Greenhalgh D A, Rothnagel J A, Wang X J, Quintanilla M I, Orengo C C, Gagne T A, Bundman D S, Longley M A, Fisher C, Roop D R
Department of Cell Biology, Baylor College of Medicine, Houston, Texas 77030.
Oncogene. 1993 Aug;8(8):2145-57.
A vector, derived from the human K1 keratin gene, has been employed to target v-fos expression exclusively in the epidermis of transgenic mice. Adult transgenic mice expressors (3-4 months) displayed hyperplasia and hyperkeratosis, initially in wounded (tagged) ears, which later became bilateral. This phenotype appeared at other epidermal sites, most notably in the axilla and inguinal areas. This indicates that a second promoting event, such as wounding or friction, is required to elicit these pathological changes. Highly keratotic benign ear lesions and benign squamous papillomas appeared after long latency at sites of phenotypic epidermis. These data suggest that v-fos may be interfering with c-fos function in normal keratinocyte differentiation, but by itself is insufficient to elicit overt benign lesions.
一种源自人类K1角蛋白基因的载体已被用于在转基因小鼠的表皮中特异性靶向v-fos表达。成年转基因小鼠表达者(3 - 4个月)表现出增生和角化过度,最初出现在受伤(标记)的耳朵中,随后变为双侧性。这种表型出现在其他表皮部位,最明显的是腋窝和腹股沟区域。这表明需要第二个促进事件,如受伤或摩擦,才能引发这些病理变化。在表型表皮部位经过长时间潜伏期后,出现了高度角化的良性耳部病变和良性鳞状乳头状瘤。这些数据表明,v-fos可能在正常角质形成细胞分化过程中干扰c-fos功能,但仅凭其自身不足以引发明显的良性病变。
