TRIM36, a novel androgen-responsive gene, enhances anti-androgen efficacy against prostate cancer by inhibiting MAPK/ERK signaling pathways

Chao Liang; Shangqian Wang; Chao Qin; Meilin Bao; Gong Cheng; Bianjiang Liu; Pengfei Shao; Qiang Lv; Ninghong Song; Lixin Hua; Min Gu; Jie Li; Zengjun Wang

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TRIM36, a novel androgen-responsive gene, enhances anti-androgen efficacy against prostate cancer by inhibiting MAPK/ERK signaling pathways

机译：TRIM36是一种新型雄激素反应性基因，可通过抑制MAPK / ERK信号通路来增强抗前列腺癌的抗雄激素功效

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Hormone therapy drugs, such as bicalutamide and enzalutamide, directed against prostate cancer focus on androgen receptor (AR) signaling and are initially effective, but the disease progresses to lethality as resistance to these drugs develops. A method to prolong the drug response time and improve the drug efficacy is still unavailable. TRIM36 was reported as a novel androgen signaling target gene and is upregulated in prostate cancer. In this study, we found that 63.4% (64/95) of PCa in TMA expressed the TRIM36 protein. Interestingly, patients with negative TRIM36 expression had a shorter biochemical recurrence-free survival. TRIM36 expression was significantly associated with the Gleason score (P?=?0.005), delayed prostate cancer cell cycle progression and inhibited cell proliferation in vitro and in vivo, and these effects were mediated via inhibition of the MAPK/ERK phosphorylation pathway. Remarkably, we found that rescuing the expression of TRIM36 during anti-androgen therapy could improve the drug efficacy. Collectively, TRIM36 is a novel androgen-responsive gene, and it dramatically enhanced the efficacy of anti-androgen drugs against prostate cancer.

机译：针对前列腺癌的激素治疗药物，例如比卡鲁胺和恩杂鲁胺，侧重于雄激素受体（AR）信号传导，最初有效，但随着对这些药物产生耐药性，疾病发展为致死性。仍然没有延长药物反应时间并改善药物功效的方法。据报道，TRIM36是一种新型的雄激素信号传导靶基因，在前列腺癌中被上调。在这项研究中，我们发现TMA中63.4％（64/95）的PCa表达了TRIM36蛋白。有趣的是，TRIM36表达阴性的患者的生化无复发生存期较短。 TRIM36的表达与格里森评分（P≥0.005），前列腺癌细胞周期进程的延迟和体内外抑制均显着相关，这些作用是通过抑制MAPK / ERK磷酸化途径来介导的。值得注意的是，我们发现在抗雄激素治疗期间挽救TRIM36的表达可以提高药物疗效。总的来说，TRIM36是一个新的雄激素反应基因，它显着增强了抗雄激素药物对抗前列腺癌的功效。

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《Cell death & disease.》 |2018年第2期|共页
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Chao Liang; Shangqian Wang; Chao Qin; Meilin Bao; Gong Cheng; Bianjiang Liu; Pengfei Shao; Qiang Lv; Ninghong Song; Lixin Hua; Min Gu; Jie Li; Zengjun Wang;
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中图分类细胞生物学;
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机译：异智激肽原蛋白通过下调JAK1 / STAT1，IRF3 / MyD88，ERK / MAPK，JNK / MAPK和PI3K / Akt信号通路的激活抑制肝细胞中干扰素-γ诱导基因的表达
2. 17beta-Estradiol differentially regulates androgen-responsive genes through estrogen receptor-beta- and extracellular-signal regulated kinase-dependent pathways in LNCaP human prostate cancer cells. [J] . Takahashi Y, Perkins SN, Hursting SD, Molecular Carcinogenesis . 2007,第2期

机译：17β-雌二醇通过LNCaP人前列腺癌细胞中的雌激素受体-β和细胞外信号调节的激酶依赖性途径，差异调节雄激素应答基因。
3. A Chinese herbal formula, Yi-Qi-Fu-Sheng, inhibits migration/invasion of colorectal cancer by down-regulating MMP-2/9 via inhibiting the activation of ERK/MAPK signaling pathways [J] . Wanli Deng, Hua Sui, Qiaolin Wang, BMC Complementary and Alternative Medicine . 2013,第1期

机译：益气复生中药通过抑制ERK / MAPK信号通路的激活而下调MMP-2 / 9，从而抑制结直肠癌的迁移/侵袭。
4. INHIBITORS OF THE RAS/ERK SIGNALING PATHWAY INCORPORATING THE FXF MOTIF FOR FHE DEVELOPMENT OF ANTICANCER DRUGS [C] . Theodore Skarlas, EugeniaJPanou-Pomonis, Dimitrios Krikorian the European Peptide Symposium . 2007

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5. Targeting Ras and Rho family GTPases for the treatment of cancer through inhibition of CAAX-signaled modifications and the ERK MAPK pathway. [D] . Roberts, Patrick J. 2007

机译：通过抑制CAAX信号修饰和ERK MAPK途径，靶向Ras和Rho家族GTPases治疗癌症。
6. TRIM36 a novel androgen-responsive gene enhances anti-androgen efficacy against prostate cancer by inhibiting MAPK/ERK signaling pathways [O] . Chao Liang, Shangqian Wang, Chao Qin, 2018

机译：TRIM36是一种新的雄激素应答基因通过抑制MAPK / ERK信号通路增强抗雄激素的抗前列腺癌功效
7. TRIM36, a novel androgen-responsive gene, enhances anti-androgen efficacy against prostate cancer by inhibiting MAPK/ERK signaling pathways [O] . Chao Liang, Shangqian Wang, Chao Qin, 2018

机译：Trim36是一种新的雄激素响应基因，通过抑制MAPK / ERK信号通路来增强针对前列腺癌的抗雄激素疗效

TRIM36, a novel androgen-responsive gene, enhances anti-androgen efficacy against prostate cancer by inhibiting MAPK/ERK signaling pathways

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