Tankyrase Inhibition Blocks Wnt/beta-Catenin Pathway and Reverts Resistance to PI3K and AKT Inhibitors in the Treatment of Colorectal Cancer

Arques Oriol; Chicote Irene; Puig Isabel; Tenbaum Stephan P.; Argiles Guillem; Dienstmann Rodrigo; Fernandez Natalia; Caratu Ginevra; Matito Judit; Silberschmidt Daniel; Rodon Jordi; Landolfi Stefania; Prat Aleix; Espin Eloy; Charco Ramon; Nuciforo Paolo; Vivancos Ana; Shao Wenlin; Tabernero Josep; Palmer Hector G.

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Tankyrase Inhibition Blocks Wnt/beta-Catenin Pathway and Reverts Resistance to PI3K and AKT Inhibitors in the Treatment of Colorectal Cancer

机译：Tankyrase抑制作用可阻断Wnt /β-Catenin通路并恢复对PI3K和AKT抑制剂的抵抗性，以治疗结直肠癌。

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Purpose: Oncogenic mutations in the KRAS/PI3K/AKT pathway are one of the most frequent alterations in cancer. Although PI3K or AKT inhibitors show promising results in clinical trials, drug resistance frequently emerges. We previously revealed Wnt/beta-catenin signaling hyperactivation as responsible for such resistance in colorectal cancer. Here we investigate Wnt-mediated resistance in patients treated with PI3K or AKT inhibitors in clinical trials and evaluate the efficacy of a new Wnt/tankyrase inhibitor, NVP-TNKS656, to overcome such resistance.

机译：目的：KRAS / PI3K / AKT途径中的致癌突变是癌症中最常见的改变之一。尽管PI3K或AKT抑制剂在临床试验中显示出令人鼓舞的结果，但耐药性却经常出现。我们先前发现Wnt /β-catenin信号过度激活是造成这种结直肠癌耐药性的原因。在这里，我们在临床试验中研究了用PI3K或AKT抑制剂治疗的患者中Wnt介导的耐药性，并评估了新型Wnt / tankyrase抑制剂NVP-TNKS656克服此类耐药性的功效。

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《Clinical cancer research: an official journal of the American Association for Cancer Research 》 |2016年第3期| 共13页
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Arques Oriol; Chicote Irene; Puig Isabel; Tenbaum Stephan P.; Argiles Guillem; Dienstmann Rodrigo; Fernandez Natalia; Caratu Ginevra; Matito Judit; Silberschmidt Daniel; Rodon Jordi; Landolfi Stefania; Prat Aleix; Espin Eloy; Charco Ramon; Nuciforo Paolo; Vivancos Ana; Shao Wenlin; Tabernero Josep; Palmer Hector G.;
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1. Tankyrase Inhibition Blocks Wnt/beta-Catenin Pathway and Reverts Resistance to PI3K and AKT Inhibitors in the Treatment of Colorectal Cancer [J] . Arques Oriol, Chicote Irene, Puig Isabel, Clinical cancer research: an official journal of the American Association for Cancer Research . 2016 ,第3期

机译：Tankyrase抑制作用可阻断Wnt /β-Catenin通路并恢复对PI3K和AKT抑制剂的抵抗性，以治疗结直肠癌。
2. Pin1 inhibition potently suppresses gastric cancer growth and blocks PI3K/AKT and Wnt/beta-catenin oncogenic pathways [J] . Zhang Zhenzhen, Yu Weixing, Zheng Min, Molecular Carcinogenesis . 2019 ,第8期

机译：Pin1抑制效果抑制胃癌生长并阻断PI3K / AKT和WNT / Beta-catenin致癌途径
3. Knockdown of long non-coding RNA HOTAIR inhibits cisplatin resistance of gastric cancer cells through inhibiting the PI3K/Akt and Wnt/beta-catenin signaling pathways by up-regulating miR-34a [J] . Cheng Chuanyao, Qin Yaguang, Zhi Qiongjie, International Journal of Biological Macromolecules: Structure, Function and Interactions . 2018 ,第Pta2期

机译：长期非编码RNA HotaH的敲低通过抑制PI3K / AKT和WNT / Beta-catenin信号传导途径来抑制胃癌细胞的顺铂抗性，通过上调miR-34a
4. M2-A, A Novel Amonafide Analogue, Induces Apoptosis and G2-M Arrest via Decreasing Topoisomerase LIa Activity and Inhibits PI3K/Akt Pathway on HL60 Cells [C] . The 12th Asian Pacific Confederation of Chemical Engineering Congress(第十二届亚太化工联盟大会暨化工展览会)论文集 . 2008

机译：M2-A，一种新颖的阿莫那肽类似物，通过降低拓扑异构酶LIa活性诱导HL60细胞凋亡和G2-M逮捕并抑制PI3K / Akt途径。
5. Jade-1 acts through the PI3K-AKT pathway and the Wnt pathway to inhibit renal cancer growth. [D] . Zeng, Liling. 2011

机译：Jade-1通过PI3K-AKT途径和Wnt途径抑制肾癌的生长。
6. Inhibition of miR-19a partially reversed the resistance of colorectal cancer to oxaliplatin via PTEN/PI3K/AKT pathway [O] . Ye Zhang, Xinxin Liu, Junying Zhang, 2020

机译：miR-19a的抑制通过PTEN / PI3K / AKT途径部分逆转了结直肠癌对奥沙利铂的耐药性
7. Combination treatment of ligustrazine piperazine derivate DLJ14 and adriamycin inhibits progression of resistant breast cancer through inhibition of the EGFR/PI3K/Akt survival pathway and induction of apoptosis [O] . Jinhua Chen, Wenfang Wang, Hongyuan Wang, 2014

机译：Ligustrazine Piperazine衍生物DLJ14和Adriamycin的组合治疗通过抑制EGFR / PI3K / AKT存活途径和诱导细胞凋亡，抑制抗性乳腺癌的进展

Tankyrase Inhibition Blocks Wnt/beta-Catenin Pathway and Reverts Resistance to PI3K and AKT Inhibitors in the Treatment of Colorectal Cancer

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