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微小RNA和DICER1在前列腺基质中受1,25-二羟维生素D调控。

microRNAs and DICER1 are regulated by 1,25-dihydroxyvitamin D in prostate stroma.

作者信息

Dambal Shweta, Giangreco Angeline A, Acosta Andres M, Fairchild Andrew, Richards Zachary, Deaton Ryan, Wagner Dennis, Vieth Reinhold, Gann Peter H, Kajdacsy-Balla Andre, Van der Kwast Theodorus, Nonn Larisa

机构信息

Department of Pathology, University of Illinois at Chicago, Chicago, IL, United States.

Department of Nutritional Sciences, Laboratory Medicine and Pathobiology, University of Toronto, ON, Canada.

出版信息

J Steroid Biochem Mol Biol. 2017 Mar;167:192-202. doi: 10.1016/j.jsbmb.2017.01.004. Epub 2017 Jan 12.

Abstract

Vitamin D deficiency increases the risk of lethal prostate adenocarcinomas (PCa) and the majority of older men are deficient. Although PCa arises from the epithelium, the surrounding stroma has hormonal regulatory control over the epithelium and contributes to carcinogenesis. Herein, we describe regulation of microRNAs (miRs) by the active hormone dihydroxyvitamin D (1,25(OH)D) in human prostate stroma. 1,25(OH)D binds the vitamin D receptor (VDR) transcription factor to regulate gene expression, including miRs, which have emerged as potent regulators of protein expression. 1,25(OH)D-regulated miRs were identified by profiling in primary human prostatic stromal cells (PrS) and three miRs, miR-126-3p, miR 154-5p and miR-21-5p were subsequently validated in laser-capture micro-dissected prostate stromal tissue from a vitamin D3 clinical trial (N=45). Regulation of these miRs by 1,25(OH)D was VDR-dependent. Network analysis of known and putative mRNA targets of these miRs was enriched with cancer and inflammation pathways, consistent with known roles of stroma and of vitamin D in carcinogenesis. Expression of the miR processing ribonuclease, DICER1, positively correlated with vitamin D metabolite levels in the clinical trial specimens. High epithelial/stromal ratios of DICER1 were significantly associated biochemical recurrence (OR 3.1, p=0.03) in a tissue microarray of 170 matched PCa patients. In summary, these results underscore the role of the prostate stroma in regulating responses to the hormone 1,25(OH)D and identified miRs and DICER1 as being regulated in human prostate stroma. Regulation of stromal DICER1 by 1,25(OH)D may also have clinical relevance in protection against aggressive PCa.

摘要

维生素D缺乏会增加致命性前列腺腺癌(PCa)的风险,而且大多数老年男性都缺乏维生素D。虽然PCa起源于上皮细胞,但周围的基质对上皮细胞具有激素调节控制作用,并参与致癌过程。在此,我们描述了活性激素二羟基维生素D(1,25(OH)D)对人前列腺基质中微小RNA(miRs)的调节作用。1,25(OH)D与维生素D受体(VDR)转录因子结合以调节基因表达,包括miRs,而miRs已成为蛋白质表达的有效调节因子。通过对原代人前列腺基质细胞(PrS)进行分析鉴定出1,25(OH)D调节的miRs,随后在一项维生素D3临床试验(N = 45)的激光捕获显微切割前列腺基质组织中验证了三种miRs,即miR - 126 - 3p、miR 154 - 5p和miR - 21 - 5p。1,25(OH)D对这些miRs的调节是VDR依赖性的。对这些miRs已知和推测的mRNA靶标的网络分析富集了癌症和炎症途径,这与基质和维生素D在致癌过程中的已知作用一致。在临床试验标本中,miR加工核糖核酸酶DICER1的表达与维生素D代谢物水平呈正相关。在170例匹配的PCa患者的组织微阵列中,DICER1的上皮/基质高比值与生化复发显著相关(OR 3.1,p = 0.03)。总之,这些结果强调了前列腺基质在调节对激素1,25(OH)D的反应中的作用,并确定了miRs和DICER1在人前列腺基质中受到调节。1,25(OH)D对基质DICER1的调节在预防侵袭性PCa方面可能也具有临床意义。

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