| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 11029134 | Oral Oncology | 2018 | 9 Pages |
Abstract
To determine whether TLR3 status affects the stress response of OC2 cells to cisplatin, we generated TLR3 knockdown OC2 cells (psi-TLR3 cells) with a psiRNA-hTLR3 plasmid containing shRNA to TLR3 and control OC2 cells (psi-NT cells) expressing non-silencing shRNA. OC2 cells were more sensitive to cisplatin treatment after TLR3 knockdown. In our animal model, OC2 psi-NT cells were more tumorigenic than were OC2 psi-TLR3 cells. Together, our in vitro and in vivo data imply TLR3 may contribute to tumor development and protect cisplatin-induced DNA damage response leading to cisplatin resistance in head and neck cancer cells.
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Authors
Hui-Ching Chuang, Ming-Huei Chou, Chih-Yen Chien, Jiin-Haur Chuang, Yu-Li Liu,