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胰岛素样生长因子结合蛋白-3对胰岛素样生长因子(IGF)作用的增强:潜在机制研究

Potentiation of insulin-like growth factor (IGF) action by IGF-binding protein-3: studies of underlying mechanism.

作者信息

Conover C A

机构信息

Endocrine Research Unit, Mayo Clinic, Rochester, Minnesota 55905.

出版信息

Endocrinology. 1992 Jun;130(6):3191-9. doi: 10.1210/endo.130.6.1375895.

Abstract

In this study we investigated the mechanism(s) by which insulin-like growth factor-binding protein-3 (IGFBP-3) potentiates IGF-I action in cultured bovine fibroblasts. Preincubation of cells with glycosylated or nonglycosylated recombinant human IGFBP-3 enhanced responsiveness to IGF-I in a time-dependent manner. A preincubation period of at least 24 h with IGFBP-3 was required to see a significant effect. Pretreatment with IGFBP-3 for 72 h resulted in a 2- to 4-fold augmentation of IGF-I-stimulated [3H]aminoisobutyric acid uptake; IGFBP-3 had no effect on basal [3H]aminoisobutyric acid uptake. During the preincubation period, exogenous IGFBP-3 associated with the fibroblast surface and exhibited time-dependent processing to lower mol wt forms that retained the ability to bind radiolabeled IGF-I. Initial surface adherence (preincubation time of 24 h or less) was readily reversible. However, IGFBP-3, once processed, appeared to be closely associated with the cell. After 72 h of exposure to bovine fibroblasts, cell-associated IGFBP-3 had a 10-fold lower affinity for IGF-I compared to intact IGFBP-3 in solution. In addition, incubation of bovine fibroblasts with IGFBP-3 had modifying effects on type I IGF receptor-mediated signalling because 1) the bioeffectiveness of [Gln3,Ala4,Tyr15,Leu16]IGF-I and insulin, IGF-I receptor activators with little or no affinity for IGFBP-3, was potentiated by preincubation with IGFBP-3; and 2) fibroblast responsiveness to IGF-I analogs with different affinities for the type I IGF receptor was enhanced in direct relation to the ability of the peptide to bind to the receptor. There was no evidence for an increase in receptor number or affinity as a result of IGFBP-3 treatment. These data suggest that IGFBP-3 potentiation of IGF-I action in bovine fibroblasts may involve changes in IGFBP-3 and type I IGF receptor responsiveness. Thus, cell-associated IGFBP-3 may provide a mechanism for optimal presentation of IGF-I to its receptor as well as a means to heighten receptor reactivity to IGF-I and related peptides.

摘要

在本研究中,我们探究了胰岛素样生长因子结合蛋白-3(IGFBP-3)增强培养的牛成纤维细胞中IGF-I作用的机制。用糖基化或非糖基化重组人IGFBP-3对细胞进行预孵育,以时间依赖性方式增强了细胞对IGF-I的反应性。需要用IGFBP-3预孵育至少24小时才能观察到显著效果。用IGFBP-3预处理72小时导致IGF-I刺激的[³H]氨基异丁酸摄取增加2至4倍;IGFBP-3对基础[³H]氨基异丁酸摄取无影响。在预孵育期间,外源性IGFBP-3与成纤维细胞表面结合,并呈现出时间依赖性的加工过程,形成保留结合放射性标记IGF-I能力的较低分子量形式。最初的表面黏附(预孵育时间为24小时或更短)很容易逆转。然而,一旦加工,IGFBP-3似乎与细胞紧密结合。在暴露于牛成纤维细胞72小时后,与细胞相关的IGFBP-3对IGF-I的亲和力比溶液中的完整IGFBP-3低10倍。此外,用IGFBP-3孵育牛成纤维细胞对I型IGF受体介导的信号传导有调节作用,因为:1)[Gln3,Ala4,Tyr15,Leu16]IGF-I和胰岛素(对IGFBP-3几乎没有或没有亲和力的IGF-I受体激活剂)的生物有效性通过与IGFBP-3预孵育而增强;2)成纤维细胞对I型IGF受体具有不同亲和力的IGF-I类似物的反应性增强,这与该肽结合受体的能力直接相关。没有证据表明IGFBP-3处理会导致受体数量或亲和力增加。这些数据表明,IGFBP-3增强牛成纤维细胞中IGF-I作用可能涉及IGFBP-3和I型IGF受体反应性的变化。因此,与细胞相关的IGFBP-3可能为将IGF-I最佳呈递给其受体提供一种机制,以及增强受体对IGF-I和相关肽的反应性的一种手段。

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