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Posttranscriptional Upregulation of IDH1 by HuR Establishes a Powerful Survival Phenotype in Pancreatic Cancer Cells.HuR对异柠檬酸脱氢酶1(IDH1)的转录后上调在胰腺癌细胞中建立了强大的生存表型。
Cancer Res. 2017 Aug 15;77(16):4460-4471. doi: 10.1158/0008-5472.CAN-17-0015. Epub 2017 Jun 26.
2
PARP1 promotes gene expression at the post-transcriptiona level by modulating the RNA-binding protein HuR.PARP1 通过调节 RNA 结合蛋白 HuR 促进转录后水平的基因表达。
Nat Commun. 2017 Mar 8;8:14632. doi: 10.1038/ncomms14632.
3
CRISPR Knockout of the HuR Gene Causes a Xenograft Lethal Phenotype.HuR基因的CRISPR敲除导致异种移植致死表型。
Mol Cancer Res. 2017 Jun;15(6):696-707. doi: 10.1158/1541-7786.MCR-16-0361. Epub 2017 Feb 27.
4
WEE1 inhibition in pancreatic cancer cells is dependent on DNA repair status in a context dependent manner.在依赖上下文的方式中,胰腺癌细胞中的 WEE1 抑制取决于 DNA 修复状态。
Sci Rep. 2016 Sep 12;6:33323. doi: 10.1038/srep33323.
5
GPRC5A is a potential oncogene in pancreatic ductal adenocarcinoma cells that is upregulated by gemcitabine with help from HuR.GPRC5A是胰腺导管腺癌细胞中的一种潜在致癌基因,在HuR的帮助下,它会被吉西他滨上调。
Cell Death Dis. 2016 Jul 14;7(7):e2294. doi: 10.1038/cddis.2016.169.
6
HuR Contributes to TRAIL Resistance by Restricting Death Receptor 4 Expression in Pancreatic Cancer Cells.HuR通过限制胰腺癌细胞中死亡受体4的表达促进对TRAIL的抗性。
Mol Cancer Res. 2016 Jul;14(7):599-611. doi: 10.1158/1541-7786.MCR-15-0448. Epub 2016 Apr 6.
7
Insights from HuR biology point to potential improvement for second-line ovarian cancer therapy.HuR生物学的见解为二线卵巢癌治疗带来了潜在的改善方向。
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8
Cis-acting elements in its 3' UTR mediate post-transcriptional regulation of KRAS.其3'非翻译区中的顺式作用元件介导KRAS的转录后调控。
Oncotarget. 2016 Mar 15;7(11):11770-84. doi: 10.18632/oncotarget.7599.
9
The mRNA-binding protein HuR promotes hypoxia-induced chemoresistance through posttranscriptional regulation of the proto-oncogene PIM1 in pancreatic cancer cells.信使核糖核酸结合蛋白HuR通过对胰腺癌细胞中原癌基因PIM1的转录后调控促进缺氧诱导的化疗耐药性。
Oncogene. 2016 May;35(19):2529-41. doi: 10.1038/onc.2015.325. Epub 2015 Sep 21.
10
Cardiomyocyte-specific overexpression of the ubiquitin ligase Wwp1 contributes to reduction in Connexin 43 and arrhythmogenesis.泛素连接酶Wwp1在心肌细胞中的特异性过表达导致连接蛋白43减少并引发心律失常。
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胰腺中高表达的 HuR 促进类似胰腺炎的炎症微环境,从而促进肿瘤发展。

Elevated HuR in Pancreas Promotes a Pancreatitis-Like Inflammatory Microenvironment That Facilitates Tumor Development.

机构信息

Lankenau Institute for Medical Research, Wynnewood, Pennsylvania, USA.

Sidney Kimmel Cancer Center at the Jefferson Pancreatic, Biliary, and Related Cancer Center, Thomas Jefferson University, Philadelphia, Pennsylvania, USA.

出版信息

Mol Cell Biol. 2018 Jan 16;38(3). doi: 10.1128/MCB.00427-17. Print 2018 Feb 1.

DOI:10.1128/MCB.00427-17
PMID:29133460
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5770537/
Abstract

Human antigen R (ELAVL1; HuR) is perhaps the best-characterized RNA-binding protein. Through its overexpression in various tumor types, HuR promotes posttranscriptional regulation of target genes in multiple core signaling pathways associated with tumor progression. The role of HuR overexpression in pancreatic tumorigenesis is unknown and led us to explore the consequences of HuR overexpression using a novel transgenic mouse model that has a >2-fold elevation of pancreatic HuR expression. Histologically, HuR-overexpressing pancreas displays a fibroinflammatory response and other pathological features characteristic of chronic pancreatitis. This pathology is reflected in changes in the pancreatic gene expression profile due, in part, to genes whose expression changes as a consequence of direct binding of their respective mRNAs to HuR. Older mice develop pancreatic steatosis and severe glucose intolerance. Elevated HuR cooperated with mutant K-ras to result in a 3.4-fold increase in pancreatic ductal adenocarcinoma (PDAC) incidence compared to PDAC presence in K-ras alone. These findings implicate HuR as a facilitator of pancreatic tumorigenesis, especially in the setting of inflammation, and a novel therapeutic target for pancreatitis treatment.

摘要

人类抗原 R(ELAVL1;HuR)可能是研究最透彻的 RNA 结合蛋白。通过在各种肿瘤类型中的过表达,HuR 促进了与肿瘤进展相关的多个核心信号通路中靶基因的转录后调控。HuR 过表达在胰腺肿瘤发生中的作用尚不清楚,这促使我们使用一种新型转基因小鼠模型来探索 HuR 过表达的后果,该模型中胰腺 HuR 的表达水平升高了 2 倍以上。组织学上,HuR 过表达的胰腺显示出纤维化炎症反应和其他特征性的慢性胰腺炎病理特征。这种病理学反映在胰腺基因表达谱的变化中,部分原因是由于其各自的 mRNA 与 HuR 直接结合,导致这些基因的表达发生变化。老年小鼠发生胰腺脂肪变性和严重的葡萄糖不耐受。与单独的 K-ras 相比,高表达的 HuR 与突变型 K-ras 共同作用,导致胰腺导管腺癌(PDAC)的发生率增加了 3.4 倍。这些发现表明 HuR 是胰腺肿瘤发生的促进因子,特别是在炎症的情况下,并且是胰腺炎治疗的一个新的治疗靶点。