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Leveraging the Role of the Metastatic Associated Protein Anterior Gradient Homologue 2 in Unfolded Protein Degradation: A Novel Therapeutic Biomarker for Cancer

机译:利用转移相关蛋白前梯度同源物2在未折叠的蛋白降解中的作用:一种新型的癌症治疗生物标志物。

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摘要

Effective diagnostic, prognostic and therapeutic biomarkers can help in tracking disease progress, predict patients’ survival, and considerably affect the drive for successful clinical management. The present review aims to determine how the metastatic-linked protein anterior gradient homologue 2 (AGR2) operates to affect cancer progression, and to identify associated potential diagnostic, prognostic and therapeutic biomarkers, particularly in central nervous system (CNS) tumors. Studies that show a high expression level of AGR2, and associate the protein expression with the resilience to chemotherapeutic treatments or with poor cancer survival, are reported. The primary protein structures of the seven variants of AGR2, including their functional domains, are summarized. Based on experiments in various biological models, this review shows an orchestra of multiple molecules that regulate AGR2 expression, including a feedback loop with p53. The AGR2-associated molecular functions and pathways including genomic integrity, proliferation, apoptosis, angiogenesis, adhesion, migration, stemness, and inflammation, are detailed. In addition, the mechanisms that can enable the rampant oncogenic effects of AGR2 are clarified. The different strategies used to therapeutically target AGR2-positive cancer cells are evaluated in light of the current evidence. Moreover, novel associated pathways and clinically relevant deregulated genes in AGR2 high CNS tumors are identified using a meta-analysis approach.
机译:有效的诊断,预后和治疗生物标志物可以帮助追踪疾病进展,预测患者的生存情况,并极大地影响成功进行临床管理的动力。本综述旨在确定转移相关蛋白前梯度同源物2(AGR2)如何影响癌症的进展,并确定相关的潜在诊断,预后和治疗生物标志物,尤其是在中枢神经系统(CNS)肿瘤中。据报道,有研究表明AGR2的表达水平很高,并且蛋白质的表达与化疗治疗的适应性或较差的癌症存活率相关。总结了AGR2的七个变体的主要蛋白质结构,包括其功能结构域。基于各种生物学模型的实验,该综述显示了调节AGR2表达的多个分子的乐团,包括带有p53的反馈环。详细介绍了与AGR2相关的分子功能和途径,包括基因组完整性,增殖,凋亡,血管生成,粘附,迁移,干和炎症。此外,阐明了可以使AGR2产生广泛致癌作用的机制。根据当前证据,评估了用于治疗性靶向AGR2阳性癌细胞的不同策略。此外,使用荟萃分析方法鉴定了AGR2高中枢神经系统肿瘤中的新型相关途径和临床相关的失调基因。

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