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难消化物质的积累会降低巨噬细胞溶酶体的融合能力。

Accumulation of indigestible substances reduces fusion competence of macrophage lysosomes.

作者信息

Montgomery R R, Webster P, Mellman I

机构信息

Department of Cell Biology, Yale University School of Medicine, New Haven, CT 06510.

出版信息

J Immunol. 1991 Nov 1;147(9):3087-95.

PMID:1919007
Abstract

It is well known that mouse macrophages loaded with indigestible substances become highly vacuolated. However, why this vacuolization occurs and its effect on lysosome function and intracellular transport during endocytosis remain unknown. Here, macrophage vacuoles were formed by incubation with sucrose or a tripeptide of the D-isomer of alanine and were determined to be lysosomal in origin by staining with the lysosomal glycoproteins and lysosomal hydrolases. However, as indicated by confocal and electron microscopy, subsequent delivery of both fluid phase (lucifer yellow, horse-radish peroxidase) and receptor-bound ligands (IgG complexes) was significantly reduced, suggesting that indigestible material reduced the ability of the loaded lysosomes to fuse with endosomes containing newly internalized tracers. Nevertheless, ligands internalized by the vacuolated cells were degraded at almost the normal rate, indicating that degradation occurs in the absence of delivery to the loaded lysosomes. We have also found that this fusion inhibition occurs in human alveolar macrophages loaded with physiologic debris from smoking and asbestos. These results suggest that indigestible material within lysosomes, such as is present in residual bodies in vivo, may affect their fusion competence.

摘要

众所周知,装载了难以消化物质的小鼠巨噬细胞会高度空泡化。然而,这种空泡化为何会发生以及其在胞吞作用期间对溶酶体功能和细胞内运输的影响仍然未知。在这里,巨噬细胞空泡是通过与蔗糖或丙氨酸D-异构体的三肽孵育形成的,并且通过用溶酶体糖蛋白和溶酶体水解酶染色确定其起源于溶酶体。然而,如共聚焦显微镜和电子显微镜所示,随后液相(荧光素黄、辣根过氧化物酶)和受体结合配体(IgG复合物)的传递均显著减少,这表明难以消化的物质降低了装载的溶酶体与含有新内化示踪剂的内体融合的能力。尽管如此,空泡化细胞内化的配体以几乎正常的速率降解,这表明降解在没有传递到装载的溶酶体的情况下发生。我们还发现,这种融合抑制发生在装载了来自吸烟和石棉的生理碎片的人肺泡巨噬细胞中。这些结果表明,溶酶体内的难以消化物质,如体内残余小体中存在的物质,可能会影响它们的融合能力。

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