Suppression of KLF5 basal expression in oral carcinoma-derived cells through three intact CREB1-binding sites in the silencer region

IF 2.6 Q1 DENTISTRY, ORAL SURGERY & MEDICINE Journal of Oral Biosciences Pub Date : 2024-03-01 DOI:10.1016/j.job.2023.12.006
Reiichi Katsuumi, Tsubasa Negishi, Kazushi Imai, Nozomi Mihara
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Abstract

Objectives

Krüppel-like factor (KLF)5, which is overexpressed in carcinomas such as oral cancer, inhibits epidermal differentiation. KLF5 induces dedifferentiation of carcinoma cells, which effectuates carcinoma progression; nevertheless, the regulatory mechanism affecting the transcription of the KLF5 gene remains ambiguous.

Methods

Transcriptional activity of the KLF5 silencer, specifically the 425-bp region (425-region), was examined using reporter assays. An additional analysis was conducted to assess the impact of the minimal essential region (MER) of KLF5 on its basal expression. The affinity of cAMP responsive element binding protein 1 (CREB1) for three potential CREB1-binding sites in the 425-region was analyzed using DNA pull-down and quantitative chromatin immunoprecipitation assays. Reporter assays employing a human oral squamous carcinoma cell line, HSC2, transfected with small interfering RNA or complementary DNA for CREB1, were performed to investigate the effect of CREB1 binding sites on MER activity.

Results

The 425-region exhibited no transcriptional activity and suppressed MER transcriptional activity. This region encodes three putative CREB1-binding sites, and CREB1 demonstrated equal binding affinity for all three sites. The deletion of each of these binding sites reduced CREB1 precipitation and enhanced MER activity. Endogenous CREB1 knockdown and overexpression elevated and reduced MER activity, respectively, at the intact sites. Conversely, site deletion hampered and improved MER activity upon CREB1 knockdown and overexpression, respectively.

Conclusions

Suppression of KLF5 basal expression via CREB1 binding to the 425-region requires all three CREB1-binding sites to remain intact in oral carcinoma cells. Consequently, deletion of the CREB1-binding site relieves suppression of KLF5 basal expression.

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通过沉默区中三个完整的 CREB1 结合位点抑制口腔癌衍生细胞中 KLF5 的基础表达。
目的:在口腔癌等癌肿中过度表达的Krüppel样因子(KLF)5会抑制表皮分化。然而,影响 KLF5 基因转录的调控机制仍不明确:方法:使用报告分析法检测了 KLF5 沉默因子的转录活性,特别是 425-bp 区域(425-区域)。另外还进行了一项分析,以评估 KLF5 的最小基本区(MER)对其基础表达的影响。利用 DNA 牵引和定量染色质免疫共沉淀实验分析了 cAMP 反应元件结合蛋白 1(CREB1)与 425 区域中三个潜在的 CREB1 结合位点的亲和力。利用转染了 CREB1 的小干扰 RNA 或互补 DNA 的人类口腔鳞癌细胞系 HSC2 进行了报告实验,以研究 CREB1 结合位点对 MER 活性的影响:结果:425区域没有转录活性,但抑制了MER的转录活性。该区域编码了三个假定的 CREB1 结合位点,CREB1 与这三个位点的结合亲和力相同。删除每个结合位点都会减少 CREB1 的沉淀,增强 MER 的活性。内源性 CREB1 的敲除和过表达分别提高和降低了完整位点的 MER 活性。相反,在 CREB1 敲除和过表达时,位点缺失分别阻碍和提高了 MER 活性:结论:在口腔癌细胞中,通过 CREB1 与 425 区域的结合抑制 KLF5 的基础表达需要所有三个 CREB1 结合位点保持完整。因此,删除 CREB1 结合位点可解除对 KLF5 基础表达的抑制。
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来源期刊
Journal of Oral Biosciences
Journal of Oral Biosciences DENTISTRY, ORAL SURGERY & MEDICINE-
CiteScore
4.40
自引率
12.50%
发文量
57
审稿时长
37 days
期刊最新文献
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