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Dynamics of microvascular remodelling during tumor growth in bone.

机译:骨肿瘤生长过程中微血管重塑的动力学。

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Microcirculatory properties of tumors have been shown to play a pivotal role in tumor progression and inefficacy of therapies. Although the influence of the microenvironment on angiogenesis has been intensively investigated in soft tissue tumors, little is known about the microvascular properties in bone metastasis. To determine the impact of the bone microenvironment on tumor growth and microcirculation we performed intravital microscopy using the "femur window" after implantation of red-fluorescent-protein-transduced breast cancer cells into the femura of severe-combined-immunodeficient mice. Tumor size, functional vascular density, vessel diameter, and vessel distribution were quantified over 14 days. Tumor growth and microcirculation could be quantified at a high spatial resolution. Tumor progression was associated with a rapid remodeling process of the microcirculation within the tumor and the surrounding tissue. Although the total functional vascular density remained unaltered, we found a significant loss in small vessels and a concomitant increase in vascular diameter. The presented study demonstrates for the first time dynamics of morphological microcirculatory alterations of tumor growth in bone. The observed changes in tumor vascularization exhibit strong similarities to soft tissue tumors; however, the dynamics of vascular alterations are more rapid in the bone microenvironment.
机译:肿瘤的微循环特性已显示在肿瘤进展和治疗无效中起关键作用。尽管已经在软组织肿瘤中深入研究了微环境对血管生成的影响,但对于骨转移中的微血管特性知之甚少。为了确定骨微环境对肿瘤生长和微循环的影响,我们在将红色荧光蛋白转导的乳腺癌细胞植入严重合并免疫缺陷小鼠的胎儿后,使用“股骨窗”进行了活体显微镜检查。在14天内定量肿瘤大小,功能性血管密度,血管直径和血管分布。肿瘤的生长和微循环可以在高空间分辨率下进行量化。肿瘤进展与肿瘤和周围组织内微循环的快速重塑过程有关。尽管总的功能性血管密度保持不变,但我们发现小血管的明显丧失和随之而来的血管直径的增加。提出的研究首次证明了骨肿瘤生长的形态学微循环改变的动力学。观察到的肿瘤血管形成的变化与软组织肿瘤有很强的相似性。然而,在骨骼微环境中,血管改变的动力学更为迅速。

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