TY - JOUR
T1 - Mouse models for xeroderma pigmentosum group A and group C show divergent cancer phenotypes
AU - Melis, Joost P.M.
AU - Wijnhoven, Susan W.P.
AU - Beems, Rudolf B.
AU - Roodbergen, Marianne
AU - Van Den Berg, Jolanda
AU - Moon, Hojin
AU - Friedberg, Errol
AU - Van Der Horst, Gijsbertus T.J.
AU - Hoeijmakers, Jan H.J.
AU - Vijg, Jan
AU - Van Steeg, Harry
PY - 2008/3/1
Y1 - 2008/3/1
N2 - The accumulation of DNA damage is a slow but hazardous phenomenon that may lead to cell death, accelerated aging, and cancer. One of the most versatile defense mechanisms against the accumulation of DNA damage is nucleotide excision repair, in which, among others, the Xeroderma pigmentosum group C (XPC) and group A (XPA) proteins are involved. To elucidate differences in the functions of these two proteins, comprehensive survival studies with Xpa-/-, Xpc-/- and wild-type control female mice in a pure C57BL/6J background were done. The median survival of Xpc-/- mice showed a significant decrease, whereas the median survival of Xpa-/- mice did not. Strikingly, Xpa-/- and Xpc-/- mice also showed a phenotypical difference in terms of tumor spectrum. Xpc-/- mice displayed a significant increase in lung tumors and a trend toward increased liver tumors compared with Xpa-deficient or wild-type mice. Xpa-/- mice showed a significant elevation in liver tumors. Additionally, Xpc-deficient mice exhibited a strong increase in mutant frequency in lung compared with Xpa-/- mice, whereas in both models mutant frequency is increased in liver. Our in vitro data displayed an elevated sensitivity to oxygen in Xpc -/- in mouse embryonic fibroblasts (MEF) when compared with Xpa -/- and wild-type fibroblasts. We believe that XPC plays a role in the removal of oxidative DNA damage and that, therefore, Xpc-/- mice display a significant increase in lung tumors and a significant elevation in mutant frequency in lung, and Xpc-deficient MEFs show greater sensitivity to oxygen when compared with Xpa-/- and wild-type mice.
AB - The accumulation of DNA damage is a slow but hazardous phenomenon that may lead to cell death, accelerated aging, and cancer. One of the most versatile defense mechanisms against the accumulation of DNA damage is nucleotide excision repair, in which, among others, the Xeroderma pigmentosum group C (XPC) and group A (XPA) proteins are involved. To elucidate differences in the functions of these two proteins, comprehensive survival studies with Xpa-/-, Xpc-/- and wild-type control female mice in a pure C57BL/6J background were done. The median survival of Xpc-/- mice showed a significant decrease, whereas the median survival of Xpa-/- mice did not. Strikingly, Xpa-/- and Xpc-/- mice also showed a phenotypical difference in terms of tumor spectrum. Xpc-/- mice displayed a significant increase in lung tumors and a trend toward increased liver tumors compared with Xpa-deficient or wild-type mice. Xpa-/- mice showed a significant elevation in liver tumors. Additionally, Xpc-deficient mice exhibited a strong increase in mutant frequency in lung compared with Xpa-/- mice, whereas in both models mutant frequency is increased in liver. Our in vitro data displayed an elevated sensitivity to oxygen in Xpc -/- in mouse embryonic fibroblasts (MEF) when compared with Xpa -/- and wild-type fibroblasts. We believe that XPC plays a role in the removal of oxidative DNA damage and that, therefore, Xpc-/- mice display a significant increase in lung tumors and a significant elevation in mutant frequency in lung, and Xpc-deficient MEFs show greater sensitivity to oxygen when compared with Xpa-/- and wild-type mice.
UR - http://www.scopus.com/inward/record.url?scp=40449112147&partnerID=8YFLogxK
U2 - 10.1158/0008-5472.CAN-07-6067
DO - 10.1158/0008-5472.CAN-07-6067
M3 - Article
C2 - 18316597
AN - SCOPUS:40449112147
SN - 0008-5472
VL - 68
SP - 1347
EP - 1353
JO - Cancer Research
JF - Cancer Research
IS - 5
ER -