Severe immune aplastic anemia is a fatal disease due to the destruction of marrow hematopoietic cells by cytotoxic lymphocytes, serving as a paradigm for marrow failure syndromes and autoimmune diseases. To better understand its pathophysiology, we apply advanced single cell methodologies, including mass cytometry, single-cell RNA, and TCR/BCR sequencing, to patient samples from a clinical trial of immunosuppression and growth factor stimulation. We observe opposing changes in the abundance of myeloid cells and T cells, with T cell clonal expansion dominated by effector memory cells. Therapy reduces and suppresses cytotoxic T cells, but new T cell clones emerge hindering robust hematopoietic recovery. Enhanced cell-cell interactions including between hematopoietic cells and immune cells, in particular evolving IFNG and IFNGR, are noted in patients and are suppressed post-therapy. Hematologic recovery occurs with increases in the progenitor rather than stem cells. Genetic predispositions linked to immune activation genes enhances cytotoxic T cell activity and crosstalk with target cells.
Human autoimmunity at single cell resolution in aplastic anemia before and after effective immunotherapy.
有效免疫治疗前后再生障碍性贫血中单细胞分辨率的人类自身免疫
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作者:Wu Zhijie, Gao Shouguo, Feng Xingmin, Li Haoran, Sompairac Nicolas, Jamshidi Shirin, Choy Desmond, Reis Rita Antunes Dos, Gao Qingyan, Kajigaya Sachiko, Alemu Lemlem, Raffo Diego Quinones, Groarke Emma M, Kordasti Shahram, Patel Bhavisha A, Young Neal S
| 期刊: | Nature Communications | 影响因子: | 15.700 |
| 时间: | 2025 | 起止号: | 2025 May 30; 16(1):5048 |
| doi: | 10.1038/s41467-025-60213-6 | 种属: | Human |
| 研究方向: | 细胞生物学 | ||
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