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Pyruvate Kinase M2: A Potential Target for Regulating Inflammation.丙酮酸激酶M2:调节炎症的潜在靶点。
Front Immunol. 2016 Apr 21;7:145. doi: 10.3389/fimmu.2016.00145. eCollection 2016.
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OCT-4: a novel estrogen receptor-α collaborator that promotes tamoxifen resistance in breast cancer cells.OCT-4:一种新型雌激素受体-α共激活因子,可促进乳腺癌细胞对他莫昔芬产生耐药性。
Oncogene. 2016 Nov 3;35(44):5722-5734. doi: 10.1038/onc.2016.105. Epub 2016 Apr 11.
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PKM2 and cancer: The function of PKM2 beyond glycolysis.丙酮酸激酶M2与癌症:丙酮酸激酶M2在糖酵解之外的功能
Oncol Lett. 2016 Mar;11(3):1980-1986. doi: 10.3892/ol.2016.4168. Epub 2016 Jan 29.
5
Oncoprotein HBXIP Modulates Abnormal Lipid Metabolism and Growth of Breast Cancer Cells by Activating the LXRs/SREBP-1c/FAS Signaling Cascade.癌蛋白 HBXIP 通过激活 LXRs/SREBP-1c/FAS 信号级联来调节乳腺癌细胞的异常脂质代谢和生长。
Cancer Res. 2016 Aug 15;76(16):4696-707. doi: 10.1158/0008-5472.CAN-15-1734. Epub 2016 Mar 15.
6
The oncoprotein HBXIP up-regulates FGF4 through activating transcriptional factor Sp1 to promote the migration of breast cancer cells.癌蛋白HBXIP通过激活转录因子Sp1上调FGF4,从而促进乳腺癌细胞的迁移。
Biochem Biophys Res Commun. 2016 Feb 26;471(1):89-94. doi: 10.1016/j.bbrc.2016.01.174. Epub 2016 Jan 29.
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HBXIP and LSD1 Scaffolded by lncRNA Hotair Mediate Transcriptional Activation by c-Myc.HBXIP 和 LSD1 通过长链非编码 RNA Hotair 支架介导 c-Myc 的转录激活。
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Deacetylation of tumor-suppressor MST1 in Hippo pathway induces its degradation through HBXIP-elevated HDAC6 in promotion of breast cancer growth.在促进乳腺癌生长过程中,Hippo信号通路中肿瘤抑制因子MST1的去乙酰化通过HBXIP上调的HDAC6诱导其降解。
Oncogene. 2016 Aug 4;35(31):4048-57. doi: 10.1038/onc.2015.476. Epub 2015 Dec 14.
9
High Expression of Pyruvate Kinase M2 is Associated with Chemosensitivity to Epirubicin and 5-Fluorouracil in Breast Cancer.丙酮酸激酶M2的高表达与乳腺癌对表柔比星和5-氟尿嘧啶的化疗敏感性相关。
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10
The oncoprotein HBXIP promotes glucose metabolism reprogramming via downregulating SCO2 and PDHA1 in breast cancer.癌蛋白HBXIP通过下调乳腺癌中的SCO2和PDHA1促进葡萄糖代谢重编程。
Oncotarget. 2015 Sep 29;6(29):27199-213. doi: 10.18632/oncotarget.4508.

癌蛋白 HBXIP 通过转录因子 E2F1 诱导 PKM2 的表达,从而促进 ER 阳性乳腺癌细胞的增殖。

Oncoprotein HBXIP induces PKM2 via transcription factor E2F1 to promote cell proliferation in ER-positive breast cancer.

机构信息

Department of Biochemistry, State Key Laboratory of Medicinal Chemical Biology, College of Life Sciences, Nankai University, Tianjin, 300071, China.

Department of Cancer Research, State Key Laboratory of Medicinal Chemical Biology, College of Life Sciences, Nankai University, Tianjin, 300071, China.

出版信息

Acta Pharmacol Sin. 2019 Apr;40(4):530-538. doi: 10.1038/s41401-018-0015-9. Epub 2018 Jun 20.

DOI:10.1038/s41401-018-0015-9
PMID:29925919
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6462016/
Abstract

We have reported that hepatitis B X-interacting protein (HBXIP, also termed LAMTOR5) can act as an oncogenic transcriptional co-activator to modulate gene expression, promoting breast cancer development. Pyruvate kinase muscle isozyme M2 (PKM2), encoded by PKM gene, has emerged as a key oncoprotein in breast cancer. Yet, the regulatory mechanism of PKM2 is still unexplored. Here, we report that HBXIP can upregulate PKM2 to accelerate proliferation of estrogen receptor positive (ER+) breast cancer. Immunohistochemistry analysis using breast cancer tissue microarray uncovered a positive association between the expression of HBXIP and PKM2. We also discovered that PKM2 expression was positively related with HBXIP expression in clinical breast cancer patients by real-time PCR assay. Interestingly, in ER+ breast cancer cells, HBXIP was capable of upregulating PKM2 expression at mRNA and protein levels in a dose-dependent manner, as well as increasing the activity of PKM promoter. Mechanistically, HBXIP could stimulate PKM promoter through binding to the -779/-579 promoter region involving co-activation of E2F transcription factor 1 (E2F1). In function, cell viability, EdU, colony formation, and xenograft tumor growth assays showed that HBXIP contributed to accelerating cell proliferation through PKM2 in ER+ breast cancer. Collectively, we conclude that HBXIP induces PKM2 through transcription factor E2F1 to facilitate ER+ breast cancer cell proliferation. We provide new evidence for the mechanism of transcription regulation of PKM2 in promotion of breast cancer progression.

摘要

我们曾报道乙型肝炎 X 交互蛋白(HBXIP,也称为 LAMTOR5)可作为致癌转录共激活因子,调节基因表达,促进乳腺癌的发展。丙酮酸激酶肌肉同工酶 M2(PKM2)由 PKM 基因编码,已成为乳腺癌中的关键癌蛋白。然而,PKM2 的调控机制仍未被探索。在这里,我们报告 HBXIP 可上调 PKM2 以加速雌激素受体阳性(ER+)乳腺癌的增殖。使用乳腺癌组织微阵列的免疫组织化学分析揭示了 HBXIP 和 PKM2 表达之间存在正相关。我们还通过实时 PCR 检测发现,在临床乳腺癌患者中,PKM2 的表达与 HBXIP 的表达呈正相关。有趣的是,在 ER+乳腺癌细胞中,HBXIP 能够以剂量依赖性方式上调 PKM2 的 mRNA 和蛋白表达水平,并增加 PKM 启动子的活性。在机制上,HBXIP 可以通过结合 -779/-579 启动子区域来刺激 PKM 启动子,从而涉及 E2F 转录因子 1(E2F1)的共激活。在功能上,细胞活力、EdU、集落形成和异种移植肿瘤生长实验表明,HBXIP 通过 PKM2 促进 ER+乳腺癌细胞的增殖。总之,我们得出结论,HBXIP 通过转录因子 E2F1 诱导 PKM2 促进 ER+乳腺癌细胞的增殖。我们为 PKM2 在促进乳腺癌进展中的转录调控机制提供了新的证据。