Volume 76, Issue 1 , Pages 5-8, January 2010
Lin28-let7 Modulates Radiosensitivity of Human Cancer Cells With Activation of K-Ras
Purpose
To evaluate the potential of targeting Lin28-let7 microRNA regulatory network for overcoming the radioresistance of cancer cells having activated K-Ras signaling.
Methods and Materials
A549 lung carcinoma cells and ASPC1 pancreatic cancer cells possessing K-RAS mutation were transfected with pre-let7a microRNA or Lin28 siRNA, respectively. Clonogenic assay, quantitative reverse transcription polymerase chain reaction, and Western analysis were performed. The effects of Lin28 on SQ20B cells having wild-type K-RAS, and a normal fibroblast were also assessed.
Results
The overexpression of let-7a decreased expression of K-Ras and radiosensitized A549 cells. Inhibition of Lin28, a repressor of let-7, attenuated K-Ras expression and radiosensitized A549 and ASPC1 cells. Neither SQ20B cells expressing wild-type K-RAS nor HDF, the normal human fibroblasts, were radiosensitized by this approach.
Conclusions
The Lin28-let7 regulatory network may be a potentially useful therapeutic target for overcoming the radioresistance of human cancers having activated K-Ras signaling.
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J.-S. Oh, J.-J. Kim, and J.-Y. B. contributed equally to this study.
Supported by grants from the Korean Ministry of Education, Science & Technology (BAERI #M20708630001-07B0863-00110 & KRF#E00381).
Conflict of interest: none.
PII: S0360-3016(09)02969-1
doi:10.1016/j.ijrobp.2009.08.028
© 2010 Elsevier Inc. All rights reserved.
Volume 76, Issue 1 , Pages 5-8, January 2010
