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Leishmania Donovani. Hamster macrophage interactions in vitro: cell entry, intracellular survival, and multiplication of amastigotes

机译:利什曼原虫Donovani。体外仓鼠巨噬细胞相互作用:细胞进入,细胞内存活和变形虫的繁殖。

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摘要

An in vitro system was developed for studying host-parasite cellular interactions in visceral leishmaniasis with amastigotes isolated from infected spleens of hamsters and their peritoneal macrophages maintained by an improved method. The culture system supports the growth of Leishmania donovani amastigotes with different parasite/macrophage ratios for up to 2 wk, yielding results more consistent and reproducible than previously possible. Results indicated that the “forms” of the amastigotes (with or without adherent host membranes) and the “state” of the macrophages (with or without stimulation in vivo by thioglycollate or in vitro by aging) had no effect on the growth rate of the parasites, which, however, seems to vary with the macrophage subpopulations. An electron microscope study suggests that amastigotes are ingested through phagocytosis by the macrophages and become lodged in loose phagosomes. Additional evidence with quantitative data is presented to support the earlier findings that phagosome-lysosome fusion occurs after the interiorization of the parasites and that they not only survive but multiply in these vacuoles. During the postinfection periods, reorientation of amastigotes in vacuolar space results in the appearance of three types of parasitophorous vacuoles (parasites in loose vacuoles, in tight-fitting vacuoles or abutting in part against the inner lining of vacuoles). The last category may be the predominant type giving rise to the variations observed. Exogenously introduced dense marker accumulated in these parasitophorous vacuoles of the macrophages infected for several days indicating a continuous accessibility of amastigotes to the ambient mestruum via phagosome-lysosome vacuolar system of the host cells. This finding may have significant implications in parasite nutrition, host immunity, and chemotherapy of leishmaniasis.
机译:开发了一种体外系统,用于研究内脏利什曼病中宿主与寄生虫之间的细胞相互作用,该小鼠与从受感染的仓鼠脾脏及其腹膜巨噬细胞中分离得到的变形虫(通过改良方法得以维持)。该培养系统支持具有不同寄生虫/巨噬细胞比率的多形利什曼原虫amastigotes的生长,长达2 wk,比以前可能产生的结果更加一致和可重复。结果表明,变形虫的“形式”(带有或不带有粘附的宿主膜)和巨噬细胞的“状态”(带有或不带有巯基乙酸盐的体内刺激或体外受衰老的刺激)均不影响其生长速度。寄生虫,但是,似乎与巨噬细胞亚群不同。电子显微镜研究表明,变形虫通过巨噬细胞的吞噬作用被吞噬,并滞留在疏松的吞噬物中。提供了带有定量数据的其他证据来支持早期发现,即寄生虫内化后发生吞噬体-溶酶体融合,并且它们不仅存活,而且在这些液泡中繁殖。在感染后的时期,变形虫在液泡空间中的重新定向导致出现三种类型的寄生虫液泡(寄生于液泡中,紧密贴合的液泡中或部分地邻接液泡的内衬)。最后一类可能是导致观察到的变化的主要类型。外源导入的致密标记物在被感染巨噬细胞的这些亚寄生液泡中积累了数天,这表明变形虫可以通过宿主细胞的吞噬体-溶酶体液泡系统连续进入周围环境。这一发现可能对寄生虫的营养,宿主免疫力和利什曼病的化学疗法具有重要意义。

著录项

  • 作者

    Chang, K-P; Dwyer, DM;

  • 作者单位
  • 年度 1978
  • 总页数
  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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