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Enhanced tumor radiosensitivity by a survivin dominant-negative mutant

Authors :
Yong-Qiu Mao
Dan-Dan Yu
Wei Li
Li Pan
Yuquan Wei
Xiang Chen
Huashan Shi
Chun-Ting Wang
Qing-Zhong Yuan
Zhi-Yong Li
Tian-Tai Ma
Fei Leng
Peng Zhang
Fan Wu
Jing-Hui Xu
Wei Ying
Yuan Wen
Source :
Oncology reports. 23(1)
Publication Year :
2009

Abstract

Radiosensitivity of tumors is due to a complex interaction of various factors, it has been reported that survivin also acts as a constitutive and inducible radioresistance factor in a panel of tumor cells and approaches designed to inhibit survivin expression or function may lead to tumor sensitisation to chemical and physical agents. Previously, we found that the plasmid encoding the phosphorylation-defective mouse survivin threonine 34-->alanine mutant complexed to DOTAP-chol liposome (Lip-mS) can suppress murine primary breast carcinoma. However, little is known regarding the biological effect of Lip-mS combined with radiation. The present study was designed to determine whether Lip-mS could enhance the anti-tumor activity of radiation. The Lewis Lung Carcinoma (LLC) cells treated with a combination of Lip-mS and radiation displayed apparently increased apoptosis compared with those treated with Lip-mS or radiation alone. Mice bearing LLC tumors were treated with intravenous injections of Lip-mS and radiation, the combined treatment significantly reduced mean tumor volume compared with either treatment alone. Moreover, the anti-tumor effect of Lip-mS combined with radiation was greater than their additive effect when compared with the expected effect of the combined treatment. These data suggest that inhibition of survivin using a dominant-negative mutant, survivin T34A, could sensitize LLC cells to radiation efficiently and the synergistic anti-tumor activity may in part result from increasing the apoptosis of tumor cells, inhibiting tumor angiogenesis and inducing a tumor-protective immune response in the combined treatment.

Details

ISSN :
17912431
Volume :
23
Issue :
1
Database :
OpenAIRE
Journal :
Oncology reports
Accession number :
edsair.doi.dedup.....e88e862c8b28525e73fabf7ced90590e