骨髓移植将年龄相关的易感性转移到小鼠激光诱导脉络膜新生血管化中的新生血管重塑中。
Bone marrow transplantation transfers age-related susceptibility to neovascular remodeling in murine laser-induced choroidal neovascularization.
机构信息
The Duke Center for Macular Diseases, Duke Eye Center, Durham, North Carolina.
出版信息
Invest Ophthalmol Vis Sci. 2013 Nov 13;54(12):7439-49. doi: 10.1167/iovs.13-12546.
PURPOSE
Neovascular remodeling (NVR), the progression of small capillaries into large-caliber arterioles with perivascular fibrosis, represents a major therapeutic challenge in neovascular age-related macular degeneration (AMD). Neovascular remodeling occurs after laser-induced choroidal neovascularization (CNV) in aged but not young mice. Additionally, bone marrow-derived cells, including macrophages, endothelial precursor cells, and mesenchymal precursor cells, contribute to CNV severity. In this study, we investigated the impact of aged bone marrow transplantation (BMT) on the degree of fibrosis, size, and vascular morphology of CNV lesions in a mouse model of laser-induced CNV.
METHODS
Young (2 months) and old (16 months) mice were transplanted with green fluorescent protein (GFP)-labeled bone marrow isolated from either young or old donors. Laser CNV was induced 1 month following transplant, and eyes were analyzed via choroidal flat mounts and immunohistochemistry 1 month postlaser. The identity of cells infiltrating CNV lesions was determined using specific markers for the labeled transplanted cells (GFP+), macrophages (F4/80+), perivascular mesenchymal-derived cells (smooth muscle actin, SMA+), and endothelial cells (CD31+).
RESULTS
Bone marrow transplantation from aged mice transferred susceptibility to NVR into young recipients. Inversely, transplantation of young marrow into old mice prevented NVR, preserving small size and minimal fibrosis. Mice with NVR demonstrated a greater relative contribution of marrow-derived SMA+ perivascular mesenchymal cells as compared to other cells.
CONCLUSIONS
Our findings indicate that the status of bone marrow is an important determining factor of neovascular severity. Furthermore, we find that perivascular mesenchymal cells, rather than endothelial cells, derived from aged bone marrow may contribute to increased CNV severity in this murine model of experimental neovascularization.
目的
新血管重构(NVR)是指小毛细血管向大口径小动脉的进展,伴有血管周围纤维化,是新生血管性年龄相关性黄斑变性(AMD)的主要治疗挑战。在老年但不是年轻的小鼠中,激光诱导脉络膜新生血管(CNV)后会发生新血管重构。此外,骨髓来源的细胞,包括巨噬细胞、内皮前体细胞和间充质前体细胞,有助于 CNV 的严重程度。在这项研究中,我们研究了老年骨髓移植(BMT)对激光诱导 CNV 小鼠模型中 CNV 病变纤维化程度、大小和血管形态的影响。
方法
年轻(2 个月)和老年(16 个月)小鼠分别接受来自年轻或老年供体的 GFP 标记骨髓移植。移植后 1 个月诱导激光 CNV,激光后 1 个月通过脉络膜平铺和免疫组织化学分析眼睛。使用标记的移植细胞(GFP+)、巨噬细胞(F4/80+)、血管周围间充质来源细胞(平滑肌肌动蛋白,SMA+)和内皮细胞(CD31+)的特异性标记物确定浸润 CNV 病变的细胞的身份。
结果
来自老年小鼠的骨髓移植将易感性转移到年轻受体中,导致 NVR。相反,将年轻骨髓移植到老年小鼠中可防止 NVR,保持较小的大小和最小的纤维化。发生 NVR 的小鼠显示骨髓来源的 SMA+血管周围间充质细胞的相对贡献大于其他细胞。
结论
我们的发现表明骨髓状态是新生血管严重程度的重要决定因素。此外,我们发现源自老年骨髓的血管周围间充质细胞而不是内皮细胞可能有助于增加该实验性新生血管小鼠模型中 CNV 的严重程度。
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