Stage 1 type 1 diabetes memory B lymphocytes transcriptionally differ from healthy controls and harbor insulin-binding specificities
Lindsay E Bass, Wyatt J McDonnell, Christina T Brannon, Nilesh P Kumar, Simon A Mallal, Ivelin S Georgiev, James W Thomas, Daniel J Moore, Rachel H Bonami

TL;DR
Early-stage type 1 diabetes B cells show unique gene activity and insulin-binding traits compared to healthy individuals.
Contribution
Identified transcriptional and BCR differences in early-stage T1D B cells with insulin-binding specificities.
Findings
Stage 1 T1D memory B cells upregulate 122 genes related to BCR signaling and antigen presentation.
Atypical-like memory B cells show reduced somatic hypermutation and insulin-binding specificities.
Insulin-binding B cells exhibit non-significant gene upregulation in key B cell functions.
Abstract
Autoreactive B cell activity defines the earliest detectable stage (Stage 1) of type 1 diabetes (T1D) but is incompletely understood, particularly for B cells reactive against the key T1D autoantigen, insulin. To test whether Stage 1 T1D B cells are transcriptionally rewired compared to healthy individuals, we performed single-cell transcriptional, phenotypic, and immune repertoire profiling of CD19+ cells isolated from the peripheral blood of Stage 1 T1D individuals, identified via Type 1 Diabetes TrialNet as being positive for ≥ 2/5 islet autoantibodies, and healthy controls. Stage 1 T1D memory B cells upregulated n = 122 genes compared to healthy controls, including genes involved in actin cytoskeleton rearrangement, B cell receptor (BCR) signaling, and antigen presentation, and exhibited reduced BCR somatic hypermutation, particularly in atypical-like memory B cells. Clonally…
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Taxonomy
TopicsDiabetes and associated disorders · Pancreatic function and diabetes · T-cell and B-cell Immunology
