Islet-autoreactive CD4+ T cells are linked with response to alefacept in type 1 diabetes
Elisa Balmas, Janice Chen, Alex K. Hu, Hannah A. DeBerg, Mario G. Rosasco, Vivian H. Gersuk, Elisavet Serti, Cate Speake, Carla J. Greenbaum, Gerald T. Nepom, Peter S. Linsley, Karen Cerosaletti
Elisa Balmas, Janice Chen, Alex K. Hu, Hannah A. DeBerg, Mario G. Rosasco, Vivian H. Gersuk, Elisavet Serti, Cate Speake, Carla J. Greenbaum, Gerald T. Nepom, Peter S. Linsley, Karen Cerosaletti
View: Text | PDF
Research Article

Islet-autoreactive CD4+ T cells are linked with response to alefacept in type 1 diabetes

Abstract

Variation in the preservation of β cell function in clinical trials in type 1 diabetes (T1D) has emphasized the need to define biomarkers to predict treatment response. The T1DAL trial targeted T cells with alefacept (LFA-3–Ig) and demonstrated C-peptide preservation in approximately 30% of new-onset T1D individuals. We analyzed islet antigen–reactive (IAR) CD4+ T cells in PBMC samples collected prior to treatment from alefacept- and placebo-treated individuals using flow cytometry and single-cell RNA sequencing. IAR CD4+ T cells at baseline had heterogeneous phenotypes. Transcript profiles formed phenotypic clusters of cells along a trajectory based on increasing maturation and activation, and T cell receptor (TCR) chains showed clonal expansion. Notably, the frequency of IAR CD4+ T cells with a memory phenotype and a unique transcript profile (cluster 3) were inversely correlated with C-peptide preservation in alefacept-treated, but not placebo-treated, individuals. Cluster 3 cells had a proinflammatory phenotype characterized by expression of the transcription factor BHLHE40 and the cytokines GM-CSF and TNF-α, and shared TCR chains with effector memory–like clusters. Our results suggest IAR CD4+ T cells as a potential baseline biomarker of response to therapies targeting the CD2 pathway and warrant investigation for other T cell–related therapies.

Authors

Elisa Balmas, Janice Chen, Alex K. Hu, Hannah A. DeBerg, Mario G. Rosasco, Vivian H. Gersuk, Elisavet Serti, Cate Speake, Carla J. Greenbaum, Gerald T. Nepom, Peter S. Linsley, Karen Cerosaletti

×

Figure 4

The frequency of IAR CD4+ T cells with a cluster 3 phenotype is linked with C-peptide change in alefacept-treated new-onset T1D patients.

Options: View larger image (or click on image) Download as PowerPoint
The frequency of IAR CD4+ T cells with a cluster 3 phenotype is linked w...
(A) Heatmap representation of adjusted P values from Spearman’s correlations of the fraction of IAR CD4+ T cells per individual in each Monocle cluster versus the rate of C-peptide change in alefacept-treated (n = 11) and placebo-treated (n = 7) participants over the 2-year clinical trial, as listed in Table 1. Spearman’s r values are shown in each square. (B) Correlation between the fraction of IAR CD4+ T cells per individual in cluster 3, with rate of C-peptide change in alefacept- and placebo-treated individuals performed as in A. The linear regression line is shown with 95% confidence intervals in dotted lines. (C) Spearman’s correlation of the fraction of IAR CD4+ T cells subject in Monocle cluster 3 versus the frequency of IAR CD4+ TCM cells per 1 × 106 CD4+ T cells in PBMCs from alefacept- (n = 11) or placebo-treated (n = 7) individuals. P values were adjusted for multiple testing using the Benjamini-Hochberg test correction.