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Bone marrow-derived endothelial progenitor cells are a major determinant of nascent tumor neovascularization

机译:骨髓来源的内皮祖细胞是新生肿瘤新生血管形成的主要决定因素

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摘要

Tumors build vessels by cooption of pre-existing vasculature and de novo recruitment of bone marrow (BM)-derived endothelial progenitor cells (EPCs). However, the contribution and the functional role of EPCs in tumor neoangiogenesis are controversial. Therefore, by using genetically marked BM progenitor cells, we demonstrate the precise spatial and temporal contribution of EPCs to the neovascularization of three transplanted and one spontaneous breast tumor in vivo using high-resolution microscopy and flow cytometry. We show that early tumors recruit BM-derived EPCs that differentiate into mature BM-derived endothelial cells (ECs) and luminally incorporate into a subset of sprouting tumor neovessels. Notably, in later tumors, these BM-derived vessels are diluted with non-BM-derived vessels from the periphery, which accounts for purported differences in previously published reports. Furthermore, we show that specific ablation of BM-derived EPCs with α-particle-emitting anti-VE-cadherin antibody markedly impaired tumor growth associated with reduced vascularization. Our results demonstrate that BM-derived EPCs are critical components of the earliest phases of tumor neoangiogenesis.
机译:肿瘤通过预先存在的脉管系统和从骨髓(BM)衍生的内皮祖细胞(EPC)的从头募集来构建血管。然而,EPC在肿瘤新血管生成中的贡献和功能作用是有争议的。因此,通过使用遗传标记的BM祖细胞,我们使用高分辨率的显微镜和流式细胞仪证明了EPC在体内对三个已移植和一个自发性乳腺肿瘤的新血管形成的精确时空贡献。我们显示,早期肿瘤募集了BM衍生的EPC,这些EPC分化为成熟的BM衍生的内皮细胞(EC),并在发光中整合到了新芽的肿瘤新血管中。值得注意的是,在以后的肿瘤中,这些BM来源的血管从周围被非BM来源的血管稀释,这解释了先前发表的报道中所声称的差异。此外,我们显示与α发射抗VE-钙黏着蛋白抗体的BM衍生的EPCs的特异性消融明显损害了与血管生成减少相关的肿瘤生长。我们的结果表明,BM衍生的EPC是肿瘤新血管生成最早阶段的关键组成部分。

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