T cell monocyte complexes exhibit distinct immune signatures during infection.
Abstract
Communication between immune cells through direct contact is a critical feature of immune responses. Here, we developed an innovative high-throughput workflow to study the transcriptome and adaptive immune receptor repertoire of single cells forming complexes without needing bioinformatic deconvolution. We found that T cells and monocytes forming complexes in blood during active tuberculosis (TB) and dengue hold distinct transcriptomic signatures from singlets, with the upregulation of genes associated with immune activation and MHC-II complex. Additionally, in TB, T cells in complexes showed enrichment for cytotoxic T cells, higher TCR clonality, and increased immune activity at diagnosis compared to after anti-TB therapy. We also found that T cells and monocytes forming complexes were markedly enriched for "dual-expressing" cells (i.e., co-expressing T cell and monocyte genes), suggesting intercellular RNA acquisition occurs during cell-cell interactions. Thus, studying immune cell complexes at single-cell resolution provides insights into immune cell-cell interactions in the blood during infection.
| Authors: | Kang N, Chawla A, Hillman H, Tippalagama R, Kim C, Mikulski Z, McArdle S, Seumois G, Vijayanand P, Scriba TJ, De Silva AD, Balmaseda A, Harris E, Weiskopf D, Sette A, Arlehamn CL, Peters B, Burel JG, |
|---|---|
| Journal: | iScience;2025Sep19; 28 (9) 113432. doi:10.1016/j.isci.2025.113432 |
| Year: | 2025 |
| PubMed: | PMID: 40989028 (Go to PubMed) |