作者
V Kostourou, JE Cartwright, AP Johnstone, JKR Boult, ER Cullis, GStJ Whitley, SP Robinson
发表日期
2011/1
期刊
British journal of cancer
卷号
104
期号
1
页码范围
83-90
出版商
Nature Publishing Group
简介
Background:
Progressive tumour growth is dependent on the development of a functional tumour vasculature and highly regulated by growth factors and cytokines. Nitric oxide (NO) is a free radical, produced both by tumour and host cells, and functions as a signalling molecule downstream of several angiogenic factors. Both pro-and antitumourigenic properties have been attributed to NO.
Methods:
The expression of the inducible isoform of NO synthase (iNOS) was knocked down in the C6 glioma cell line using constitutive expression of antisense RNA, and the effect of tumour-derived NO on tumour progression and angiogenesis was investigated.
Results:
Tumours in which iNOS expression was decreased displayed significantly reduced growth rates compared with tumours derived from parental C6 cells. Quantitative non-invasive magnetic resonance imaging and fluorescence microscopy of tumour uptake of …
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V Kostourou, JE Cartwright, AP Johnstone, JKR Boult… - British journal of cancer, 2011