Polyamine metabolism is a central determinant of helper T cell lineage fidelity | Zendy

Daniel J. Puleston | Zendy; Francesc Baixauli | Zendy; David E. Sanin | Zendy; Joy Edwards-Hicks | Zendy; Matteo Villa | Zendy; Agnieszka M. Kabat | Zendy; Marcin M. Kamiński | Zendy; Michal Stanckzak | Zendy; Hauke J. Weiss | Zendy; Katarzyna M. Grzes | Zendy; Klara Piletič | Zendy; Cameron S. Field | Zendy; Mauro Corrado | Zendy; Fabian Haessler | Zendy; Chao Wang | Zendy; Yaarub Musa | Zendy; Lena Schimmelpfennig | Zendy; Lea J. Flachsmann | Zendy; Gerhard Mittler | Zendy; Nir Yosef | Zendy; Vijay K. Kuchroo | Zendy; Joerg M. Buescher | Zendy; Stefan Balabanov | Zendy; Edward J. Pearce | Zendy; Douglas R. Green | Zendy; Erika L. Pearce | Zendy

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Polyamine metabolism is a central determinant of helper T cell lineage fidelity

Author(s) -

Daniel J. Puleston,

Francesc Baixauli,

David E. Sanin,

Joy Edwards-Hicks,

Matteo Villa,

Agnieszka M. Kabat,

Marcin M. Kamiński,

Michal Stanckzak,

Hauke J. Weiss,

Katarzyna M. Grzes,

Klara Piletič,

Cameron S. Field,

Mauro Corrado,

Fabian Haessler,

Chao Wang,

Yaarub Musa,

Lena Schimmelpfennig,

Lea J. Flachsmann,

Gerhard Mittler,

Nir Yosef,

Vijay K. Kuchroo,

Joerg M. Buescher,

Stefan Balabanov,

Edward J. Pearce,

Douglas R. Green,

Erika L. Pearce

Publication year - 2021

Publication title -

cell

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 26.304

H-Index - 776

eISSN - 1097-4172

pISSN - 0092-8674

DOI - 10.1016/j.cell.2021.06.007

Subject(s) - biology , lineage (genetic) , cell lineage , microbiology and biotechnology , metabolism , fidelity , cell metabolism , evolutionary biology , genetics , cell , cellular differentiation , gene , biochemistry , electrical engineering , engineering

Summary Polyamine synthesis represents one of the most profound metabolic changes during T cell activation, but the biological implications of this are scarcely known. Here, we show that polyamine metabolism is a fundamental process governing the ability of CD4 + helper T cells (T H ) to polarize into different functional fates. Deficiency in ornithine decarboxylase, a crucial enzyme for polyamine synthesis, results in a severe failure of CD4 + T cells to adopt correct subset specification, underscored by ectopic expression of multiple cytokines and lineage-defining transcription factors across T H cell subsets. Polyamines control T H differentiation by providing substrates for deoxyhypusine synthase, which synthesizes the amino acid hypusine, and mice in which T cells are deficient for hypusine develop severe intestinal inflammatory disease. Polyamine-hypusine deficiency caused widespread epigenetic remodeling driven by alterations in histone acetylation and a re-wired tricarboxylic acid (TCA) cycle. Thus, polyamine metabolism is critical for maintaining the epigenome to focus T H cell subset fidelity.

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