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- Title
- Txnip regulates the Oct4-mediated pluripotency circuitry via metabolic changes upon differentiation
- Author(s)
- SoJung Kwak; Cho Lok Song; Yee Sook Cho; In Pyo Choi; Jae Eun Byun; Haiyoung Jung; Jungwoon Lee
- Bibliographic Citation
- Cellular and Molecular Life Sciences, vol. 81, pp. 142-142
- Publication Year
- 2024
- Abstract
- Thioredoxin interacting protein (Txnip) is a stress-responsive factor regulating Trx1 for redox balance and involved in diverse cellular processes including proliferation, differentiation, apoptosis, inflammation, and metabolism. However, the biological role of Txnip function in stem cell pluripotency has yet to be investigated. Here, we reveal the novel functions of mouse Txnip in cellular reprogramming and differentiation onset by involving in glucose-mediated histone acetylation and the regulation of Oct4, which is a fundamental component of the molecular circuitry underlying pluripotency. During reprogramming or PSC differentiation process, cellular metabolic and chromatin remodeling occur in order to change its cellular fate. Txnip knockout promotes induced pluripotency but hinders initial differentiation by activating pluripotency factors and promoting glycolysis. This alteration affects the intracellular levels of acetyl-coA, a final product of enhanced glycolysis, resulting in sustained histone acetylation on active PSC gene regions. Moreover, Txnip directly interacts with Oct4, thereby repressing its activity and consequently deregulating Oct4 target gene transcriptions. Our work suggests that control of Txnip expression is crucial for cell fate transitions by modulating the entry and exit of pluripotency.
- Keyword
- Thioredoxin interacting protein (Txnip)Pluripotent stem cells (PSCs)ReprogrammingPluripotencyDiferentiationGlycolysisHistone acetylationOct4
- ISSN
- 1420-682X
- Publisher
- Springer
- Full Text Link
- http://dx.doi.org/10.1007/s00018-024-05161-y
- Type
- Article
- Appears in Collections:
- Division of A.I. & Biomedical Research > Immunotherapy Research Center > 1. Journal Articles
Aging Convergence Research Center > 1. Journal Articles
Division of Research on National Challenges > Environmental diseases research center > 1. Journal Articles
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