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MCF-7细胞中结合雌激素与抗雌激素的交换:雌激素受体配体诱导稳定构象的证据

Exchange of bound estrogens and antiestrogens in MCF-7 cells: evidence for ligand-induced stable configurations of the estrogen receptor.

作者信息

El khissiin A, Leclercq G

机构信息

Laboratoire J.-C. Heuson de Cancérologie Mammaire, Institut Jules Bordet, Brussels, Belgium.

出版信息

Steroids. 1998 Nov;63(11):565-74. doi: 10.1016/s0039-128x(98)00064-6.

Abstract

Estrogens and antiestrogens promote specific conformations of the estrogen receptor (ER). To analyze the influence of such configurations on the stability of the ligand-ER complexes, MCF-7 breast cancer cells were exposed for 1 h to either [3H]E2 or an unlabeled estrogen or antiestrogen (E2, DES, E1, BP; OH-Tam, RU 39,411, ICI 164,384, RU 58,668); mutual exchange rates of bound compounds (i.e., [3H]E2-->ligand; ligand-->[3H]E2) were then analyzed in cell extracts by measuring [3H]E2. Addition of cycloheximide (CHX) to the incubation medium eliminated the potential interference of E2-induced ER loss. Extracts from control untreated cells were labeled with [3H]E2 or one of these various ligands and similarly submitted to exchange. Displacement of bound compounds occurred at moderate temperature (18 degrees C) but not at 4 degrees C. Remarkably, exchange proceeded at a lower rate in extracts from cells preincubated with [3H]E2 or a ligand. Antiestrogens RU 39,411 and RU 58,668 appeared especially refractory to displacement. Such low exchange rates were also recorded in experiments conducted on whole cells although to a higher extent than in extracts from preincubated cells. Enzyme immunoassays demonstrated that absence of major exchange could not be attributed to ER loss. Moreover, displacement of bound ligands appeared independent of their binding affinity for the receptor. These data suggest that estrogen and antiestrogen binding is stabilized by at least one factor (coactivators or corepressors) thus fixing the receptor molecules in a configuration that is relatively resistant to subsequent exchange. FPLC and PgR induction revealed that a significant proportion of ER maintained in a sufficiently flexible status was still able to exchange and transduce the transcriptional message of the displacer ligand.

摘要

雌激素和抗雌激素可促进雌激素受体(ER)形成特定构象。为分析此类构象对配体-ER复合物稳定性的影响,将MCF-7乳腺癌细胞分别用[³H]E2或未标记的雌激素或抗雌激素(E2、己烯雌酚、E1、BP;羟基他莫昔芬、RU 39,411、ICI 164,384、RU 58,668)处理1小时;然后通过测量[³H]E2来分析细胞提取物中结合化合物的相互交换率(即[³H]E2→配体;配体→[³H]E2)。向孵育培养基中添加放线菌酮(CHX)消除了E2诱导的ER损失的潜在干扰。用[³H]E2或这些不同配体之一标记未处理的对照细胞提取物,并同样进行交换。结合化合物的置换在中等温度(18℃)下发生,但在4℃时不发生。值得注意的是,在用[³H]E2或配体预孵育的细胞提取物中,交换以较低的速率进行。抗雌激素RU 39,411和RU 58,668似乎特别难以被置换。在全细胞实验中也记录到了如此低的交换率,尽管程度比预孵育细胞的提取物中更高。酶免疫测定表明,主要交换的缺失不能归因于ER损失。此外,结合配体的置换似乎与其对受体的结合亲和力无关。这些数据表明,雌激素和抗雌激素的结合通过至少一种因子(共激活剂或共抑制剂)得以稳定,从而将受体分子固定在一种对后续交换具有相对抗性的构象中。快速蛋白质液相色谱(FPLC)和孕激素受体(PgR)诱导显示,相当一部分保持足够灵活状态的ER仍能够交换并转导置换配体的转录信息。

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