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造血和基质细胞中标记的 DMP1-Cre 细胞在骨髓中形成一个独特的龛位。

Hematopoietic and stromal DMP1-Cre labeled cells form a unique niche in the bone marrow.

机构信息

Center for Regenerative Medicine and Skeletal Development, MC 3705, School of Dental Medicine, UConn Health, 263 Farmington Ave, Farmington, CT, 06030, USA.

Division of Pediatric Dentistry, MC1610, School of Dental Medicine, UConn Health, 263 Farmington Ave, Farmington, CT, 06030, USA.

出版信息

Sci Rep. 2023 Dec 16;13(1):22403. doi: 10.1038/s41598-023-49713-x.

Abstract

Skeletogenesis and hematopoiesis are interdependent. Niches form between cells of both lineages where microenvironmental cues support specific lineage commitment. Because of the complex topography of bone marrow (BM), the identity and function of cells within specialized niches has not been fully elucidated. Dentin Matrix Protein 1 (DMP1)-Cre mice have been utilized in bone studies as mature osteoblasts and osteocytes express DMP1. DMP1 has been identified in CXCL12 cells and an undefined CD45 population. We crossed DMP1-Cre with Ai9 reporter mice and analyzed the tdTomato (tdT) population in BM and secondary hematopoietic organs. CD45tdT express myeloid markers including CD11b and are established early in ontogeny. CD45tdT cells phagocytose, respond to LPS and are radioresistant. Depletion of macrophages caused a significant decrease in tdTCD11b myeloid populations. A subset of CD45tdT cells may be erythroid island macrophages (EIM) which are depleted after G-CSF treatment. tdTCXCL12 cells are in direct contact with F4/80 macrophages, express RANKL and form a niche with B220 B cells. A population of resident cells within the thymus are tdT and express myeloid markers and RANKL. In conclusion, in addition to targeting osteoblast/osteocytes, DMP1-Cre labels unique cell populations of macrophage and stromal cells within BM and thymus niches and expresses key microenvironmental factors.

摘要

成骨细胞生成和造血是相互依存的。细胞之间形成龛位,微环境线索支持特定谱系的承诺。由于骨髓(BM)的复杂拓扑结构,专门龛位中细胞的身份和功能尚未完全阐明。牙本质基质蛋白 1(DMP1)-Cre 小鼠已在骨研究中被用于研究,因为成熟成骨细胞和成骨细胞表达 DMP1。已经在 CXCL12 细胞和未定义的 CD45 群体中鉴定出 DMP1。我们将 DMP1-Cre 与 Ai9 报告小鼠杂交,并分析 BM 和次级造血器官中的 tdTomato(tdT)群体。CD45tdT 表达髓样标记物,包括 CD11b,并且在胚胎发生早期就已建立。CD45tdT 细胞吞噬、对 LPS 作出反应且具有辐射抗性。巨噬细胞耗竭导致 tdTCD11b 髓样群体显著减少。CD45tdT 细胞的一个亚群可能是红细胞岛巨噬细胞(EIM),在 G-CSF 处理后会被耗尽。tdTCXCL12 细胞与 F4/80 巨噬细胞直接接触,表达 RANKL 并与 B220 B 细胞形成龛位。胸腺内的一群固有细胞是 tdT,表达髓样标记物和 RANKL。总之,除了靶向成骨细胞/成骨细胞外,DMP1-Cre 还标记了 BM 和胸腺龛位中独特的巨噬细胞和基质细胞群体,并表达关键的微环境因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db33/10725438/65067880a0e1/41598_2023_49713_Fig1_HTML.jpg

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