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莫能菌素和氯喹可抑制培养的小鼠腹腔巨噬细胞中内吞大分子向溶酶体的转运。

Monensin and chloroquine inhibit transfer to lysosomes of endocytosed macromolecules in cultured mouse peritoneal macrophages.

作者信息

Stenseth K, Thyberg J

机构信息

Department of Medical Cell Biology, Karolinska Institutet, Stockholm/Sweden.

出版信息

Eur J Cell Biol. 1989 Aug;49(2):326-33.

PMID:2776777
Abstract

The effects of the Na+/H+ ionophore monensin and the weak base chloroquine on lysosomal uptake of endocytosed macromolecules were studied in cultured mouse peritoneal macrophages using horseradish peroxidase (HRP) and ferritin as exogenous tracers. The lysosomes were first loaded with HRP using a pulse-chase protocol. The cells were then exposed to ferritin for 30 to 120 min, either in control medium or in medium containing 3 microM monensin or 50 microM chloroquine. Semiquantitative electron microscopic analyses indicated that the uptake of ferritin into HRP-labeled lysosomes was inhibited in the drug-treated cells, and that the tracer particles accumulated in endosomes. At the same time the volume density of the endosomes was increased, fourfold by monensin and threefold by chloroquine; with the latter drug there was also an increase in lysosome volume density. Further, both drugs decreased the rate of endocytosis as measured biochemically, but not in proportion to the reduction of lysosomal ferritin uptake. After withdrawal of the drugs, cell morphology returned to normal and transfer of ferritin from endosomes to HRP-labeled lysosomes was resumed. The recovery was more rapid and complete in monensin-treated than in chloroquine-treated cells. On the basis of these findings and earlier investigations demonstrating that monensin and chloroquine both raise the pH in acid cell compartments, it is suggested that the transfer of soluble and not only membrane-bound macromolecules from endosomes to lysosomes is modulated by the pH in these organelles.

摘要

利用辣根过氧化物酶(HRP)和铁蛋白作为外源性示踪剂,在培养的小鼠腹腔巨噬细胞中研究了Na+/H+离子载体莫能菌素和弱碱氯喹对内吞大分子溶酶体摄取的影响。首先使用脉冲追踪方案使溶酶体装载HRP。然后将细胞在对照培养基中或含有3 microM莫能菌素或50 microM氯喹的培养基中暴露于铁蛋白30至120分钟。半定量电子显微镜分析表明,在药物处理的细胞中,铁蛋白进入HRP标记的溶酶体的摄取受到抑制,并且示踪颗粒在内体中积累。同时,内体的体积密度增加,莫能菌素使其增加四倍,氯喹使其增加三倍;使用后一种药物时,溶酶体体积密度也增加。此外,两种药物均降低了通过生化方法测量的内吞作用速率,但与溶酶体铁蛋白摄取的减少不成比例。停药后,细胞形态恢复正常,铁蛋白从内体向HRP标记的溶酶体的转运恢复。莫能菌素处理的细胞比氯喹处理的细胞恢复更快且更完全。基于这些发现以及早期研究表明莫能菌素和氯喹均会提高酸性细胞区室的pH值,提示从内体到溶酶体的可溶性而非仅膜结合大分子的转运受这些细胞器中pH值的调节。

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