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125I标记的人表皮生长因子。在人成纤维细胞中的结合、内化和降解

125I-labeled human epidermal growth factor. Binding, internalization, and degradation in human fibroblasts.

作者信息

Carpenter G, Cohen S

出版信息

J Cell Biol. 1976 Oct;71(1):159-71. doi: 10.1083/jcb.71.1.159.

Abstract

125I-labeled human epidermal growth factor (hEGF) binds in a specific and saturable manner to human fibroblasts. At 37 degrees C, the cell-bound 125I-hEGF initially may be recovered in a native form by acid extraction; upon subsequent incubation, the cell-bound 125I-hEGF is degraded very rapidly, with the appearance in the medium of 125I-monoiodotyrosine. At 0 degrees C, cell-bound 125I-hEGF is not degraded but slowly dissociates from the cell. The data are consistent with a mechanism in which 125I-hEGF initially is bound to the cell surface and subsequently is internlized before degradation. The degradation is blocked by inhibitors of metabolic energy production (azide, cyanide, dinitrophenol), some protease inhibitors (Tos-Lys-CH2Cl, benzyl guanidobenzoate), a lysosomotropic agent (chloroquine) various local anesthetics (cocaine, lidocaine, procaine), and ammonium chloride. After the binding and degradation of 125I-hEGF the fibroblasts are no longer able to rebind fresh hormone. The binding capacity of these cells is restored by incubation in a serum-containing medium; this restoration is inhibited by cycloheximide or actinomycin D.

摘要

125I标记的人表皮生长因子(hEGF)以特异性和可饱和的方式与人成纤维细胞结合。在37℃时,细胞结合的125I-hEGF最初可通过酸提取以天然形式回收;随后孵育时,细胞结合的125I-hEGF迅速降解,培养基中出现125I-单碘酪氨酸。在0℃时,细胞结合的125I-hEGF不降解,但会缓慢从细胞上解离。这些数据与一种机制一致,即125I-hEGF最初与细胞表面结合,随后在降解前被内化。代谢能量产生抑制剂(叠氮化物、氰化物、二硝基苯酚)、一些蛋白酶抑制剂(甲苯磺酰-L-赖氨酸氯甲基酮、苄基胍苯甲酸酯)、溶酶体促渗剂(氯喹)、各种局部麻醉剂(可卡因、利多卡因、普鲁卡因)和氯化铵可阻断降解。125I-hEGF结合并降解后,成纤维细胞不再能够重新结合新鲜激素。通过在含血清的培养基中孵育可恢复这些细胞的结合能力;这种恢复受到环己酰亚胺或放线菌素D的抑制。

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Commentary. Lysosomotropic agents.述评。溶酶体亲和剂。
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