Dynamic changes in the regulatory T-cell heterogeneity and function by murine IL-2 mutein

Author:

Lu Daniel R1ORCID,Wu Hao2,Driver Ian1ORCID,Ingersoll Sarah2,Sohn Sue2ORCID,Wang Songli1,Li Chi-Ming1ORCID,Phee Hyewon2ORCID

Affiliation:

1. Genome Analysis Unit, Amgen Research, Amgen Inc, South San Francisco, CA, USA

2. Department of Oncology and Inflammation, Amgen Research, Amgen Inc, South San Francisco, CA, USA

Abstract

The therapeutic expansion of Foxp3+ regulatory T cells (Tregs) shows promise for treating autoimmune and inflammatory disorders. Yet, how this treatment affects the heterogeneity and function of Tregs is not clear. Using single-cell RNA-seq analysis, we characterized 31,908 Tregs from the mice treated with a half-life extended mutant form of murine IL-2 (IL-2 mutein, IL-2M) that preferentially expanded Tregs, or mouse IgG Fc as a control. Cell clustering analysis revealed that IL-2M specifically expands multiple sub-states of Tregs with distinct expression profiles. TCR profiling with single-cell analysis uncovered Treg migration across tissues and transcriptional changes between clonally related Tregs after IL-2M treatment. Finally, we identified IL-2M–expanded Tnfrsf9+Il1rl1+ Tregs with superior suppressive function, highlighting the potential of IL-2M to expand highly suppressive Foxp3+ Tregs.

Publisher

Life Science Alliance, LLC

Subject

Health, Toxicology and Mutagenesis,Plant Science,Biochemistry, Genetics and Molecular Biology (miscellaneous),Ecology

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