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表皮生长因子和转化生长因子-α:配体-受体复合物在细胞内的不同转运与加工过程

Epidermal growth factor and transforming growth factor-alpha: differential intracellular routing and processing of ligand-receptor complexes.

作者信息

Ebner R, Derynck R

机构信息

Department of Developmental Biology, Genentech, Inc., South San Francisco, California 94080.

出版信息

Cell Regul. 1991 Aug;2(8):599-612. doi: 10.1091/mbc.2.8.599.

Abstract

Two structurally related but different polypeptide growth factors, epidermal growth factor (EGF) and transforming growth factor-alpha (TGF-alpha), exert their activities after interaction with a common cell-surface EGF/TGF-alpha-receptor. Comparative studies of the effects of both ligands have established that TGF-alpha is more potent than EGF in a variety of biological systems. This observation is not explained by differences in affinities of the ligands for the receptor, because the affinity-constants of both factors are very similar. We have compared the intracellular processing of ligand-receptor complexes using either EGF or TGF-alpha in two different cell systems. We found that TGF-alpha dissociates from the EGF/TGF-alpha-receptor at much higher pH than EGF, which may reflect the substantial difference in the calculated isoelectric points. After internalization, the intracellular TGF-alpha is more rapidly cleared than EGF, and a substantial portion of the released TGF-alpha represents undegraded TGF-alpha in contrast to the mostly degraded EGF. In addition, TGF-alpha did not induce a complete down-regulation of cell surface receptors, as observed with EGF, which is at least in part responsible for a much sooner recovery of the ligand-binding ability after down-regulation, in the case of TGF-alpha. These differences in processing of the ligand-receptor complexes may explain why TGF-alpha exerts quantitatively higher activities than EGF.

摘要

两种结构相关但不同的多肽生长因子,即表皮生长因子(EGF)和转化生长因子-α(TGF-α),在与共同的细胞表面EGF/TGF-α受体相互作用后发挥其活性。对两种配体作用的比较研究表明,在多种生物系统中,TGF-α比EGF更具活性。这种观察结果不能用配体与受体亲和力的差异来解释,因为两种因子的亲和常数非常相似。我们在两种不同的细胞系统中比较了使用EGF或TGF-α时配体-受体复合物的细胞内加工过程。我们发现,TGF-α在比EGF高得多的pH值下从EGF/TGF-α受体上解离,这可能反映了计算出的等电点的显著差异。内化后,细胞内的TGF-α比EGF清除得更快,并且释放的TGF-α的很大一部分代表未降解的TGF-α,这与大多已降解的EGF形成对比。此外,与EGF不同,TGF-α不会诱导细胞表面受体的完全下调,这至少部分是TGF-α下调后配体结合能力更快恢复的原因。配体-受体复合物加工过程中的这些差异可能解释了为什么TGF-α比EGF发挥更高的定量活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b56c/361851/bd007f5226ad/cellregul00033-0019-a.jpg

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