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胰岛素样生长因子2信使核糖核酸结合蛋白3通过对……的翻译调控影响对抗胰岛素样生长因子系统药物的敏感性 。 (原文句末不完整)

Insulin-Like Growth Factor 2 mRNA-Binding Protein 3 Influences Sensitivity to Anti-IGF System Agents Through the Translational Regulation of .

作者信息

Mancarella Caterina, Pasello Michela, Manara Maria Cristina, Toracchio Lisa, Sciandra Evelina Fiorenza, Picci Piero, Scotlandi Katia

机构信息

CRS Development of Biomolecular Therapies, Experimental Oncology Laboratory, Orthopedic Rizzoli Institute, Bologna, Italy.

Pathology Section, Orthopedic Rizzoli Institute, Bologna, Italy.

出版信息

Front Endocrinol (Lausanne). 2018 Apr 20;9:178. doi: 10.3389/fendo.2018.00178. eCollection 2018.

Abstract

Insulin-like growth factor 2 (IGF2) mRNA-binding protein 3 (IGF2BP3) is an oncofetal protein that binds RNA, thereby influencing the fate of target transcripts. IGF2BP3 is synthesized in cancer, where it promotes proliferation, drug resistance, and metastasis both IGF2-dependent and IGF2-independent mechanisms. Ewing sarcoma (ES) is a rare bone and soft tissue tumor in which the IGF system plays a pivotal role. This study aimed to investigate the effect of IGF2BP3 on the regulation of the IGF system in ES. Among the components of the IGF axis, a direct significant correlation was identified between IGF2BP3 and IGF1R at mRNA and protein levels in two independent series of clinical specimens from patients with localized ES. After the formal demonstration of a direct association between IGF2BP3 and mRNA using ribo-immunoprecipitation assay, we performed studies using A673 and TC-71 ES cell lines to demonstrate that IGF2BP3 loss promotes the downregulation of IGF1R and a decreased biological response to IGF1, represented by reduced migration and cell growth. Additionally, the compensatory activation of insulin receptor (IR) and its mitogenic ligand IGF2 is triggered in some but not all cell lines in response to IGF2BP3-mediated IGF1R loss. These findings have therapeutic implications because cells with a decreased expression of IGF2BP3/IGF1R axis but an increased expression of the IR/IGF2 loop display higher sensitivity to the dual inhibitor OSI-906 than do control cells. Therefore, studies on IGF2BP3, which was confirmed as a post-transcriptional regulator of IGF1R, provide a step forward in the identification of new mechanisms regulating the IGF system. In addition, our results demonstrate that the detection of IGF2BP3 expression should be combined with the assessment of the IGF1R/IR ratio to predict cell responses to anti-IGF1R/IR agents.

摘要

胰岛素样生长因子2(IGF2)mRNA结合蛋白3(IGF2BP3)是一种癌胚蛋白,可结合RNA,从而影响靶转录本的命运。IGF2BP3在癌症中合成,在那里它通过依赖IGF2和不依赖IGF2的机制促进增殖、耐药和转移。尤因肉瘤(ES)是一种罕见的骨和软组织肿瘤,其中IGF系统起关键作用。本研究旨在探讨IGF2BP3对ES中IGF系统调节的影响。在IGF轴的组成部分中,在来自局限性ES患者的两个独立系列临床标本中,在mRNA和蛋白质水平上确定了IGF2BP3与IGF1R之间存在直接显著相关性。在使用核糖免疫沉淀试验正式证明IGF2BP3与mRNA之间存在直接关联后,我们使用A673和TC-71 ES细胞系进行研究,以证明IGF2BP3缺失促进IGF1R的下调以及对IGF1的生物学反应降低,表现为迁移和细胞生长减少。此外,在一些但不是所有细胞系中,响应IGF2BP3介导的IGF1R缺失会触发胰岛素受体(IR)及其促有丝分裂配体IGF2的代偿性激活。这些发现具有治疗意义,因为IGF2BP3/IGF1R轴表达降低但IR/IGF2环表达增加的细胞比对照细胞对双重抑制剂OSI-906表现出更高的敏感性。因此,对被确认为IGF1R转录后调节因子的IGF2BP3的研究为确定调节IGF系统的新机制向前迈进了一步。此外,我们的结果表明,检测IGF2BP3表达应与评估IGF1R/IR比率相结合,以预测细胞对抗IGF1R/IR药物的反应。

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