Literature DB >> 26835354

Lin28 and let-7 in cell metabolism and cancer.

Liem H Nguyen1, Hao Zhu1.   

Abstract

Malignant cells exhibit major metabolic alterations. The regulatory gene networks that regulate metabolism and the impact of these alterations on overall cellular fitness deserve further exploration. The let-7 microRNAs and their antagonists, the Lin28 RNA-binding proteins, are well-known for controlling the timing of embryonic development. This pathway has recently been shown to regulate glucose metabolism in adult mice and to reprogram metabolism during tissue injury and repair. In addition, many lines of evidence have established that Lin28 is an oncogene that drives tumorigenesis in part by suppressing let-7. The metabolic underpinnings of this oncogenic program are just beginning to be uncovered. Here, we will review the current understanding of how Lin28 exerts regenerative and oncogenic effects through metabolic mechanisms.

Entities:  

Keywords:  Lin28, let-7; cancer; metabolism; regeneration

Year:  2015        PMID: 26835354      PMCID: PMC4729067          DOI: 10.3978/j.issn.2224-4336.2015.01.05

Source DB:  PubMed          Journal:  Transl Pediatr        ISSN: 2224-4336


  71 in total

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6.  Reduced expression of the let-7 microRNAs in human lung cancers in association with shortened postoperative survival.

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7.  A feedback loop comprising lin-28 and let-7 controls pre-let-7 maturation during neural stem-cell commitment.

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7.  Lin28a overexpression reveals the role of Erk signaling in articular cartilage development.

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8.  Achillea Wilhelmsii C. KochHydroalcoholic Extract Induces Apoptosis and Alters LIN28B and p53 Gene Expression in Hela Cervical Cancer Cells.

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