Willingham M C, Maxfield F R, Pastan I H
J Cell Biol. 1979 Sep;82(3):614-25. doi: 10.1083/jcb.82.3.614.
Using transmission electron microscopy, we have studied the interaction of alpha 2 macroglobulin (alpha 2 M) with the surface of cultured fibroblasts. When cells were incubated for 2 h at 4 degrees C with ferritin-conjugated alpha 2 M, approximately 90% of the alpha 2 M was diffusely distributed on the cell surface, and the other 10% was concentrated in "coated" pits. A pattern of diffuse labeling with some clustering in "coated" pits was also obtained when cells were incubated for 5 min at 4 degrees C with alpha 2 M, fixed with glutaraldehyde, and the alpha 2 M was localized with affinity-purified, peroxidase-labeled antibody to alpha 2 M. Experiments in which cells were fixed with 0.2% paraformaldehyde before incubation with alpha 2 M showed that the native distribution of alpha 2 M receptors was entirely diffuse without significant clustering in "coated" pits. This indicates that some redistribution of the alpha 2 M-receptor complexes into clusters occurred even at 4 degrees C. In experiments with concanavalin A(Con A), we found that some of the Con A clustered in coated regions of the membrane and was internalized in coated vesicles, but much of the Con A was directly internalized in uncoated vesicles or pinosomes. We conclude that unoccupied alpha 2 M receptors are diffusely distributed on the cell surface. When alpha 2 M-receptor complexes are formed, they rapidly cluster in coated regions or pits in the plasma membrane and subsequently are internalized in coated vesicles. Because insulin and epidermal growth factor are internalized in the same structures as alpha 2 M (Maxfield, F.R., J. Schlessinger, Y. Schechter, I. Pastan, and M.C. Willingham. 1978. Cell, 14: 805--810.), we suggest that all peptide hormones, as well as other proteins that enter the cell by receptor-mediated endocytosis, follow this same pathway.
利用透射电子显微镜,我们研究了α2巨球蛋白(α2M)与培养的成纤维细胞表面的相互作用。当细胞在4℃下与铁蛋白结合的α2M孵育2小时时,约90%的α2M分散分布在细胞表面,另外10%集中在“有被”小窝中。当细胞在4℃下与α2M孵育5分钟,用戊二醛固定,并用亲和纯化的、过氧化物酶标记的抗α2M抗体定位α2M时,也得到了一种在“有被”小窝中有一些聚集的弥散标记模式。在与α2M孵育前先用0.2%多聚甲醛固定细胞的实验表明,α2M受体的天然分布完全是弥散的,在“有被”小窝中无明显聚集。这表明即使在4℃时,α2M - 受体复合物也会重新分布形成聚集。在用伴刀豆球蛋白A(Con A)进行的实验中,我们发现一些Con A聚集在膜的有被区域并被内化到有被小泡中,但许多Con A直接被内化到无被小泡或胞饮体中。我们得出结论,未被占据的α2M受体分散分布在细胞表面。当α2M - 受体复合物形成时,它们迅速聚集在质膜的有被区域或小窝中,随后被内化到有被小泡中。由于胰岛素和表皮生长因子与α2M在相同结构中被内化(马克斯菲尔德,F.R.,J.施莱辛格,Y.谢克特,I.帕斯坦,和M.C.韦林厄姆。1978年。细胞,14:805 - 810.),我们认为所有肽类激素以及其他通过受体介导的内吞作用进入细胞的蛋白质都遵循相同的途径。