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β型转化生长因子的细胞受体。人类和啮齿动物细胞系中的配体结合与亲和标记

Cellular receptors for type beta transforming growth factor. Ligand binding and affinity labeling in human and rodent cell lines.

作者信息

Massagué J, Like B

出版信息

J Biol Chem. 1985 Mar 10;260(5):2636-45.

PMID:2982829
Abstract

Type beta transforming growth factor (beta TGF) purified from human platelets to homogeneity as judged by NH2-terminal amino acid sequence analysis has been labeled with 125I to characterize its interaction with cellular receptors. Binding of 125I-beta TGF to target cells is temperature- and time-dependent, specific, saturable, and reversible. About 1.6-1.9 X 10(4) binding sites/cell with high affinity for beta TGF (Kd = 5.6-7.8 X 10(-11) M and 9.1-14 X 10(-11) M, respectively) are found in NRK-49F and BALB/c 3T3 cells. beta TGF receptors do not appear to undergo acute down-regulation by the ligand. Specific binding of 125I-beta TGF has been observed in several human, rat, and mouse fibroblast lines and in some, but not all, tumor-derived cell lines examined. 125I-beta TGF has been cross-linked to intact cells and isolated membrane preparations using disuccinimidyl suberate. Cells and isolated membranes from human, rat, and mouse origin affinity labeled with 125I-beta TGF exhibit a major labeled species of approximately 280 kilodaltons that has the properties of high affinity and specificity expected from a physiologically relevant beta TGF receptor. Minor labeled species of 70-90 kilodaltons are also labeled by 125I-beta TGF, but they correspond to molecular species with low apparent affinity (Kd approximately 10(-8) M) for 125I-beta TGF.

摘要

通过氨基末端氨基酸序列分析判断,从人血小板中纯化至同质的β型转化生长因子(β-TGF)已用125I标记,以表征其与细胞受体的相互作用。125I-β-TGF与靶细胞的结合是温度和时间依赖性的、特异性的、可饱和的且可逆的。在NRK-49F和BALB/c 3T3细胞中发现约1.6 - 1.9×10(4)个对β-TGF具有高亲和力的结合位点/细胞(Kd分别为5.6 - 7.8×10(-11) M和9.1 - 14×10(-11) M)。β-TGF受体似乎不会因配体而发生急性下调。在几种人、大鼠和小鼠成纤维细胞系以及一些(但不是全部)所检测的肿瘤衍生细胞系中观察到了125I-β-TGF的特异性结合。已使用辛二酸二琥珀酰亚胺酯将125I-β-TGF与完整细胞和分离的膜制剂进行交联。用人、大鼠和小鼠来源的细胞及分离膜进行125I-β-TGF亲和标记后,显示出一种主要的标记物种,其分子量约为280千道尔顿,具有生理相关β-TGF受体所预期的高亲和力和特异性特性。70 - 90千道尔顿的次要标记物种也被125I-β-TGF标记,但它们对应于对125I-β-TGF表观亲和力较低(Kd约为10(-8) M)的分子物种。

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