL1-mediated lysis. Protection against trypanosome lytic factor requires the direct interaction between SRA protein and ApoL1 within the endocytic apparatus of the trypanosome, but some uncertainty remains as to the precise mechanism and location of this interaction. In order to provide more insight into the mechanism of SRA-mediated resistance to trypanosome lytic factor, we assessed the localization of SRA in T. b. rhodesiense EATRO3 using a novel monoclonal antibody raised against SRA together with a set of well-characterized endosomal markers. By three-dimensional deconvolved immunofluorescence single-cell analysis, combined with double-labelling immunoelectron microscopy, we found that ≈ 50% of SRA protein localized to the lysosome, with the remaining population being distributed through the endocytic pathway, but apparently absent from the flagellar pocket membrane. These data suggest that the SRA/trypanolytic factor interaction is intracellular, with the concentration within the endosomes potentially crucial for ensuring a high efficiency.

摘要

非洲锥虫可感染多种哺乳动物,但人类和一些高等灵长类动物受到血清锥虫溶解因子的保护,这些因子含有载脂蛋白L1(ApoL1)。在布氏锥虫的人类感染亚种——罗德西亚锥虫中,一种源自可变表面糖蛋白基因家族成员血清抗性相关蛋白(SRA蛋白)的基因产物可抵御ApoL1介导的细胞溶解。抵御锥虫溶解因子需要SRA蛋白与锥虫内吞装置中的ApoL1直接相互作用,但这种相互作用的确切机制和位置仍存在一些不确定性。为了更深入了解SRA介导的对锥虫溶解因子抗性的机制,我们使用针对SRA产生的新型单克隆抗体以及一组特征明确的内体标记物,评估了SRA在罗德西亚锥虫EATRO3中的定位。通过三维去卷积免疫荧光单细胞分析,结合双标记免疫电子显微镜,我们发现约50%的SRA蛋白定位于溶酶体,其余部分分布在内吞途径中,但鞭毛袋膜中显然没有。这些数据表明,SRA/锥虫溶解因子相互作用是在细胞内进行的,内体中的浓度对于确保高效性可能至关重要。

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