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骨骼和骨髓剂量模型的发展与现状。

Evolution and status of bone and marrow dose models.

作者信息

Stabin M G, Eckerman K F, Bolch W E, Bouchet L G, Patton P W

机构信息

Department of Radiology and Radiological Sciences Vanderbilt University, Nashville, TN 37232, USA.

出版信息

Cancer Biother Radiopharm. 2002 Aug;17(4):427-33. doi: 10.1089/108497802760363213.

Abstract

Investigations at the University of Leeds under the direction of F.W. Spiers in the early 1960s through the late 1970s established the first comprehensive assessment of marrow dose conversion factors (DCFs) for beta-emitting radionuclides within the volume or on the surface of trabecular bone. These DCFs were subsequently used in deriving radionuclide S values for skeletal tissues published in MIRD Pamphlet No. 11. Eckerman re-evaluated this work and extended the methods of Spiers to radionuclides within the marrow to provide DCFs for fifteen skeletal regions in computational models representing individuals of six different ages. These results were used in the MIRDOSE3 software. Bouchet et al. used updated information on regional bone and marrow masses, as well as 3D electron transport techniques, to derive radionuclide S values in skeletal regions of the adult. Although these two efforts are similar in most regards, the models differ in three respects in: (1) the definition of the red marrow region, (2) the definition of a surface source of activity, and (3) the assumption applied in transporting electrons through the trabecular endosteum. In this study, a review of chord-based skeletal models is given, followed by a description of the differences in the Eckerman and Bouchet et al. transport models. Finally, new data from NMR microscopy and radiation transport in trabecular bone is applied to address item (1) above. Dose conversion factors from MIRD 11, the Eckerman model, the Bouchet et al. model, and a revised model are compared for several radionuclides important to internal emitter therapy.

摘要

20世纪60年代初至70年代末,在F.W. 斯皮尔斯的指导下,利兹大学开展了多项研究,首次对小梁骨体积内或表面发射β射线的放射性核素的骨髓剂量转换因子(DCF)进行了全面评估。这些DCF随后被用于推导《MIRD手册第11号》中公布的骨骼组织的放射性核素S值。埃克曼重新评估了这项工作,并将斯皮尔斯的方法扩展到骨髓内的放射性核素,以在代表六个不同年龄个体的计算模型中提供15个骨骼区域的DCF。这些结果被用于MIRDOSE3软件。布歇等人使用了关于区域骨和骨髓质量的最新信息以及三维电子传输技术,来推导成年人骨骼区域的放射性核素S值。尽管这两项工作在大多数方面相似,但这两个模型在三个方面存在差异:(1)红骨髓区域的定义;(2)表面活性源的定义;(3)在电子穿过小梁骨内膜时应用的假设。在本研究中,首先对基于弦的骨骼模型进行了综述,随后描述了埃克曼和布歇等人的传输模型的差异。最后,应用来自核磁共振显微镜和小梁骨中辐射传输的数据来解决上述第(1)项问题。对几种对体内发射体治疗重要的放射性核素,比较了《MIRD第11号》、埃克曼模型、布歇等人的模型以及一个修订模型的剂量转换因子。

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