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肿瘤血管对血管紧张素 II 的不同反应:肿瘤体积对灌注和氧合的依赖性影响。

Disparate responses of tumour vessels to angiotensin II: tumour volume-dependent effects on perfusion and oxygenation.

作者信息

Thews O, Kelleher D K, Vaupel P

机构信息

Institute of Physiology and Pathophysiology, University of Mainz, Germany.

出版信息

Br J Cancer. 2000 Jul;83(2):225-31. doi: 10.1054/bjoc.2000.1229.

Abstract

Perfusion and oxygenation of experimental tumours were studied during angiotensin II (AT II) administration whereby the rate of the continuous AT II infusion was chosen to increase the mean arterial blood pressure (MABP) by 50-70 mmHg. In subcutaneous DS-sarcomas the red blood cell (RBC) flux was assessed using the laser Doppler technique and the mean tumour oxygen partial pressure (pO2) was measured polarographically using O2-sensitive catheter and needle electrodes. Changes in RBC flux with increasing MABP depended mainly on tumour size. In small tumours, RBC flux decreased with rising MABP whereas in larger tumours RBC flux increased parallel to the MABP. As a result of these volume-dependent effects on tumour blood flow, the impact of AT II on tumour pO2 was also mainly tumour volume-related. In small tumours oxygenation decreased with increasing MABP during AT II infusion, whereas in large tumours a positive relationship between blood pressure and O2 status was found. This disparate behaviour might be the result of the co-existence of two functionally distinct populations of tumour vessels. In small tumours, perfusion decreases presumably due to vasoconstriction of pre-existing host vessels feeding the tumour. In larger malignancies, newly formed tumour vessels predominate and seem not to have this vasoresponsive capability (lack of smooth muscle cells and/or AT receptors), resulting in an improvement of perfusion which is not tumour-related per se, but is due to the increased perfusion pressure.

摘要

在给予血管紧张素II(AT II)期间,对实验性肿瘤的灌注和氧合进行了研究,其中选择持续输注AT II的速率,以使平均动脉血压(MABP)升高50 - 70 mmHg。在皮下DS - 肉瘤中,使用激光多普勒技术评估红细胞(RBC)通量,并使用对氧敏感的导管和针电极通过极谱法测量肿瘤平均氧分压(pO2)。随着MABP升高,RBC通量的变化主要取决于肿瘤大小。在小肿瘤中,RBC通量随MABP升高而降低,而在大肿瘤中,RBC通量与MABP平行增加。由于这些对肿瘤血流的体积依赖性影响,AT II对肿瘤pO2的影响也主要与肿瘤体积相关。在小肿瘤中,在输注AT II期间氧合随着MABP升高而降低,而在大肿瘤中,发现血压与氧状态呈正相关。这种不同的行为可能是两种功能不同的肿瘤血管群体共存的结果。在小肿瘤中,灌注减少可能是由于为肿瘤供血的既有宿主血管收缩所致。在较大的恶性肿瘤中,新形成的肿瘤血管占主导,并且似乎没有这种血管反应能力(缺乏平滑肌细胞和/或AT受体),导致灌注改善,这本身与肿瘤无关,而是由于灌注压力增加所致。

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