Therapeutic Targeting of the CBP/p300 Bromodomain Blocks the Growth of Castration-Resistant Prostate Cancer

Jin Lingyan; Garcia Jesse; Chan Emily; de la Cruz Cecile; Segal Ehud; Merchant Mark; Kharbanda Samir; Raisner Ryan; Haverty Peter M.; Modrusan Zora; Ly Justin; Choo Edna; Kaufman Susan; Beresini Maureen H.; Romero F. Anthony; Magnuson Steven; Gascoigne Karen E.

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Therapeutic Targeting of the CBP/p300 Bromodomain Blocks the Growth of Castration-Resistant Prostate Cancer

机译：CBP / P300 Bromodomain的治疗靶向阻断抗阉割前列腺癌的生长

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Resistance invariably develops to antiandrogen therapies used to treat newly diagnosed prostate cancers, but effective treatments for castration-resistant disease remain elusive. Here, wereport that the transcriptional coactivator CBP/p300 is required to maintain the growth of castration-resistant prostate cancer. To exploit this vulnerability, we developed a novel small-molecule inhibitor of the CBP/p300 bromodomain that blocks prostate cancer growth in vitro and in vivo. Molecular dissection of the consequences of drug treatment revealed a critical role for CBP/p300 in histone acetylation required for the transcriptional activity of the androgen receptor and its target gene expression. Our findings offer a preclinical proof of concept for small-molecule therapies to target the CBP/p300 bromodomain as a strategy to treat castration-resistant prostate cancer. (C) 2017 AACR.

机译：抗性总是发展到用于治疗新诊断的前列腺癌的抗衰老疗法，但对阉割疾病的有效治疗仍然难以捉摸。在此，在此检测转录共酰剂CBP / P300需要维持抗阉割前列腺癌的生长。为了利用这种脆弱性，我们开发了一种新型的CBP / P300溴衍生物的小分子抑制剂，其在体外和体内阻断前列腺癌生长。药物治疗后果的分子解剖显示CBP / P300在雄激素受体的转录活性所需的组蛋白乙酰化中的关键作用及其靶基因表达。我们的研究结果为小分子疗法提供了临床前概念，以靶向CBP / P300溴莫氏域作为治疗抗阉割前列腺癌的策略。（c）2017年AACR。

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《Cancer research: The official organ of the American Association for Cancer Research, Inc》 |2017年第20期|共12页
作者
Jin Lingyan; Garcia Jesse; Chan Emily; de la Cruz Cecile; Segal Ehud; Merchant Mark; Kharbanda Samir; Raisner Ryan; Haverty Peter M.; Modrusan Zora; Ly Justin; Choo Edna; Kaufman Susan; Beresini Maureen H.; Romero F. Anthony; Magnuson Steven; Gascoigne Karen E.;
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作者单位

Genentech Inc Dept Discovery Oncol San Francisco CA 94080 USA;

Genentech Inc Dept Translat Oncol San Francisco CA 94080 USA;

Genentech Inc Dept Translat Oncol San Francisco CA 94080 USA;

Genentech Inc Dept Translat Oncol San Francisco CA 94080 USA;

Genentech Inc Dept Translat Oncol San Francisco CA 94080 USA;

Genentech Inc Dept Translat Oncol San Francisco CA 94080 USA;

Calico Labs San Francisco CA USA;

Genentech Inc Dept Discovery Oncol San Francisco CA 94080 USA;

Genentech Inc Dept Bioinformat San Francisco CA 94080 USA;

Genentech Inc Dept Mol Biol San Francisco CA 94080 USA;

Genentech Inc Dept DMPK San Francisco CA 94080 USA;

Genentech Inc Dept DMPK San Francisco CA 94080 USA;

Genentech Inc Dept Biochem &

Cellular Pharmacol San Francisco CA 94080 USA;

Genentech Inc Dept Biochem &

Cellular Pharmacol San Francisco CA 94080 USA;

Unity Biotechnol Brisbane CA USA;

Genentech Inc Dept Discovery Chem San Francisco CA 94080 USA;

Genentech Inc Dept Discovery Oncol San Francisco CA 94080 USA;

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正文语种 eng
中图分类肿瘤学;
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1. Therapeutic Targeting of the CBP/p300 Bromodomain Blocks the Growth of Castration-Resistant Prostate Cancer [J] . Jin Lingyan, Garcia Jesse, Chan Emily, Cancer research: The official organ of the American Association for Cancer Research, Inc . 2017,第20期

机译：CBP / P300 Bromodomain的治疗靶向阻断抗阉割前列腺癌的生长
2. Bromodomain inhibition of the transcriptional coactivators CBP/EP300 as a therapeutic strategy to target the IRF4 network in multiple myeloma [J] . Andrew R Conery, Richard C Centore, Adrianne Neiss, eLife journal . 2016,第11期

机译：溴结构域抑制转录共激活因子CBP / EP300作为靶向治疗多发性骨髓瘤IRF4网络的治疗策略
3. Therapeutic targeting of BET bromodomain proteins in castration-resistant prostate cancer [J] . Irfan A. Asangani, Vijaya L. Dommeti, Xiaoju Wang, Nature . 2014,第7504期

机译：BET溴结构域蛋白在去势抵抗性前列腺癌中的治疗靶向
4. The Coactivators CBP and p300 in Androgen Independent Prostate Cancer [C] . Jose D. Debes, Zoran Culig, Donald J. Tindal International Symposium on Hormonal Carcinogenesis . 2005

机译：CBP和P300在雄激素独立前列腺癌中的CBP和P300
5. Therapeutic Targeting of Stat5a/b in Advanced Prostate Cancer: Inhibition of Stat5a/b Suppresses Growth of Prostate Cancer through Mechanisms Dependent and Independent of Androgen Receptor. [D] . Hoang, David Timothy. 2016

机译：Stat5a / b在晚期前列腺癌中的治疗靶点：Stat5a / b的抑制作用通过依赖于雄激素受体的机制来抑制前列腺癌的生长。
6. Correction: Bromodomain inhibition of the transcriptional coactivators CBP/EP300 as a therapeutic strategy to target the IRF4 network in multiple myeloma [O] . Andrew R Conery, Richard C Centore, Adrianne Neiss, 2016

机译：纠正：抑制转录共激活因子CBP / EP300的溴结构域作为一种靶向多发性骨髓瘤中IRF4网络的治疗策略
7. Correction: Bromodomain inhibition of the transcriptional coactivators CBP/EP300 as a therapeutic strategy to target the IRF4 network in multiple myeloma [O] . Andrew R Conery, Richard C Centore, Adrianne Neiss, 2016

机译：校正：溴琼瘤抑制转录共觉器CBP / EP300作为靶向多发性骨髓瘤中IRF4网络的治疗策略
8. Novel Therapeutic Targets to Inhibit Tumor Microenvironment Induced Castration-Resistant Prostate Cancer. [R] . Yang, F. 2017

机译：新型治疗靶点抑制肿瘤微环境诱导去势抵抗前列腺癌。

Therapeutic Targeting of the CBP/p300 Bromodomain Blocks the Growth of Castration-Resistant Prostate Cancer

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