Stem Cell Reports (Mar 2017)

A Role for KLF4 in Promoting the Metabolic Shift via TCL1 during Induced Pluripotent Stem Cell Generation

  • Ken Nishimura,
  • Shiho Aizawa,
  • Fransiska Liliani Nugroho,
  • Emi Shiomitsu,
  • Yen Thi Hai Tran,
  • Phuong Linh Bui,
  • Evgeniia Borisova,
  • Yuta Sakuragi,
  • Hitomi Takada,
  • Akira Kurisaki,
  • Yohei Hayashi,
  • Aya Fukuda,
  • Mahito Nakanishi,
  • Koji Hisatake

DOI
https://doi.org/10.1016/j.stemcr.2017.01.026
Journal volume & issue
Vol. 8, no. 3
pp. 787 – 801

Abstract

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Reprogramming of somatic cells into induced pluripotent stem cells (iPSCs) is accompanied by morphological, functional, and metabolic alterations before acquisition of full pluripotency. Although the genome-wide effects of the reprogramming factors on gene expression are well documented, precise mechanisms by which gene expression changes evoke phenotypic responses remain to be determined. We used a Sendai virus-based system that permits reprogramming to progress in a strictly KLF4-dependent manner to screen for KLF4 target genes that are critical for the progression of reprogramming. The screening identified Tcl1 as a critical target gene that directs the metabolic shift from oxidative phosphorylation to glycolysis. KLF4-induced TCL1 employs a two-pronged mechanism, whereby TCL1 activates AKT to enhance glycolysis and counteracts PnPase to diminish oxidative phosphorylation. These regulatory mechanisms described here highlight a central role for a reprogramming factor in orchestrating the metabolic shift toward the acquisition of pluripotency during iPSC generation.

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