4.7 Article

Regulation of L-Threonine Dehydrogenase in Somatic Cell Reprogramming

Journal

STEM CELLS
Volume 31, Issue 5, Pages 953-965

Publisher

WILEY
DOI: 10.1002/stem.1335

Keywords

TDH; miR-9; PRMT5; Arginine methylation; Somatic cell reprogramming

Funding

  1. Chinese Academy of Sciences [XDA01020104]
  2. Ministry of Science and Technology of China [2010CB912804, 2011CB966302]
  3. National Natural Science Foundation of China [31030046]
  4. Fundamental Research Funds for Central Universities (USTC) [WK2060190018]

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Increasing evidence suggests that metabolic remodeling plays an important role in the regulation of somatic cell reprogramming. Threonine catabolism mediated by L-threonine dehydrogenase (TDH) has been recognized as a specific metabolic trait of mouse embryonic stem cells. However, it remains unknown whether TDH-mediated threonine catabolism could regulate reprogramming. Here, we report TDH as a novel regulator of somatic cell reprogramming. Knockdown of TDH inhibits, whereas induction of TDH enhances reprogramming efficiency. Moreover, microRNA-9 post-transcriptionally regulates the expression of TDH and thereby inhibits reprogramming efficiency. Furthermore, protein arginine methyltransferase (PRMT5) interacts with TDH and mediates its post-translational arginine methylation. PRMT5 appears to regulate TDH enzyme activity through both methyltransferase-dependent and -independent mechanisms. Functionally, TDH-facilitated reprogramming efficiency is further enhanced by PRMT5. These results suggest that TDH-mediated threonine catabolism controls somatic cell reprogramming and indicate the importance of post-transcriptional and post-translational regulation of TDH. STEM CELLS 2013;31:953-965

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