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基于PHITS并结合微剂量动力学模型的靶向α治疗个体剂量测定系统。

Individual dosimetry system for targeted alpha therapy based on PHITS coupled with microdosimetric kinetic model.

作者信息

Sato Tatsuhiko, Furuta Takuya, Liu Yuwei, Naka Sadahiro, Nagamori Shushi, Kanai Yoshikatsu, Watabe Tadashi

机构信息

Nuclear Science and Engineering Center, Japan Atomic Energy Agency, Shirakata 2-4, Tokai, Ibaraki, 319-1195, Japan.

Research Center for Nuclear Physics, Osaka University, Suita, Japan.

出版信息

EJNMMI Phys. 2021 Jan 12;8(1):4. doi: 10.1186/s40658-020-00350-7.

Abstract

BACKGROUND

An individual dosimetry system is essential for the evaluation of precise doses in nuclear medicine. The purpose of this study was to develop a system for calculating not only absorbed doses but also EQDX(α/β) from the PET-CT images of patients for targeted alpha therapy (TAT), considering the dose dependence of the relative biological effectiveness, the dose-rate effect, and the dose heterogeneity.

METHODS

A general-purpose Monte Carlo particle transport code PHITS was employed as the dose calculation engine in the system, while the microdosimetric kinetic model was used for converting the absorbed dose to EQDX(α/β). PHITS input files for describing the geometry and source distribution of a patient are automatically created from PET-CT images, using newly developed modules of the radiotherapy package based on PHITS (RT-PHITS). We examined the performance of the system by calculating several organ doses using the PET-CT images of four healthy volunteers after injecting F-NKO-035.

RESULTS

The deposition energy map obtained from our system seems to be a blurred image of the corresponding PET data because annihilation γ-rays deposit their energies rather far from the source location. The calculated organ doses agree with the corresponding data obtained from OLINDA 2.0 within 20%, indicating the reliability of our developed system. Test calculations by replacing the labeled radionuclide from F to At suggest that large dose heterogeneity in a target volume is expected in TAT, resulting in a significant decrease of EQDX(α/β) for higher-activity injection.

CONCLUSIONS

As an extension of RT-PHITS, an individual dosimetry system for nuclear medicine was developed based on PHITS coupled with the microdosimetric kinetic model. It enables us to predict the therapeutic and side effects of TAT based on the clinical data largely available from conventional external radiotherapy.

摘要

背景

个体剂量测定系统对于核医学中精确剂量的评估至关重要。本研究的目的是开发一种系统,该系统不仅能根据靶向α治疗(TAT)患者的PET-CT图像计算吸收剂量,还能计算EQDX(α/β),同时考虑相对生物有效性的剂量依赖性、剂量率效应和剂量异质性。

方法

该系统采用通用蒙特卡罗粒子输运代码PHITS作为剂量计算引擎,同时使用微剂量动力学模型将吸收剂量转换为EQDX(α/β)。描述患者几何形状和源分布的PHITS输入文件使用基于PHITS的放射治疗软件包(RT-PHITS)的新开发模块从PET-CT图像自动创建。我们通过使用注射F-NKO-035后四名健康志愿者的PET-CT图像计算多个器官剂量来检验该系统的性能。

结果

从我们的系统获得的沉积能量图似乎是相应PET数据的模糊图像,因为湮灭γ射线在离源位置相当远的地方沉积能量。计算得到的器官剂量与从OLINDA 2.0获得的相应数据在20%以内相符,表明我们开发的系统具有可靠性。通过将标记的放射性核素从F替换为At进行的测试计算表明,在TAT中靶体积内预期存在较大的剂量异质性,导致高活度注射时EQDX(α/β)显著降低。

结论

作为RT-PHITS的扩展,基于PHITS并结合微剂量动力学模型开发了一种用于核医学的个体剂量测定系统。它使我们能够基于传统外照射放疗中大量可得的临床数据预测TAT的治疗效果和副作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7444/7801536/54674476f62f/40658_2020_350_Fig1_HTML.jpg

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