OSU-A9, a potent indole-3-carbinol derivative, suppresses breast tumor growth by targeting the Akt-NF-kappaB pathway and stress response signaling.

Weng JR; Tsai CH; Omar HA

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OSU-A9, a potent indole-3-carbinol derivative, suppresses breast tumor growth by targeting the Akt-NF-kappaB pathway and stress response signaling.

机译：OSU-A9是有效的吲哚-3-甲醇衍生物，可通过靶向Akt-NF-kappaB途径和应激反应信号来抑制乳腺肿瘤的生长。

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The molecular heterogeneity of human tumors challenges the development of effective preventive and therapeutic strategies. To overcome this issue, a rational approach is the concomitant targeting of clinically relevant cellular abnormalities with combination therapy or a potent multi-targeted agent. OSU-A9 is a novel indole-3-carbinol derivative that retains the parent compound's ability to perturb multiple components of oncogenic signaling, but provides marked advantages in chemical stability and antitumor potency. Here, we show that OSU-A9 exhibits two orders of magnitude greater potency than indole-3-carbinol in inducing apoptosis in various breast cancer cell lines with distinct genetic abnormalities, including MCF-7, MDA-MB-231 and SKBR3, with the half maximal inhibitory concentration in the range of 1.2-1.8 microM vis-a-vis 200 microM for indole-3-carbinol. This differential potency was paralleled by OSU-A9's superior activity against multiple components of the Akt-nuclear factor-kappa B (NF-kappaB) and stress response signaling pathways. Notable among these were the increased estrogen receptor (ER)-beta/ERalpha expression ratio, reduced expression of HER2 and CXCR4 and the upregulation of aryl hydrocarbon receptor expression and its downstream target NF-E2 p45-regulated factor (Nrf2). Non-malignant MCF-10A cells were resistant to OSU-A9's antiproliferative effects. Daily oral administration of OSU-A9 at 25 and 50 mg/kg for 49 days significantly inhibited MCF-7 tumor growth by 59 and 70%, respectively, without overt signs of toxicity or evidence of induced hepatic biotransformation enzymes. In summary, OSU-A9 is a potent, orally bioavailable inhibitor of the Akt-NF-kappaB signaling network, targeting multiple aspects of breast tumor pathogenesis and progression. Thus, its translational potential for the treatment or prevention of breast cancer warrants further investigation.

机译：人类肿瘤的分子异质性挑战了有效预防和治疗策略的发展。为了克服这个问题，一种合理的方法是与联合疗法或有效的多靶点药物同时靶向临床相关的细胞异常。 OSU-A9是一种新型的吲哚-3-甲醇衍生物，它保留了母体化合物干扰致癌信号传导多个成分的能力，但在化学稳定性和抗肿瘤效力方面具有明显优势。在这里，我们显示OSU-A9在诱导具有不同遗传异常的各种乳腺癌细胞系（包括MCF-7，MDA-MB-231和SKBR3）的细胞凋亡中，比吲哚-3-甲醇具有两个数量级的效力。吲哚-3-甲醇的最大抑制浓度的一半为1.2-1.8 microM相对于200 microM。 OSU-A9对Akt-核因子-κB（NF-kappaB）和应激反应信号通路的多个组成部分具有出色的活性，同时具有这种差异的功效。其中值得注意的是雌激素受体（ER）-β/ ERalpha表达比增加，HER2和CXCR4表达降低，芳基烃受体表达及其下游目标NF-E2 p45调节因子（Nrf2）上调。非恶性MCF-10A细胞对OSU-A9的抗增殖作用有抗性。每天口服OSU-A9 25和50 mg / kg持续49天，分别可显着抑制MCF-7肿瘤生长59％和70％，而没有明显的毒性迹象或诱导的肝生物转化酶的迹象。总之，OSU-A9是Akt-NF-kappaB信号网络的一种有效的，口服生物利用的抑制剂，靶向乳腺癌肿瘤的发生和发展的多个方面。因此，其在治疗或预防乳腺癌方面的翻译潜力值得进一步研究。

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《Carcinogenesis》 |2009年第10期|共8页
作者
Weng JR; Tsai CH; Omar HA;
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1. OSU-A9, a potent indole-3-carbinol derivative, suppresses breast tumor growth by targeting the Akt-NF-kappaB pathway and stress response signaling. [J] . Weng JR, Tsai CH, Omar HA Carcinogenesis . 2009,第10期

机译：OSU-A9是有效的吲哚-3-甲醇衍生物，可通过靶向Akt-NF-kappaB途径和应激反应信号来抑制乳腺肿瘤的生长。
2. Targeting of the Akt-nuclear factor-kappa B signaling network by (1-(4-chloro-3-nitrobenzenesulfonyl)-1H-indol-3-yl)-methanol (OSU-A9), a novel indole-3-carbinol derivative, in a mouse model of hepatocellular carcinoma. [J] . Omar HA, Sargeant AM, Weng JR, Molecular pharmacology. . 2009,第5期

机译：新型吲哚-3-甲醇衍生物（1-（4-氯-3-硝基苯磺酰基）-1H-吲哚-3-基）-甲醇（OSU-A9）靶向Akt-核因子-κB信号网络，在肝细胞癌的小鼠模型中。
3. Breast cancer vaccines delivered by dendritic cell-targeted lentivectors induce potent antitumor immune responses and protect mice from mammary tumor growth [J] . Vaccine . 2017,第43期

机译：由树突细胞靶向慢动病患者递送的乳腺癌疫苗诱导有效的抗肿瘤免疫应答并保护小鼠免受乳腺肿瘤生长
4. The PERK pathway of the unfolded protein response (UPR): Its role in hypoxia tolerance and as a target for anti-tumor strategies [D] . Fels, Diane Renee 2008

机译：展开蛋白反应（UPR）的PERK途径：其在低氧耐受性中的作用以及作为抗肿瘤策略的靶标
5. OSU-A9 a potent indole-3-carbinol derivative suppresses breast tumor growth by targeting the Akt–NF-κB pathway and stress response signaling [O] . Jing-Ru Weng, Chen-Hsun Tsai, Hany A. Omar, -1

机译：OSU-A9是有效的吲哚-3-甲醇衍生物通过靶向Akt–NF-κB途径和应激反应信号传导来抑制乳腺肿瘤的生长
6. OSU-A9, a potent indole-3-carbinol derivative, suppresses breast tumor growth by targeting the Akt–NF-κB pathway and stress response signaling [O] . Weng, Jing-Ru, Tsai, Chen-Hsun, Omar, Hany A., 2009

机译：OSU-A9是有效的吲哚-3-甲醇衍生物，可通过靶向Akt–NF-κB途径和应激反应信号来抑制乳腺肿瘤的生长
7. Chemotherapeutic Potential of G1 Cell Cycle Inhibitor Indole-3-Carbinol and Its More Potent N-Alkoxy Derivatives in Human Breast Cancer Xenografts in Mice [R] . Kerekatte, V. S. , Firestone, G. 2004

机译：G1细胞周期抑制剂吲哚-3-甲醇及其更有效的N-烷氧基衍生物在小鼠人乳腺癌异种移植物中的化疗潜力

OSU-A9, a potent indole-3-carbinol derivative, suppresses breast tumor growth by targeting the Akt-NF-kappaB pathway and stress response signaling.

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