氧化应激特异性地下调survivin 以促进乳腺癌的形成。

Oxidative stress specifically downregulates survivin to promote breast tumour formation.

机构信息

Department of Internal Medicine, Charles Drew University of Medicine and Science, Los Angeles, CA 90059, USA.

出版信息

Br J Cancer. 2013 Mar 5;108(4):848-58. doi: 10.1038/bjc.2013.40. Epub 2013 Feb 12.

DOI:10.1038/bjc.2013.40

PMID:23403820

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3590675/

Abstract

BACKGROUND

Breast cancer, a heterogeneous disease has been broadly classified into oestrogen receptor positive (ER+) or oestrogen receptor negative (ER-) tumour types. Each of these tumours is dependent on specific signalling pathways for their progression. While high levels of survivin, an anti-apoptotic protein, increases aggressive behaviour in ER- breast tumours, oxidative stress (OS) promotes the progression of ER+ breast tumours. Mechanisms and molecular targets by which OS promotes tumourigenesis remain poorly understood.

RESULTS

DETA-NONOate, a nitric oxide (NO)-donor induces OS in breast cancer cell lines by early re-localisation and downregulation of cellular survivin. Using in vivo models of HMLE(HRAS) xenografts and E2-induced breast tumours in ACI rats, we demonstrate that high OS downregulates survivin during initiation of tumourigenesis. Overexpression of survivin in HMLE(HRAS) cells led to a significant delay in tumour initiation and tumour volume in nude mice. This inverse relationship between survivin and OS was also observed in ER+ human breast tumours. We also demonstrate an upregulation of NADPH oxidase-1 (NOX1) and its activating protein p67, which are novel markers of OS in E2-induced tumours in ACI rats and as well as in ER+ human breast tumours.

CONCLUSION

Our data, therefore, suggest that downregulation of survivin could be an important early event by which OS initiates breast tumour formation.

摘要

背景

乳腺癌是一种异质性疾病，通常被分为雌激素受体阳性（ER+）或雌激素受体阴性（ER-）肿瘤类型。这些肿瘤的每一种都依赖于特定的信号通路来促进其进展。虽然凋亡抑制蛋白 survivin 的高水平增加了 ER-乳腺癌的侵袭性行为，但氧化应激（OS）会促进 ER+乳腺癌的进展。OS 促进肿瘤发生的机制和分子靶点仍知之甚少。

结果

DETA-NONOate 是一种一氧化氮（NO）供体，通过早期重定位和下调细胞 survivin，在乳腺癌细胞系中诱导 OS。通过 HMLE(HRAS)异种移植的体内模型和 ACI 大鼠中 E2 诱导的乳腺癌，我们证明在肿瘤发生的起始阶段，高 OS 会下调 survivin。在 HMLE(HRAS)细胞中过表达 survivin 会导致裸鼠中的肿瘤起始和肿瘤体积显著延迟。在 ER+人乳腺癌中也观察到 survivin 和 OS 之间的这种反比关系。我们还证明了 NADPH 氧化酶-1（NOX1）及其激活蛋白 p67 的上调，这是 ACI 大鼠中 E2 诱导的肿瘤以及 ER+人乳腺癌中的 OS 的新标志物。

结论

因此，我们的数据表明，survivin 的下调可能是 OS 引发乳腺癌形成的一个重要早期事件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f7da/3590675/bb10333f1e60/bjc201340f1.jpg

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氧化应激特异性地下调survivin 以促进乳腺癌的形成。

Oxidative stress specifically downregulates survivin to promote breast tumour formation.

机构信息

Department of Internal Medicine, Charles Drew University of Medicine and Science, Los Angeles, CA 90059, USA.