The Natural Product Butylcycloheptyl Prodiginine Binds Pre-miR-21, Inhibits Dicer-Mediated Processing of Pre-miR-21, and Blocks Cellular Proliferation

Joe S. Matarlo; Lauren R.H. Krumpe; William F. Heinz; Daniel Oh; Shilpa R. Shenoy; Cheryl L. Thomas; Ekaterina I. Goncharova; Stephen J. Lockett; Barry R. OKeefe

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The Natural Product Butylcycloheptyl Prodiginine Binds Pre-miR-21, Inhibits Dicer-Mediated Processing of Pre-miR-21, and Blocks Cellular Proliferation

机译：天然产物丁基环蟾酸Propiginine结合miR-21，抑制Dicer介导的预热剂-11的加工，并阻断细胞增殖

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Identification of RNA-interacting pharmacophores could provide chemical probes and, potentially, small molecules for RNA-based therapeutics. Using a high-throughput differential scanning fluorimetry assay, we identified small-molecule natural products with the capacity to bind the discrete stem-looped structure of pre-miR-21. The most potent compound identified was a prodiginine-type compound, butylcycloheptyl prodiginine (bPGN), with the ability to inhibit Dicer-mediated processing of pre-miR-21in?vitroand in cells. Time-dependent RT-qPCR, western blot, and transcriptomic analyses showed modulation of miR-21 expression and its target genes such asPDCD4andPTENupon treatment with bPGN, supporting on-target inhibition. Consequently, inhibition of cellular proliferation in HCT-116 colorectal cancer cells was also observed when treated with bPGN. The discovery that bPGN can bind and modulate the expression of regulatory RNAs such as miR-21 helps set the stage for further development of this class of natural product as a molecular probe or therapeutic agent against miRNA-dependent diseases.

机译：鉴定RNA相互作用的药物团可以为RNA的治疗剂提供化学探针和潜在的小分子。使用高通量差分扫描荧光测定法，我们确定了具有粘合前MiR-21的离散茎环结构的能力的小分子天然产物。鉴定的最有效的化合物是Prodiginine型化合物，丁基环庚基培养蛋白（BPGN），其能够抑制细胞中培养皿中的vir-21培养物的Dicer介导的介导的加工。时间依赖性的RT-QPCR，Western印迹和转录组分析显示MiR-21表达及其靶基因的调节，如BPGN的aspdcd4andptenupon治疗，支持靶抑制。因此，当用BPGN处理时，还观察到在HCT-116结肠直肠癌细胞中对细胞增殖的抑制。发现BPGN可以结合和调节调节RNA的表达，例如miR-21，有助于设定作为分子探针或治疗剂对针对miRNA依赖性疾病的分子探针或治疗剂进一步发展的阶段。

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来源
《Cell chemical biology》 |2019年第8期|共14页
作者
Joe S. Matarlo; Lauren R.H. Krumpe; William F. Heinz; Daniel Oh; Shilpa R. Shenoy; Cheryl L. Thomas; Ekaterina I. Goncharova; Stephen J. Lockett; Barry R. OKeefe;
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作者单位

Molecular Targets Program Center for Cancer Research National Cancer Institute National Institutes of Health;

Molecular Targets Program Center for Cancer Research National Cancer Institute National Institutes of Health;

Optical Microscopy and Analysis Laboratory Frederick National Laboratory for Cancer Research;

Molecular Targets Program Center for Cancer Research National Cancer Institute National Institutes of Health;

Molecular Targets Program Center for Cancer Research National Cancer Institute National Institutes of Health;

Molecular Targets Program Center for Cancer Research National Cancer Institute National Institutes of Health;

Molecular Targets Program Center for Cancer Research National Cancer Institute National Institutes of Health;

Optical Microscopy and Analysis Laboratory Frederick National Laboratory for Cancer Research;

Molecular Targets Program Center for Cancer Research National Cancer Institute National Institutes of Health;

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原文格式 PDF
正文语种 eng
中图分类普通生物学;生物化学;
关键词
natural products; microRNA; pre-miR-21; differential scanning fluorometry; colon cancer;

机译：天然产品;microRNA;前miR-21;差分扫描荧光测定法;结肠癌;

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1. The Natural Product Butylcycloheptyl Prodiginine Binds Pre-miR-21, Inhibits Dicer-Mediated Processing of Pre-miR-21, and Blocks Cellular Proliferation [J] . Joe S. Matarlo, Lauren R.H. Krumpe, William F. Heinz, Cell chemical biology . 2019,第8期

机译：天然产物丁基环蟾酸Propiginine结合miR-21，抑制Dicer介导的预热剂-11的加工，并阻断细胞增殖
2. Inhibitory effect of ODN, a naturally occurring processing product of diazepam binding inhibitor, on secretagogues-induced insulin secretion. [J] . De Stefanis P, Impagnatiello F, Berkovich A, Regulatory peptides. . 1995,第2a3期

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3. Identification of a Novel Blocker of I{kappa}B{alpha} Kinase That Enhances Cellular Apoptosis and Inhibits Cellular Invasion through Suppression of NF-{kappa}B-Regulated Gene Products. [J] . Ichikawa H, Takada Y, Murakami A, The Journal of Immunology: Official Journal of the American Association of Immunologists . 2005,第11期

机译：通过抑制NF-κB调控基因产物，增强细胞凋亡并抑制细胞侵袭的IκBBα激酶新型阻断剂的鉴定。
4. Identification of natural products as an inhibitor of β-OG pocket binder of dengue virus envelope protein using fragment-based drug design and molecular docking approach [C] . U. S. F. Tambunan, A. H. Alkaff International Symposium on Current Progress in Mathematics and Sciences . 2018

机译：用基于片段的药物设计和分子对接方法鉴定天然产物作为登革热病毒包膜蛋白β-OG口袋粘合剂的抑制剂
5. Analysis of the binding mechanisms and cellular targets of peptide inhibitors that block site-specific recombination in vitro. [D] . Kepple, Kevin V. 2006

机译：分析在体外阻断位点特异性重组的肽抑制剂的结合机制和细胞靶标。
6. β-Cell pre-mir-21 induces dysfunction and loss of cellular identity by targeting transforming growth factor beta 2 (Tgfb2) and Smad family member 2 (Smad2) mRNAs [O] . Sara Ibrahim, Macey Johnson, Clarissa Hernandez Stephens, 2021

机译：β-细胞前miR-21通过靶向转化生长因子β2（TGFB2）和Smad家族成员2（Smad2）MRNA来诱导功能障碍和细胞同一性的功能障碍和丧失
7. p-SMAD2/3 and DICER promote pre-miR-21 processing during pressure overload-associated myocardial remodeling [O] . García Raquel, Nistal J. Francisco, Merino David, 2015

机译：p-SMAD2 / 3和DICER在压力超负荷相关的心肌重塑过程中促进pre-miR-21加工

The Natural Product Butylcycloheptyl Prodiginine Binds Pre-miR-21, Inhibits Dicer-Mediated Processing of Pre-miR-21, and Blocks Cellular Proliferation

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