Blood cell counts often fail to report on immune processes occurring in remote tissues. Here, we use immune cell type-specific methylation patterns in circulating cell-free DNA (cfDNA) for studying human immune cell dynamics. We characterized cfDNA released from specific immune cell types in healthy individuals (N = 242), cross sectionally and longitudinally. Immune cfDNA levels had no individual steady state as opposed to blood cell counts, suggesting that cfDNA concentration reflects adjustment of cell survival to maintain homeostatic cell numbers. We also observed selective elevation of immune-derived cfDNA upon perturbations of immune homeostasis. Following influenza vaccination (N = 92), B-cell-derived cfDNA levels increased prior to elevated B-cell counts and predicted efficacy of antibody production. Patients with eosinophilic esophagitis (N = 21) and B-cell lymphoma (N = 27) showed selective elevation of eosinophil and B-cell cfDNA, respectively, which were undetectable by cell counts in blood. Immune-derived cfDNA provides a novel biomarker for monitoring immune responses to physiological and pathological processes that are not accessible using conventional methods.
Remote immune processes revealed by immune-derived circulating cell-free DNA.
通过免疫来源的循环游离DNA揭示远程免疫过程
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作者:Fox-Fisher Ilana, Piyanzin Sheina, Ochana Bracha Lea, Klochendler Agnes, Magenheim Judith, Peretz Ayelet, Loyfer Netanel, Moss Joshua, Cohen Daniel, Drori Yaron, Friedman Nehemya, Mandelboim Michal, Rothenberg Marc E, Caldwell Julie M, Rochman Mark, Jamshidi Arash, Cann Gordon, Lavi David, Kaplan Tommy, Glaser Benjamin, Shemer Ruth, Dor Yuval
| 期刊: | Elife | 影响因子: | 6.400 |
| 时间: | 2021 | 起止号: | 2021 Nov 29; 10:e70520 |
| doi: | 10.7554/eLife.70520 | 研究方向: | 免疫/内分泌 |
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