期刊论文详细信息
  1. 返回上一页
Molecules
Nitric Oxide-Releasing Aspirin Suppresses NF-κB Signaling in Estrogen Receptor Negative Breast Cancer Cells in Vitro and in Vivo
Niharika Nath1  Mitali Chattopadhyay1  Deborah B. Rodes1  Anna Nazarenko1  Ravinder Kodela1  Khosrow Kashfi1 
[1] Department of Physiology, Pharmacology and Neuroscience, Sophie Davis School of Biomedical Education, City University of New York Medical School, New York, NY 10031, USA; E-Mails:
关键词: NSAIDs;    NO-NSAIDs;    NF-κB;    oxidative stress;    breast cancer;    estrogen receptor;   
DOI  :  10.3390/molecules200712481
来源: mdpi
PDF
【 摘 要 】

Estrogen receptor negative (ER(−)) breast cancer is aggressive, responds poorly to current treatments and has a poor prognosis. The NF-κB signaling pathway is implicated in ER(−) tumorigenesis. Aspirin (ASA) is chemopreventive against ER(+) but not for ER(−) breast cancers. Nitric oxide-releasing aspirin (NO-ASA) is a safer ASA where ASA is linked to an NO-releasing moiety through a spacer. In vitro, we investigated anti-proliferation effects of NO-ASA (para- and meta-isomers) against ER(−) breast cancer cells MDA-MB-231 and SK-BR-23, effects on NF-κB signaling, and reactive oxygen species by standard techniques. In vivo, effects of NO-ASA were evaluated in a mouse xenograft model using MDA-MB-231 cells. p-NO-ASA inhibited the growth of MDA-MB-231 and SK-BR-3 cells at 24 h, the respective IC50s were 13 ± 2 and 17 ± 2 μM; ASA had an IC50 of >3000 μM in both cell lines. The IC50s for m-NO-ASA in MDA-MB-231 and SK-BR-3 were 173 ± 15 and 185 ± 12 μM, respectively, therefore, implying p-NO-ASA as a stronger inhibitor of growth p-NO-ASA reduced cell growth by inhibiting proliferation, inducing apoptosis and causing G0/G1 cell cycle block. Activation of NF-κB was inhibited by both isomers as demonstrated by decreases in NF-κB-DNA binding and luciferase activity at 24 h, However, m-NO-ASA produced transient effects at 3 h such as increased NF-κB-DNA-binding, increased levels of nuclear p50, even though both isomers inhibited IκB degradation. Increase in nuclear p50 by m-NO-ASA was associated with translocation of p50 in to the nucleus as observed by immunoflouresence at 3 h. NO-ASA induced reactive oxygen species (ROS) as evidenced by overall increases in both H2DCFDA (2′,7′-dichlorodihydrofluorescein) and DHE (dihydroethidium)-derived fluorescence. Inhibition of ROS by N-acetyl-cysteine reversed the m-NO-ASA-mediated translocation of p50 in to the nucleus. In xenografts, p-NO-ASA inhibited tumor growth by inhibiting proliferation (PCNA and tumor volume), inducing apoptosis (TUNEL positive cells) and reducing NF-κB expression. Both isomers inhibit cancer cells, inhibit NF-κB pathway and induce ROS, and have potential as anticancer compounds.

【 授权许可】

CC BY   
© 2015 by the authors; licensee MDPI, Basel, Switzerland.

【 预 览 】
附件列表
Files Size Format View
RO202003190009632ZK.pdf 2365KB PDF download
  文献评价指标  
  下载次数:7次 浏览次数:11次
   
推荐资源列表
关于我们|团队介绍|帮助中心|联系我们

Copyright © 2016 中国科学院文献情报中心

京公网安备340104078870146号  878987797  028-85220240

OAinOne平台基于对开放资源的发现、遴选和评价方式,发现、获取、集成9类优质的开放科技资源,包括开放期刊、开放会议论文、开放课件、科技政策、开放学位论文、开放图书、开放科技报告、科研项目、开放科学数据。同时,为实现开放知识资源普遍服务、个性化服务、精准服务,基于OAinONE集成的丰富开放资源,开发建设领域开放知识资源服务定制工具(OAtoYOU)、开放资源评价评估体系(OAEvaluation),建设集成OAinONE资源及其他第三方资源的OA Hub,及其面向我院分布式大数据知识资源系统及其他第三方的开放接口服务,并打造特色专题数据库产品建设,包括科技政策集成及趋势平台、开放课程大讲堂等。此外,OAinOne构建开放知识资源建设的可持续发展机制,支持我院研究所特色馆藏资源、自建资源、古籍资源等在OAinONE平台上的集成、开放、共享。