作者
Suat Erdogan, Eda Tosyali, Vesile Duzguner, Altug Kucukgul, Ozkan Aslantas, Sefa Celik
发表日期
2010/4/1
期刊
Research in veterinary science
卷号
88
期号
2
页码范围
218-226
出版商
WB Saunders
简介
Brucella species are able to survive and replicate within the phagocytic cells and cause chronic infections in domestic animals and humans. Modulation of programmed cell death by Brucella spp. may be one of the reasons of the chronicity of the infection. In this study, whether cisplatin treatment, an apoptotic anticancer agent, would enhance the host resistance against Brucella melitensis-infected human macrophage-like cells was investigated. The infection neither induced inflammation nor oxidative stress. But, Brucella caused a decrease in infected macrophage viability of 36% at 48h postinfection (p.i.) as compared with uninfected cells. Treatment of infected macrophages with 20μM cisplatin for 48h caused a large increase in nitric oxide (NO) levels in a time-dependent manner via induction of iNOS transcription. Cisplatin also enhanced glutathione peroxidase, myeloperoxidase and xanthine oxidase activities …
引用总数
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