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在杆状外段吞噬过程中,培养的正常和营养不良大鼠色素上皮细胞中肌动蛋白的分布。

The distribution of actin in cultured normal and dystrophic rat pigment epithelial cells during the phagocytosis of rod outer segments.

作者信息

Chaitin M H, Hall M O

出版信息

Invest Ophthalmol Vis Sci. 1983 Jul;24(7):821-31.

PMID:6345446
Abstract

In the previous article the authors reported that the ingestion phase of phagocytosis is defective in cultured dystrophic rat pigment epithelial (PE) cells. When these cells are challenged with isolated rod outer segments (ROS), attachment of ROS to the PE cell surfaces occurs to a normal extent. However, only a small number of these bound ROS are subsequently ingested. This raised the possibility that the contractile protein actin might not function normally in the dystrophic rat PE cells, since actin is intimately involved in the ingestion mechanism in other phagocytic cells. Utilizing actin antibodies and the technique of indirect immunofluorescence, we have studied the distribution of actin in cultured normal and dystrophic rat PE cells. Results show that the arrangement of actin fibers in the dystrophic cells appears normal both before and during the attachment of ROS to the cell surfaces. With the additional use of an ROS antiserum to label externally bound ROS, it is also possible to show that actin is involved with the ingestion of ROS by both normal and dystrophic PE cells. Thus, it appears that actin can function normally in dystrophic PE cells, but that the ingestion mechanism becomes activated at only a few sites of ROS attachment. The results of a scanning electron microscope study support this conclusion and also show the presence of a saucer-shaped elaboration of the PE cell plasma membrane beneath attached ROS. These may correspond to the actin feltworks seen with immunofluorescence microscopy at sites of ROS attachment.

摘要

在前一篇文章中,作者报道了在培养的营养不良大鼠色素上皮(PE)细胞中,吞噬作用的摄取阶段存在缺陷。当用分离的视杆外段(ROS)刺激这些细胞时,ROS与PE细胞表面的附着在正常程度上发生。然而,随后只有少量结合的ROS被摄取。这就提出了一种可能性,即收缩蛋白肌动蛋白在营养不良大鼠的PE细胞中可能无法正常发挥作用,因为肌动蛋白在其他吞噬细胞的摄取机制中密切相关。利用肌动蛋白抗体和间接免疫荧光技术,我们研究了肌动蛋白在培养的正常和营养不良大鼠PE细胞中的分布。结果表明,在ROS附着于细胞表面之前和期间,营养不良细胞中肌动蛋白纤维的排列看起来都是正常的。通过额外使用ROS抗血清来标记外部结合的ROS,还可以表明正常和营养不良的PE细胞中肌动蛋白都参与了ROS的摄取。因此,看起来肌动蛋白在营养不良的PE细胞中可以正常发挥作用,但摄取机制仅在ROS附着的少数位点被激活。扫描电子显微镜研究的结果支持这一结论,并且还显示在附着的ROS下方存在PE细胞质膜的碟形精细结构。这些可能与在ROS附着位点通过免疫荧光显微镜观察到的肌动蛋白网络相对应。

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