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用于肿瘤植入的特殊骨髓内皮微区的体内成像。

In vivo imaging of specialized bone marrow endothelial microdomains for tumour engraftment.

作者信息

Sipkins Dorothy A, Wei Xunbin, Wu Juwell W, Runnels Judith M, Côté Daniel, Means Terry K, Luster Andrew D, Scadden David T, Lin Charles P

机构信息

Wellman Center for Photomedicine, Massachusetts General Hospital, Harvard Medical School, 55 Fruit St, Boston, Massachusetts 02114, USA.

出版信息

Nature. 2005 Jun 16;435(7044):969-73. doi: 10.1038/nature03703.

Abstract

The organization of cellular niches is known to have a key role in regulating normal stem cell differentiation and regeneration, but relatively little is known about the architecture of microenvironments that support malignant metastasis. Using dynamic in vivo confocal imaging, here we show that murine bone marrow contains unique anatomic regions defined by specialized endothelium. This vasculature expresses the adhesion molecule E-selectin and the chemoattractant stromal-cell-derived factor 1 (SDF-1) in discrete, discontinuous areas that influence the homing of a variety of tumour cell lines. Disruption of the interactions between SDF-1 and its receptor CXCR4 inhibits the homing of Nalm-6 cells (an acute lymphoblastic leukaemia cell line) to these vessels. Further studies revealed that circulating leukaemic cells can engraft around these vessels, suggesting that this molecularly distinct vasculature demarcates a microenvironment for early metastatic tumour spread in bone marrow. Finally, purified haematopoietic stem/progenitor cells and lymphocytes also localize to the same microdomains, indicating that this vasculature might also function in benign states to demarcate specific portals for the entry of cells into the marrow space. Specialized vascular structures therefore appear to delineate a microenvironment with unique physiology that can be exploited by circulating malignant cells.

摘要

细胞龛的组织在调节正常干细胞分化和再生中起着关键作用,然而对于支持恶性转移的微环境结构却知之甚少。利用动态体内共聚焦成像技术,我们在此表明,小鼠骨髓包含由特殊内皮细胞界定的独特解剖区域。这种脉管系统在离散、不连续的区域表达黏附分子E-选择素和趋化因子基质细胞衍生因子1(SDF-1),这些区域影响多种肿瘤细胞系的归巢。SDF-1与其受体CXCR4之间相互作用的破坏会抑制Nalm-6细胞(一种急性淋巴细胞白血病细胞系)向这些血管的归巢。进一步研究表明,循环中的白血病细胞能够在这些血管周围植入,这表明这种分子特征明显的脉管系统划定了骨髓中早期转移性肿瘤扩散的微环境。最后,纯化的造血干/祖细胞和淋巴细胞也定位于相同的微区,这表明这种脉管系统在良性状态下可能也发挥作用,划定细胞进入骨髓腔的特定入口。因此,特殊的血管结构似乎划定了一个具有独特生理学特征的微环境,循环中的恶性细胞可以利用这一微环境。

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