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USE OF MIR-494 TO MODULATE TRAIL-INDUCED APOPTOSIS THROUGH BIM DOWN-REGULATION

机译:使用MIR-494通过BIM下调调节小径诱导的细胞凋亡

摘要

Methods and compositions for inhibiting tumorigenicity both in vitro and in vivo in a subject in need thereof, comprising administering an effective amount of an anti-miR-494 nucleic acid construct sufficient to target one or more tumor suppressor genes (TSGs) are described. Activation of the ERK1/2 pathway is a major determinant of diverse cellular processes and cancer development and is responsible for the transcription of several important miRNAs. Described herein is a link between the ERK1/2 pathway and BIM expression through miR-494. This ERK1/2 pathway regulates apoptosis and cell proliferation through miR-494 and mechanisms responsible for TRAIL resistance. Materials and methods related to the study and treatment of cancer are described.
机译:描述了用于在有需要的受试者中体内和体外抑制致瘤性的方法和组合物,包括给予足以靶向一种或多种肿瘤抑制基因(TSG)的有效量的抗miR-494核酸构建体。 ERK1 / 2途径的激活是多种细胞过程和癌症发展的主要决定因素,并负责几个重要miRNA的转录。本文描述的是ERK1 / 2途径与通过miR-494的BIM表达之间的联系。该ERK1 / 2途径通过miR-494和负责TRAIL抗性的机制调节细胞凋亡和细胞增殖。描述了与癌症的研究和治疗有关的材料和方法。

著录项

  • 公开/公告号EP2897648A4

    专利类型

  • 公开/公告日2016-06-22

    原文格式PDF

  • 申请/专利权人 THE OHIO STATE UNIVERSITY;

    申请/专利号EP20130838838

  • 发明设计人 CROCE CARLO M.;GIULIA ROMANO;

    申请日2013-09-23

  • 分类号A61K48;A61K31/7105;C12Q1/68;G01N33/50;

  • 国家 EP

  • 入库时间 2022-08-21 14:51:02

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