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Trypanosoma cruzi uses macropinocytosis as an additional entry pathway into mammalian host cell

机译:克鲁氏锥虫使用巨胞饮作用作为进入哺乳动物宿主细胞的另一种进入途径

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Several intracellular pathogens are internalized by host cells via multiple endocytic pathways. It is no different with Trypanosoma cruzi. Evidences indicate that T. cruzi entry may occur by endocytosis/phagocytosis or by an active manner. Although macropinocytosis is largely considered an endocytic process where cells internalize only large amounts of solutes, several pathogens use this pathway to enter into host cells. To investigate whether T. cruzi entry into peritoneal macrophages and LLC-MK2 epithelial cells can be also mediated through a macropinocytosis-like process, we used several experimental strategies presently available to characterize macropinocytosis such as the use of different inhibitors. These macropinocytosis' inhibitors blocked internalization of T. cruzi by host cells. To further support this, immunofluorescence microscopy and scanning electron microscopy techniques were used. Field emission scanning electron microscopy revealed that after treatment, parasites remained attached to the external side of host cell plasma membrane. Proteins such as Rabankyrin 5, tyrosine kinases, Pak1 and actin microfilaments, which participate in macropinosome formation, were localized at T. cruzi entry sites. We also observed co-localization between the parasite and an endocytic fluid phase marker. All together, these results indicate that T. cruzi is able to use multiple mechanisms of penetration into host cell, including macropinocytosis.
机译:宿主细胞通过多种内吞途径将几种细胞内病原体内在化。克鲁氏锥虫没有什么不同。有证据表明克鲁斯氏锥虫进入可能是通过内吞/吞噬或通过主动方式发生的。尽管巨胞饮作用在很大程度上被认为是胞吞过程,在这种过程中,细胞仅将大量溶质内在化,但一些病原体仍使用此途径进入宿主细胞。为了研究是否可以通过类似巨胞吞作用的过程介导克氏锥虫进入腹膜巨噬细胞和LLC-MK2上皮细胞,我们使用了几种目前可表征巨胞饮作用的实验策略,例如使用不同的抑制剂。这些巨胞饮抑制剂抑制了宿主细胞对克鲁维氏酵母的内在化。为了进一步证明这一点,使用了免疫荧光显微镜和扫描电子显微镜技术。场发射扫描电子显微镜显示,处理后,寄生虫仍然附着在宿主细胞质膜的外侧。参与巨鼻小球体形成的蛋白质(如Rabankyrin 5,酪氨酸激酶,Pak1和肌动蛋白微丝)位于克鲁维氏酵母的进入位点。我们还观察到了寄生虫和内吞流体相标记之间的共定位。总之,这些结果表明克鲁氏梭菌能够利用多种渗透入宿主细胞的机制,包括巨胞饮作用。

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