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新型视黄醇-多胺偶联物在人永生化角质细胞中诱导的药物表遗传学回路。

Pharmacoepigenomics circuits induced by a novel retinoid-polyamine conjugate in human immortalized keratinocytes.

机构信息

Department of Biochemistry, School of Medicine, University of Patras, Patras, Greece.

Department of Dermatology, University Hospital of Patras, School of Medicine, University of Patras, Patras, Greece.

出版信息

Pharmacogenomics J. 2021 Dec;21(6):638-648. doi: 10.1038/s41397-021-00241-9. Epub 2021 Jun 18.

Abstract

Retinoids are widely used in diseases spanning from dermatological lesions to cancer, but exhibit severe adverse effects. A novel all-trans-Retinoic Acid (atRA)-spermine conjugate (termed RASP) has shown previously optimal in vitro and in vivo anti-inflammatory and anticancer efficacy, with undetectable teratogenic and toxic side-effects. To get insights, we treated HaCaT cells which resemble human epidermis with IC concentration of RASP and analyzed their miRNA expression profile. Gene ontology analysis of their predicted targets indicated dynamic networks involved in cell proliferation, signal transduction and apoptosis. Furthermore, DNA microarrays analysis verified that RASP affects the expression of the same categories of genes. A protein-protein interaction map produced using the most significant common genes, revealed hub genes of nodal functions. We conclude that RASP is a synthetic retinoid derivative with improved properties, which possess the beneficial effects of retinoids without exhibiting side-effects and with potential beneficial effects against skin diseases including skin cancer.

摘要

类视黄醇在从皮肤病变到癌症等各种疾病中都有广泛应用,但存在严重的不良反应。一种新型的全反式视黄酸(atRA)-精脒缀合物(称为 RASP)已显示出在体外和体内具有最佳的抗炎和抗癌疗效,且无致畸和毒性副作用。为了深入了解,我们用 RASP 处理类似于人类表皮的 HaCaT 细胞,并分析它们的 miRNA 表达谱。对其预测靶标的基因本体分析表明,涉及细胞增殖、信号转导和细胞凋亡的动态网络。此外,DNA 微阵列分析证实 RASP 影响了同一类基因的表达。使用最显著的共同基因生成的蛋白质-蛋白质相互作用图,揭示了具有节点功能的枢纽基因。我们得出结论,RASP 是一种具有改良特性的合成视黄醇衍生物,它具有视黄醇的有益作用,而没有表现出副作用,并具有治疗皮肤病(包括皮肤癌)的潜在益处。

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