| Literature DB >> 23744630 |
Shinji Miwa1, Shuya Yano, Yukihiko Hiroshima, Yasunori Tome, Fuminari Uehara, Sumiyuki Mii, Elena V Efimova, Hiroaki Kimura, Katsuhiro Hayashi, Hiroyuki Tsuchiya, Robert M Hoffman.
Abstract
We have previously demonstrated that the ultraviolet (UV) light is effective against a variety of cancer cells in vivo as well as in vitro. In the present report, we imaged the DNA damage repair response of minimal cancer after UVC irradiation. DNA-damage repair response to UV irradiation was imaged on tumors growing in 3D culture and in superficial tumors grown in vivo. UV-induced DNA damage repair was imaged with GFP fused to the DNA damage response (DDR)-related chromatin-binding protein 53BP1 in MiaPaCa-2 human pancreatic cancer cells. Three-dimensional Gelfoam® histocultures and confocal imaging enabled 53BP1-GFP nuclear foci to be observed within 1 h after UVC irradiation, indicating the onset of DNA damage repair response. A clonogenic assay showed that UVC inhibited MiaPaCa-2 cell proliferation in a dose-dependent manner, while UVA and UVB showed little effect on cell proliferation. Induction of UV-induced 53BP1-GFP focus formation was limited up to a depth of 40 µm in 3D-culture of MiaPaCa-2 cells. The MiaPaCa-2 cells irradiated by UVC light in a skin-flap mouse model had a significant decrease of tumor growth compared to untreated controls. Our results also demonstrate that 53BP1-GFP is an imageable marker of UV-induced DNA damage repair response of minimal cancer and that UVC is a useful tool for the treatment of residual cancer since UVC can kill superficial cancer cells without damage to deep tissue.Entities:
Keywords: 53BP1; DNA DAMAGE; GFP; MIAPACA-2; NUDE MICE; PANCREATIC CANCER; REPAIR RESPONSE; SKIN FLAP; THREE-DIMENSIONAL CULTURE IMAGING; UVC
Mesh:
Year: 2013 PMID: 23744630 DOI: 10.1002/jcb.24599
Source DB: PubMed Journal: J Cell Biochem ISSN: 0730-2312 Impact factor: 4.429