Department of Human Oncology, School of Medicine and Public Health, University of Wisconsin-Madison, Madison, Wisconsin, USA.
J Invest Dermatol. 2010 Jan;130(1):270-7. doi: 10.1038/jid.2009.212.
Chronic exposure to UVR is the major etiologic factor in the development of human skin cancers including squamous-cell carcinoma (SCC). We have previously shown that protein Kinase C epsilon (PKCepsilon) transgenic mice on FVB/N background, which overexpress PKCepsilon protein approximately eightfold over endogenous levels in epidermis, exhibit about threefold more sensitivity than wild-type littermates to UVR-induced development of SCC. To determine whether it is PKCepsilon and not the mouse genetic background that determines susceptibility to UVR carcinogenesis, we cross-bred PKCepsilon FVB/N transgenic mice with SKH-1 hairless mice to generate PKCepsilon-overexpressing SKH-1 hairless mice. To evaluate the susceptibility of PKCepsilon SKH-1 hairless transgenic mice to UVR carcinogenesis, the mice were exposed to UVR (1-2 KJ m(-2)) three times weekly from a bank of six kodacel-filtered FS40 sunlamps. As compared with the wild-type hairless mice, PKCepsilon overexpression in SKH-1 hairless mice decreased the latency (12 weeks), whereas it increased the incidence (twofold) and multiplicity (fourfold) of SCC. The SKH hairless transgenic mice were observed to be as sensitive as FVB/N transgenic mice to UVR-induced development of SCC and expression of proliferative markers (proliferating cell nuclear antigen, signal transducers and activators of transcription 3, and extracellular signal-regulated kinase 1/2). The results indicate that PKCepsilon level dictates susceptibility, irrespective of genetic background, to UVR carcinogenesis.
慢性暴露于 UVR 是人类皮肤癌(包括鳞状细胞癌[SCC])发展的主要病因。我们之前已经表明,在 FVB/N 背景下过表达 PKCepsilon 蛋白的蛋白激酶 C ɛ(PKCepsilon)转基因小鼠,其表皮中 PKCepsilon 蛋白的表达水平比内源性水平高出约八倍,对 UVR 诱导的 SCC 发展的敏感性比野生型同窝仔高出约三倍。为了确定决定对 UVR 致癌作用易感性的是 PKCepsilon 而不是小鼠遗传背景,我们将 PKCepsilon FVB/N 转基因小鼠与 SKH-1 无毛小鼠杂交,以产生 PKCepsilon 过表达的 SKH-1 无毛小鼠。为了评估 PKCepsilon SKH-1 无毛转基因小鼠对 UVR 致癌作用的易感性,将这些小鼠从六台 kodacel 过滤 FS40 太阳灯的灯架上每周接受 3 次 UVR(1-2 KJ m(-2))照射。与野生型无毛小鼠相比,SKH-1 无毛小鼠中 PKCepsilon 的过表达缩短了潜伏期(12 周),而增加了 SCC 的发生率(两倍)和多发性(四倍)。观察到 SKH 无毛转基因小鼠对 UVR 诱导的 SCC 发展和增殖标记物(增殖细胞核抗原、信号转导和转录激活因子 3 和细胞外信号调节激酶 1/2)的表达与 FVB/N 转基因小鼠一样敏感。结果表明,PKCepsilon 水平决定了对 UVR 致癌作用的易感性,而与遗传背景无关。