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本文引用的文献

1
Targeted Therapy and Mechanisms of Drug Resistance in Breast Cancer.乳腺癌的靶向治疗与耐药机制
Cancers (Basel). 2023 Feb 19;15(4):1320. doi: 10.3390/cancers15041320.
2
Beyond HER2: Targeting the ErbB receptor family in breast cancer.超越 HER2:在乳腺癌中靶向 ErbB 受体家族。
Cancer Treat Rev. 2022 Sep;109:102436. doi: 10.1016/j.ctrv.2022.102436. Epub 2022 Jul 15.
3
SON drives oncogenic RNA splicing in glioblastoma by regulating PTBP1/PTBP2 switching and RBFOX2 activity.SON 通过调控 PTBP1/PTBP2 转换和 RBFOX2 活性来驱动神经胶质瘤中的致癌 RNA 剪接。
Nat Commun. 2021 Sep 21;12(1):5551. doi: 10.1038/s41467-021-25892-x.
4
SON inhibits megakaryocytic differentiation via repressing RUNX1 and the megakaryocytic gene expression program in acute megakaryoblastic leukemia.SON 通过抑制 RUNX1 和巨核细胞基因表达程序抑制急性巨核细胞白血病中的巨核细胞分化。
Cancer Gene Ther. 2021 Sep;28(9):1000-1015. doi: 10.1038/s41417-020-00262-9. Epub 2020 Nov 27.
5
HER2 splice variants in breast cancer: investigating their impact on diagnosis and treatment outcomes.乳腺癌中的HER2剪接变体:探究其对诊断和治疗结果的影响。
Oncotarget. 2020 Nov 17;11(46):4338-4357. doi: 10.18632/oncotarget.27789.
6
SON haploinsufficiency causes impaired pre-mRNA splicing of CAKUT genes and heterogeneous renal phenotypes.SOX 基因单倍体不足导致 CAKUT 基因的前体 mRNA 剪接受损和肾脏表型异质性。
Kidney Int. 2019 Jun;95(6):1494-1504. doi: 10.1016/j.kint.2019.01.025. Epub 2019 Mar 15.
7
HER2 expression identifies dynamic functional states within circulating breast cancer cells.HER2表达可识别循环乳腺癌细胞内的动态功能状态。
Nature. 2016 Sep 1;537(7618):102-106. doi: 10.1038/nature19328. Epub 2016 Aug 24.
8
De Novo Mutations in SON Disrupt RNA Splicing of Genes Essential for Brain Development and Metabolism, Causing an Intellectual-Disability Syndrome.SON基因的新生突变破坏大脑发育和代谢所必需基因的RNA剪接,导致一种智力残疾综合征。
Am J Hum Genet. 2016 Sep 1;99(3):711-719. doi: 10.1016/j.ajhg.2016.06.029. Epub 2016 Aug 18.
9
Proteogenomics connects somatic mutations to signalling in breast cancer.蛋白质基因组学将体细胞突变与乳腺癌中的信号传导联系起来。
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10
SON and Its Alternatively Spliced Isoforms Control MLL Complex-Mediated H3K4me3 and Transcription of Leukemia-Associated Genes.SON及其可变剪接异构体控制MLL复合物介导的H3K4me3和白血病相关基因的转录。
Mol Cell. 2016 Mar 17;61(6):859-73. doi: 10.1016/j.molcel.2016.02.024.

SON 是一种必需的 RNA 剪接因子,可促进乳腺癌中 ErbB2 和 ErbB3 的表达。

SON is an essential RNA splicing factor promoting ErbB2 and ErbB3 expression in breast cancer.

机构信息

Mitchell Cancer Institute, University of South Alabama, Mobile, AL, USA.

Research Institute, National Cancer Center, 323 Ilsan-ro, Goyang-si, Gyeonggido, Republic of Korea.

出版信息

Br J Cancer. 2024 Nov;131(9):1437-1449. doi: 10.1038/s41416-024-02853-x. Epub 2024 Sep 23.

DOI:10.1038/s41416-024-02853-x
PMID:39313574
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11519869/
Abstract

BACKGROUND

In breast cancer, ErbB receptors play a critical role, and overcoming drug resistance remains a major challenge in the clinic. However, intricate regulatory mechanisms of ErbB family genes are poorly understood. Here, we demonstrate SON as an ErbB-regulatory splicing factor and a novel therapeutic target for ErbB-positive breast cancer.

METHODS

SON and ErbB expression analyses using public database, patient tissue microarray, and cell lines were performed. SON knockdown assessed its impact on cell proliferation, apoptosis, kinase phosphorylation, RNA splicing, and in vivo tumour growth. RNA immunoprecipitation was performed to measure SON binding.

RESULTS

SON is highly expressed in ErbB2-positive breast cancer patient samples, inversely correlating with patient survival. SON knockdown induced intron retention in selective splice sites within ErbB2 and ErbB3 transcripts, impairing effective RNA splicing and reducing protein expression. SON disruption suppressed downstream kinase signalling of ErbB2/3, including the Akt, p38, and JNK pathways, with increased vulnerability in ErbB2-positive breast cancer cells compared to ErbB2-negative cells. SON silencing in ErbB2-positive breast cancer xenografts led to tumour regression in vivo.

CONCLUSION

We identified SON as a novel RNA splicing factor that plays a critical role in regulating ErbB2/3 expression, suggesting SON is an ideal therapeutic target in ErbB2-positive breast cancers.

摘要

背景

在乳腺癌中,ErbB 受体起着至关重要的作用,克服耐药性仍然是临床面临的主要挑战。然而,ErbB 家族基因的复杂调控机制仍知之甚少。在这里,我们证明 SON 是一种 ErbB 调节性剪接因子,也是 ErbB 阳性乳腺癌的一个新的治疗靶点。

方法

使用公共数据库、患者组织微阵列和细胞系进行 SON 和 ErbB 表达分析。通过 SON 敲低评估其对细胞增殖、凋亡、激酶磷酸化、RNA 剪接和体内肿瘤生长的影响。进行 RNA 免疫沉淀以测量 SON 结合。

结果

SON 在 ErbB2 阳性乳腺癌患者样本中高表达,与患者生存呈负相关。SON 敲低诱导 ErbB2 和 ErbB3 转录本中选择性剪接位点的内含子保留,从而破坏有效的 RNA 剪接并降低蛋白表达。SON 破坏抑制了 ErbB2/3 的下游激酶信号,包括 Akt、p38 和 JNK 途径,与 ErbB2 阴性细胞相比,ErbB2 阳性乳腺癌细胞的敏感性增加。SON 沉默在 ErbB2 阳性乳腺癌异种移植瘤中导致体内肿瘤消退。

结论

我们确定 SON 是一种新的 RNA 剪接因子,在调节 ErbB2/3 表达中起着关键作用,这表明 SON 是 ErbB2 阳性乳腺癌的理想治疗靶点。