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使用“组织分离”制剂对肿瘤血流进行表征。

Characterisation of tumour blood flow using a 'tissue-isolated' preparation.

作者信息

Tozer G M, Shaffi K M, Prise V E, Cunningham V J

机构信息

CRC Gray Laboratory, Mount Vernon Hospital, Northwood, Middlesex, UK.

出版信息

Br J Cancer. 1994 Dec;70(6):1040-6. doi: 10.1038/bjc.1994.445.

Abstract

Tumour blood flow was characterised in a 'tissue-isolated' rat tumour model, in which the vascular supply is derived from a single artery and vein. Tumours were perfused in situ and blood flow was calculated from simultaneous measurement of (1) venous outflow from the tumour and (2) uptake into the tumour of radiolabelled iodo-antipyrine (IAP). Comparison of results from the two measurements enabled assessment of the amount of blood 'shunted' through the tumours with minimal exchange between blood and tissue. Kinetics of IAP uptake were also used to determine the apparent volume of distribution (VDapp) for the tracer and the equilibrium tissue-blood partition coefficient (lambda). lambda was also measured by in vitro techniques and checks were made for binding and metabolism of IAP using high-pressure liquid chromatography. VDapp and lambda were used to calculate the perfused fraction (alpha) of the tumours. Tumour blood flow, as measured by IAP (TBFIAP), was 94.8 +/- 4.4% of the blood flow as measured by venous outflow, indicating only a small amount of non-exchanging flow. This level of shunting is lower than some previous estimates in which the percentage tumour entrapment of microspheres was used. The unperfused fraction ranged from 0 to 20% of the tumour volume in the majority of tumours. This could be due to tumour necrosis and/or acutely ischaemic tumour regions. For practical purposes, measurement of the total venous outflow of tumours is a reasonable measure of exchangeable tumour blood flow in this system and allows for on-line measurements. Tracer methods can be used to obtain additional information on the distribution of blood flow within tumours.

摘要

在一种“组织隔离”的大鼠肿瘤模型中对肿瘤血流进行了表征,该模型的血管供应源自单一动脉和静脉。对肿瘤进行原位灌注,并通过同时测量(1)肿瘤的静脉流出量和(2)放射性标记的碘安替比林(IAP)进入肿瘤的摄取量来计算血流量。对这两种测量结果的比较能够评估通过肿瘤“分流”的血量,同时血液与组织之间的交换最少。IAP摄取动力学还用于确定示踪剂的表观分布容积(VDapp)和平衡组织 - 血液分配系数(lambda)。lambda也通过体外技术进行测量,并使用高压液相色谱法检查IAP的结合和代谢情况。VDapp和lambda用于计算肿瘤的灌注分数(alpha)。通过IAP测量的肿瘤血流量(TBFIAP)是通过静脉流出量测量的血流量的94.8±4.4%,表明只有少量的非交换血流。这种分流水平低于一些先前的估计值,先前的估计使用微球的肿瘤截留百分比。在大多数肿瘤中,未灌注部分占肿瘤体积的0%至20%。这可能是由于肿瘤坏死和/或急性缺血性肿瘤区域所致。出于实际目的,测量肿瘤的总静脉流出量是该系统中可交换肿瘤血流量的合理测量方法,并允许进行在线测量。示踪剂方法可用于获取有关肿瘤内血流分布的更多信息。

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