PTEN is required for human Treg suppression of costimulation in vitro.
Avery J LamManjurul HaqueKirsten A Ward-HartstongePrakruti UdayChristine M WardellJana K GilliesMadeleine SpeckMajid MojibianRamon I Klein GeltinkMegan K LevingsPublished in: European journal of immunology (2022)
Regulatory T-cell (Treg) therapy is under clinical investigation for the treatment of transplant rejection, autoimmune disease, and graft-versus-host disease. With the advent of genome editing, attention has turned to reinforcing Treg function for therapeutic benefit. A hallmark of Tregs is dampened activation of PI3K-AKT signaling, of which PTEN is a major negative regulator. Loss-of-function studies of PTEN, however, have not conclusively shown a requirement for PTEN in upholding Treg function and stability. Using CRISPR-based genome editing in human Tregs, we show that PTEN ablation does not cause a global defect in Treg function and stability; rather, it selectively blocks their ability to suppress antigen-presenting cells. PTEN-KO Tregs exhibit elevated glycolytic activity, upregulate FOXP3, maintain a Treg phenotype, and have no discernible defects in lineage stability. Functionally, PTEN is dispensable for human Treg-mediated inhibition of T-cell activity in vitro and in vivo but is required for suppression of costimulatory molecule expression by antigen-presenting cells. These data are the first to define a role for a signaling pathway in controlling a subset of human Treg activity. Moreover, they point to the functional necessity of PTEN-regulated PI3K-AKT activity for optimal human Treg function.
Keyphrases
- pi k akt
- signaling pathway
- cell cycle arrest
- cell proliferation
- genome editing
- endothelial cells
- crispr cas
- induced apoptosis
- pluripotent stem cells
- induced pluripotent stem cells
- transcription factor
- poor prognosis
- dna methylation
- bone marrow
- gene expression
- machine learning
- electronic health record
- cell death
- radiofrequency ablation
- drug induced