首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >The effects of tumor-derived platelet-derived growth factor on vascular morphology and function in vivo revealed by susceptibility MRI.
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The effects of tumor-derived platelet-derived growth factor on vascular morphology and function in vivo revealed by susceptibility MRI.

机译:敏感性MRI揭示了肿瘤来源的血小板衍生生长因子对体内血管形态和功能的影响。

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摘要

Platelet-derived growth factors (PDGF) play a major role in pericyte recruitment in tumor capillaries. Pericytes are required for proper vessel development, and contribute to tumor angiogenesis by promoting stabilization and maturation of newly formed vessels. To investigate the effects of pericyte coverage on tumor vessel morphology and function in vivo, tumors derived from B16 melanoma cells transfected with either control plasmid (B16/ctr) or plasmid encoding full-length PDGF-BB (B16/PDGF), the latter previously shown to have enhanced blood vessel pericyte coverage and an increased tumor growth rate, were assessed using histopathological methods, Hoechst 33342-based perfusion analyses, and two noninvasive susceptibility magnetic resonance imaging (MRI) methods. Susceptibility-contrast MRI, incorporating the use of ultrasmall superparamagnetic iron oxide particles, revealed a significant (p < 0.05) reduction in vessel size index (R(v)) of B16/PDGF tumors, and which was validated histologically by thepresence of significantly smaller (p < 0.001), more punctate blood vessels identified by fluorescence microscopy of the perfusion marker Hoechst 33342. Intrinsic-susceptibility MRI was used to measure the transverse MRI relaxation rate R(2)*, sensitive to changes in endogenous paramagnetic [deoxyhaemoglobin], and used to probe for vascular maturation and function. Hypercapnia (5% CO(2)/95% air) induced a negligible Delta R(2)* response in the B16/ctr and B16/PDGF tumors. In contrast, hyperoxia (5% CO(2)/95% O(2)) induced a significantly greater R(2)* reduction in the B16/PDGF tumors (p < 0.02). Together the susceptibility MRI-derived biomarkers reveal novel pericyte-dependent changes in the morphology and function of the perfused tumor vasculature in vivo.
机译:血小板衍生生长因子(PDGF)在肿瘤毛细​​血管的周细胞募集中起主要作用。周细胞对于适当的血管发育是必需的,并且通过促进新形成的血管的稳定和成熟来促进肿瘤血管生成。为了研究周细胞覆盖对体内肿瘤血管形态和功能的影响,采用对照质粒(B16 / ctr)或编码全长PDGF-BB的质粒(B16 / PDGF)转染的B16黑色素瘤细胞衍生的肿瘤使用组织病理学方法,基于Hoechst 33342的灌注分析和两种非侵入性磁敏感度磁共振成像(MRI)方法对血管内皮细胞覆盖率提高和肿瘤生长速率提高的结果进行了评估。敏感性对比MRI,结合使用超小超顺磁性氧化铁颗粒,显示出B16 / PDGF肿瘤的血管大小指数(R(v))显着(p <0.05)减小,并且组织学上通过显着较小的存在对其进行了验证(p <0.001),通过荧光标记灌注标记Hoechst 33342的荧光显微镜检出了更多的点状血管。本征磁化MRI用于测量横向MRI弛豫率R(2)*,对内源性顺磁性[deoxyhaemoglobin]的变化敏感,并用于探测血管成熟和功能。高碳酸血症(5%CO(2)/ 95%空气)在B16 / ctr和B16 / PDGF肿瘤中引起的Delta R(2)*反应微不足道。相反,高氧血症(5%CO(2)/ 95%O(2))引起B16 / PDGF肿瘤的R(2)*降低明显更多(p <0.02)。 MRI敏感性生物标志物共同揭示了体内灌注肿瘤脉管系统的形态和功能的新的依赖周细胞的变化。

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