首页> 美国卫生研究院文献>Journal of Visualized Experiments : JoVE >Detection of Trypanosoma brucei Variant Surface Glycoprotein Switching by Magnetic Activated Cell Sorting and Flow Cytometry
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Detection of Trypanosoma brucei Variant Surface Glycoprotein Switching by Magnetic Activated Cell Sorting and Flow Cytometry

机译:磁激活细胞分选和流式细胞术检测布鲁氏锥虫变体表面糖蛋白开关

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摘要

Trypanosoma brucei, a protozoan parasite that causes both Human and Animal African Trypanosomiasis (known as sleeping sickness and nagana, respectively) cycles between a tsetse vector and a mammalian host. It evades the mammalian host immune system by periodically switching the dense, variant surface glycoprotein (VSG) that covers its surface. The detection of antigenic variation in Trypanosoma brucei can be both cumbersome and labor intensive. Here, we present a method for quantifying the number of parasites that have 'switched' to express a new VSG in a given population. The parasites are first stained with an antibody against the starting VSG, and then stained with a secondary antibody attached to a magnetic bead. Parasites expressing the starting VSG are then separated from the rest of the population by running the parasites over a column attached to a magnet. Parasites expressing the dominant, starting VSG are retained on the column, while the flow-through contains parasites that express a new VSG as well as some contaminants expressing the starting VSG. This flow-through population is stained again with a fluorescently labeled antibody against the starting VSG to label contaminants, and propidium iodide (PI), which labels dead cells. A known number of absolute counting beads that are visible by flow cytometry are added to the flow-through population. The ratio of beads to number of cells collected can then be used to extrapolate the number of cells in the entire sample. Flow cytometry is used to quantify the population of switchers by counting the number of PI negative cells that do not stain positively for the starting, dominant VSG. The proportion of switchers in the population can then be calculated using the flow cytometry data.
机译:布鲁氏锥虫(Trypanosoma brucei)是一种原生动物寄生虫,可导致人和动物非洲锥虫病(分别称为昏睡病和长假名)在采采蝇载体和哺乳动物宿主之间循环。它通过周期性地切换覆盖其表面的致密,变异的表面糖蛋白(VSG)来逃避哺乳动物宿主的免疫系统。布氏锥虫的抗原变异的检测既麻烦又费力。在这里,我们提出了一种量化给定种群中已“切换”以表达新VSG的寄生虫数量的方法。首先将寄生虫用针对起始VSG的抗体染色,然后再用附着在磁珠上的第二抗体染色。然后,通过将寄生虫在与磁铁相连的柱子上运行,将表达起始VSG的寄生虫与其余种群分离。表示主要起始VSG的寄生虫保留在色谱柱上,而流出物则包含表示新VSG的寄生虫以及一些表示起始VSG的污染物。再次用抗起始VSG的荧光标记抗体和标记死细胞的碘化丙锭(PI)再次对这种流通种群进行染色。通过流式细胞术可见的已知数量的绝对计数珠添加到流通人口中。珠子与收集的细胞数之比然后可以用来推断整个样品中的细胞数。流式细胞术用于通过计数未对起始显性VSG阳性染色的PI阴性细胞的数量来量化切换者的数量。然后可以使用流式细胞仪数据计算切换者在人群中的比例。

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