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Skeletal dosimetry models for alpha-particles for use in molecular radiotherapy.

机译:分子放射疗法中使用的α粒子的骨骼剂量模型。

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Molecular radiotherapy is a cancer treatment methodology whereby a radionuclide is combined with a biologically active molecule to preferentially target cancer cells. Alpha-particle emitting radionuclides show significant potential for use in molecular radiotherapy due to the short range of the alpha-particles in tissue and their high rates of energy deposition. Current radiation dosimetry models used to assess alpha emitter dose in the skeleton were developed originally for occupational applications. In medical dosimetry, individual variability in uptake, translocation and other biological factors can result in poor correlation of clinical outcome with marrow dose estimates determined using existing skeletal models. Methods presented in this work were developed in response to the need for dosimetry models which account for these biological and patient-specific factors.; Dosimetry models are presented for trabecular bone alpha particle dosimetry as well as a model for cortical bone dosimetry. These radiation transport models are the 3D chord-based infinite spongiosa transport model (3D-CBIST) and the chord-based infinite cortical transport model (CBICT), respectively. Absorbed fraction data for several skeletal tissues for several subjects are presented. Each modeling strategy accounts for biological parameters, such as bone marrow cellularity, not previously incorporated into alpha-particle skeletal dosimetry models used in radiation protection. Using these data a study investigating the variability in alpha-particle absorbed fractions in the human skeleton is also presented. Data is also offered relating skeletal tissue masses in individual bone sites for a range of ages. These data are necessary for dose calculations and have previously only been available as whole body tissue masses. A revised 3D-CBIST model is also presented which allows for changes in endosteum thickness to account for revised target cell location of tissues involved in the radiological induction of bone cancer. In addition, new data are presented on the location of bone-marrow stem cells within the marrow cavities of trabecular bone of the pelvis. All results presented in this work may be applied to occupational exposures, but their greatest utility lies in dose assessments for alpha-emitters in molecular radiotherapy.
机译:分子放射疗法是一种癌症治疗方法,其中放射性核素与生物活性分子结合以优先靶向癌细胞。由于组织中α粒子的射程短且能量沉积率高,发射α粒子的放射性核素显示出在分子放射疗法中使用的巨大潜力。用于评估骨骼中α发射体剂量的当前辐射剂量学模型最初是为职业应用开发的。在医学剂量测定中,个体摄取,易位和其他生物学因素的变异性可能导致临床结果与使用现有骨骼模型确定的骨髓剂量估计之间的相关性较差。这项工作中提出的方法是根据对这些生物学和患者特定因素的剂量学模型的需求而开发的。提出了用于小梁骨α粒子剂量测定的剂量测定模型以及用于皮质骨剂量测定的模型。这些辐射传输模型分别是基于3D和弦的无限海绵运输模型(3D-CBIST)和基于和弦的无限皮质运输模型(CBICT)。给出了几个受试者的几个骨骼组织的吸收分数数据。每种建模策略都考虑到了生物学参数,例如骨髓细胞数量,这些参数先前并未纳入辐射防护中使用的α粒子骨架剂量模型中。利用这些数据,还进行了一项研究,研究了人类骨骼中被α粒子吸收的部分的变异性。还提供了有关各个年龄段各个骨骼部位的骨骼组织质量的数据。这些数据对于剂量计算是必需的,并且以前仅作为全身组织块可用。还提出了一种经过修订的3D-CBIST模型,该模型允许改变骨内膜厚度,以解释参与放射线诱导骨癌的组织的目标细胞的修订位置。此外,还提供了有关骨干小梁骨骨髓腔内骨髓干细胞位置的新数据。这项工作中提出的所有结果都可能适用于职业暴露,但是它们最大的用途在于分子放射疗法中α发射体的剂量评估。

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