Upregulation of polycistronic microRNA-143 and microRNA-145 in colonocytes suppresses colitis and inflammation-associated colon cancer

小RNA 生物 下调和上调 结直肠癌 炎症 结肠炎 癌症研究 癌症 信使核糖核酸 转录组 基因表达 免疫学 遗传学 基因
作者
Urszula Dougherty,Reba Mustafi,Hongyan Zhu,Xiaorong Zhu,Dilip K. Deb,Stephen C. Meredith,Fatma Ayaloglu-Butun,Michelle Fletcher,Arantxa Sanchez Castillo,Joel Pekow,Zifeng Deng,Nader Amini,Vani J. Konda,Vijaya L. Rao,Atsushi Sakuraba,Akushika Kwesi,Sonia S. Kupfer,Alessandro Fichera,Loren Joseph,John Hart,Fang He,Tong‐Chuan He,Diana C. West-Szymanski,Yan Chun Li,Marc Bissonnette
出处
期刊:Epigenetics [Informa]
卷期号:16 (12): 1317-1334 被引量:12
标识
DOI:10.1080/15592294.2020.1863117
摘要

Because ADAM17 promotes colonic tumorigenesis, we investigated potential miRNAs regulating ADAM17; and examined effects of diet and tumorigenesis on these miRNAs. We also examined pre-miRNA processing and tumour suppressor roles of several of these miRNAs in experimental colon cancer. Using TargetScan, miR-145, miR-148a, and miR-152 were predicted to regulate ADAM17. miR-143 was also investigated as miR-143 and miR-145 are co-transcribed and associated with decreased tumour growth. HCT116 colon cancer cells (CCC) were co-transfected with predicted ADAM17-regulating miRNAs and luciferase reporters controlled by ADAM17-3'UTR. Separately, pre-miR-143 processing by colonic cells was measured. miRNAs were quantified by RT-PCR. Tumours were induced with AOM/DSS in WT and transgenic mice (Tg) expressing pre-miR-143/miR-145 under villin promoter. HCT116 transfection with miR-145, −148a or −152, but not scrambled miRNA inhibited ADAM17 expression and luciferase activity. The latter was suppressed by mutations in ADAM17-3'UTR. Lysates from colonocytes, but not CCC, processed pre-miR-143 and mixing experiments suggested CCC lacked a competency factor. Colonic miR-143, miR-145, miR-148a, and miR-152 were downregulated in tumours and more moderately by feeding mice a Western diet. Tg mice were resistant to DSS colitis and had significantly lower cancer incidence and tumour multiplicity. Tg expression blocked up-regulation of putative targets of miR-143 and miR-145, including ADAM17, K-Ras, XPO5, and SET. miR-145, miR-148a, and miR-152 directly suppress colonocyte ADAM17 and are down-regulated in colon cancer. This is the first direct demonstration of tumour suppressor roles for miR-143 and miR-145 in an in vivo model of colonic tumorigenesis.
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