间质细胞
造血
骨髓
间充质干细胞
生物
癌症研究
人口
祖细胞
免疫学
骨髓增生异常综合症
淋巴结间质细胞
炎症
利基
干细胞
细胞生物学
脂肪生成
髓样
医学
作者
Karin D. Prummel,Kevin Woods,Maksim Kholmatov,Eric C. Schmitt,Evi P. Vlachou,Mayssa Labyadh,Rebekka Wehner,Gereon Poschmann,Kai Stühler,Susann Winter,Uta Oelschlaegel,Manja Wobus,Logan S. Schwartz,Pedro L. Moura,Eva Hellström-Lindberg,Krishnaraj Rajalingam,Matthias Theobald,Jennifer J. Trowbridge,Clémence Carron,Thierry Jaffredo
标识
DOI:10.1038/s41467-025-65803-y
摘要
Abstract Somatic mutations in hematopoietic stem/progenitor cells (HSPCs) can lead to clonal hematopoiesis of indeterminate potential (CHIP) and progression to myelodysplastic syndromes (MDS). Using single-cell and anatomical profiling of a large cohort of human bone marrow (BM), we show that the HSPC BM niche in CHIP and MDS is undergoing inflammatory remodeling. This includes loss of CXCL12⁺ adipogenic stromal cells and the emergence of a distinct population of inflammatory mesenchymal stromal cells (iMSCs), which arise in CHIP and become more prevalent in MDS. Functional studies in primary BM HSPC-MSC co-cultures reveals that healthy aged and CHIP HSPCs activate stromal support, while MDS HSPCs fail to do so. In contrast, MDS blasts further suppress HSPC support and trigger inflammation, indicating disease-stage-specific stromal disruption. In parallel, we show that iMSCs retain partial support and angiogenic potential in MDS, coinciding with expanded BM vasculature. Additionally, we identify IFN-responsive T cells that preferentially interact with iMSCs, potentially reinforcing local inflammation. These findings position iMSCs as central mediators of early BM niche dysfunction and potential therapeutic targets for intercepting pre-malignant hematopoiesis.
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