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多个亚细胞区室参与表皮生长因子的细胞内加工过程。

Involvement of multiple subcellular compartments in intracellular processing of epidermal growth factor.

作者信息

Miskimins W K, Shimizu N

出版信息

J Cell Biochem. 1982;20(1):41-50. doi: 10.1002/jcb.240200105.

Abstract

The intracellular translocation and processing of epidermal growth factor (EGF) in 3T3 cells has been studied utilizing Percoll density gradients. EGF is internalized and rapidly becomes associated with two types of intracellular compartments. The extent to which EGF is delivered to these two compartments is apparently regulated depending upon the cell's physiological condition. In growth medium, an increased proportion of EGF is taken up into a Golgi-like element. Uptake through this pathway correlates with a decrease in degradation of the ligand. In the absence of serum and amino acids, an increased proportion of EGF is taken up into a component which has a density of 1.05. Uptake through this pathway correlates with increased degradation of the ligand. The ligand taken up through both pathways is transferred to dense vesicles which comigrate with lysosomes. In the presence of growth medium, however, dense vesicles containing EGF can be shown to be lysosomal enzyme-deficient upon further fractionation. In addition, in the presence of serum, a portion of the internalized EGF is apparently released from the cells, intact, and then re-bound. The processes described may be important in the production of a mitogenic response and the ability of cells to self-regulate their responsiveness to the growth factor.

摘要

利用Percoll密度梯度研究了表皮生长因子(EGF)在3T3细胞中的细胞内转运和加工过程。EGF被内化并迅速与两种类型的细胞内区室相关联。EGF被递送至这两个区室的程度显然根据细胞的生理状态受到调节。在生长培养基中,增加比例的EGF被摄取到一种类高尔基体成分中。通过该途径的摄取与配体降解的减少相关。在无血清和氨基酸的情况下,增加比例的EGF被摄取到一种密度为1.05的成分中。通过该途径的摄取与配体降解的增加相关。通过这两条途径摄取的配体被转移至与溶酶体共同迁移的致密小泡中。然而,在生长培养基存在的情况下,进一步分级分离时可显示含有EGF的致密小泡缺乏溶酶体酶。此外,在血清存在的情况下,一部分内化的EGF显然完整地从细胞中释放出来,然后重新结合。所描述的这些过程在产生有丝分裂反应以及细胞自我调节其对生长因子反应性的能力方面可能很重要。

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