4.6 Review

MicroRNA-210 A unique and pleiotropic hypoxamir

Journal

CELL CYCLE
Volume 9, Issue 6, Pages 1072-1083

Publisher

TAYLOR & FRANCIS INC
DOI: 10.4161/cc.9.6.11006

Keywords

microRNA; hypoxia; miR-210; hypoxia inducible factor; metabolism; proliferation; angiogenesis; apoptosis; cell cycle; Pasteur effect

Categories

Funding

  1. AHA [0825906D]
  2. NIH [HL 61795, NO1 HV 28178, PO1 81587, U54 HL 70819]

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Inadequate oxygen availability or hypoxia induces a complex and still incompletely understood set of adaptations that influence cellular survival and function. Many of these adaptations are directly controlled by a master transcription factor, hypoxia inducible factor-alpha (HIF-alpha). In response to hypoxia, HIF-alpha levels increase and directly induce the transcription of > 100 genes, influencing functions ranging from metabolism, survival, proliferation, migration, to angiogenesis, among others. Recently, it has been demonstrated that a specific set of microRNA molecules are upregulated by hypoxia, which we denote here as hypoxamirs. In particular, the HIF-responsive hypoxamir microRNA-210 (miR-210) is a unique microRNA that is evolutionarily conserved and ubiquitously expressed in hypoxic cell and tissue types. A number of direct targets of miR-210 have been identified by in silico, transcriptional and biochemical methods, a subset of which have been extensively validated. As a result, miR-210 has been mechanistically linked to the control of a wide range of cellular responses known to influence normal developmental physiology as well as a number of hypoxia-dependent disease states, including tissue ischemia, inflammation and tumorigenesis. Thus, reflecting the pleiotropic actions of HIF-alpha, miR-210 appears to function as a master microRNA relevant for the control of diverse functions in the hypoxic state.

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