Ectopic expression of the transcription factor MafB in basal keratinocytes induces hyperproliferation and perturbs epidermal homeostasis

细胞生物学 表皮(动物学) 角质形成细胞 生物 角蛋白5 转录因子 角蛋白 角蛋白14 转基因小鼠 细胞分化 转基因 异位表达 细胞培养 遗传学 解剖 基因
作者
Masashi Miyai,Yukino Tsunekage,Michiko Saito,Kenji Kohno,Kenzo Takahashi,Kohsuke Kataoka
出处
期刊:Experimental Dermatology [Wiley]
卷期号:26 (11): 1039-1045 被引量:7
标识
DOI:10.1111/exd.13364
摘要

Mammalian epidermis is composed of four morphologically and functionally distinct layers of keratinocytes. The innermost basal layer consists of proliferating self-renewing keratinocytes, which also undergo asymmetric cell division to differentiate into postmitotic suprabasal cells throughout life. Control of the balance between growth and differentiation of basal cells is important for epidermal homeostasis to prevent skin disorders including malignancies; however, the underlying mechanism remains to be elucidated. Recently, MafB was identified as one of the transcription factors that regulate epidermal keratinocyte differentiation. MafB is expressed in postmitotic differentiating keratinocytes, and epidermal differentiation is partially impaired in MafB-deficient mice. To further establish the roles of MafB in the epidermis in vivo, we generated mice transgenic for MafB under the control of the basal cell-specific keratin (Krt) 14 promoter. In the epidermis of transgenic mice at embryonic day 18.5, the number of proliferating Krt14-positive basal-like cells was increased, and the granular and cornified layers were thickened. Furthermore, these MafB transgenic mice developed papillomas spontaneously with age. Therefore, MafB promotes differentiation in postmitotic keratinocytes and simultaneously has potential to promote growth when ectopically expressed in undifferentiated basal keratinocytes.
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