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模拟 (64)Cu-ATSM 的组织活性曲线,用于放疗中的亚靶区勾画。

Simulation of tissue activity curves of (64)Cu-ATSM for sub-target volume delineation in radiotherapy.

机构信息

Department of Physics, University of Surrey, Guildford, UK.

出版信息

Phys Med Biol. 2010 Feb 7;55(3):681-94. doi: 10.1088/0031-9155/55/3/009. Epub 2010 Jan 13.

Abstract

There is much interest in positron emission tomography (PET) for measurements of regional tracer concentration in hypoxic tumour-bearing tissue, focusing on the need for accurate radiotherapy treatment planning. Generally, relevant data are taken over multiple time frames in the form of tissue activity curves (TACs), thus providing an indication of vasculature structure and geometry. This is a potential key in providing information on cellular perfusion and limited diffusion. A number of theoretical studies have attempted to describe tracer uptake in tissue cells in an effort to understand such complicated behaviour of cellular uptake and the mechanism of washout. More recently, a novel computerized reaction diffusion equation method was developed by Kelly and Brady (2006 A model to simulate tumour oxygenation and dynamic [18F]-FMISO PET data Phys. Med. Biol. 51 5859-73), where they managed to simulate the realistic dynamic TACs of (18)F-FMISO. The model was developed over a multi-step process. Here we present a refinement to the work of Kelly and Brady, such that the model allows simulation of a realistic tissue activity curve (TAC) of any hypoxia selective PET tracer, in a single step process. In this work we show particular interest in simulating the TAC of perhaps the most promising hypoxia selective tracer, (64)Cu-ATSM. In addition, we demonstrate its potential role in tumour sub-volume delineation for radiotherapy treatment planning. Simulation results have demonstrated the significant high contrast of imaging using ATSM, with a tumour to blood ratio ranging from 2.24 to 4.1.

摘要

正电子发射断层扫描(PET)在测量缺氧肿瘤组织中的示踪剂浓度方面引起了广泛关注,主要集中在需要进行准确的放射治疗计划方面。通常,相关数据以组织活性曲线(TAC)的形式在多个时间框架内获取,从而提供了对脉管结构和几何形状的指示。这是提供有关细胞灌注和有限扩散信息的潜在关键。许多理论研究都试图描述组织细胞中示踪剂的摄取,以了解细胞摄取的这种复杂行为和洗脱机制。最近,Kelly 和 Brady(2006 年)开发了一种新的计算机化反应扩散方程方法,用于模拟肿瘤氧合和动态[18F]-FMISO PET 数据。Phys。Med。Biol。51 5859-73),他们成功地模拟了(18)F-FMISO 的真实动态 TAC。该模型是通过多步过程开发的。在这里,我们对 Kelly 和 Brady 的工作进行了改进,使得该模型可以在单个步骤中模拟任何缺氧选择性 PET 示踪剂的真实组织活性曲线(TAC)。在这项工作中,我们特别感兴趣的是模拟(64)Cu-ATSM 这种最有前途的缺氧选择性示踪剂的 TAC。此外,我们还展示了它在肿瘤亚体积描绘中的潜在作用,以用于放射治疗计划。模拟结果表明,使用 ATSM 进行成像具有很高的对比度,肿瘤与血液的比值范围为 2.24 至 4.1。

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