转录因子 sp2 的过表达抑制表皮分化,并增加对创伤和致癌剂诱导的肿瘤发生的易感性。
Overexpression of transcription factor sp2 inhibits epidermal differentiation and increases susceptibility to wound- and carcinogen-induced tumorigenesis.
机构信息
Department of Molecular Biomedical Sciences, Center for Comparative Medicine and Translational Research, North Carolina State University, Raleigh, North Carolina 27606, USA.
出版信息
Cancer Res. 2010 Nov 1;70(21):8507-16. doi: 10.1158/0008-5472.CAN-10-1213. Epub 2010 Oct 19.
Abstract
Sp proteins are evolutionarily conserved transcription factors required for the expression of a wide variety of genes that are critical for development and cell cycle progression. Deregulated expression of certain Sp proteins is associated with the formation of a variety of human tumors; however, direct evidence that any given Sp protein is oncogenic has been lacking. Here, we report that Sp2 protein abundance in mice increases in concert with the progression of carcinogen-induced murine squamous cell carcinomas. Transgenic mice specifically overexpressing murine Sp2 in epidermal basal keratinocytes were highly susceptible to wound- and carcinogen-induced papillomagenesis. Transgenic animals that were homozygous rather than hemizygous for the Sp2 transgene exhibited a striking arrest in the epidermal differentiation program, perishing within 2 weeks of birth. Our results directly support the likelihood that Sp2 overexpression occurring in various human cancers has significant functional effect.
摘要
Sp 蛋白是进化上保守的转录因子,对于多种基因的表达是必需的,这些基因对于发育和细胞周期进程至关重要。某些 Sp 蛋白的失调表达与多种人类肿瘤的形成有关;然而,缺乏任何给定的 Sp 蛋白是否致癌的确切证据。在这里,我们报告说,在致癌剂诱导的小鼠鳞状细胞癌进展过程中,Sp2 蛋白的丰度在小鼠中协同增加。在表皮基底角质形成细胞中特异性过表达小鼠 Sp2 的转基因小鼠极易受到创伤和致癌剂诱导的乳头瘤形成的影响。对于 Sp2 转基因的纯合而非杂合转基因动物,表皮分化程序出现明显阻滞,在出生后 2 周内死亡。我们的结果直接支持这样一种可能性,即在各种人类癌症中发生的 Sp2 过表达具有显著的功能效应。
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