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锕-225标记的HER2/neu靶向抗体的早期正常组织效应及骨髓相对生物效应

Early Normal Tissue Effects and Bone Marrow Relative Biological Effectiveness for an Actinium 225-Labeled HER2/neu-Targeting Antibody.

作者信息

Liatsou Ioanna, Josefsson Anders, Yu Jing, Li Zhi, Davis Kaori, Brayton Cory, Wang Hao, Hobbs Robert F, Sgouros George

机构信息

Russell H. Morgan Department of Radiology and Radiological Science, Johns Hopkins University School of Medicine, Baltimore, Maryland.

Department of Radiology, University of Pittsburgh, Pittsburgh, Pennsylvania.

出版信息

Int J Radiat Oncol Biol Phys. 2023 Nov 15;117(4):1028-1037. doi: 10.1016/j.ijrobp.2023.06.003. Epub 2023 Jun 17.

Abstract

PURPOSE

In this study we determined the dose-independent relative biological effectiveness (RBE2) of bone marrow for an anti-HER2/neu antibody labeled with the alpha-particle emitter actinium 225 (Ac). Hematologic toxicity is often a consequence of radiopharmaceutical therapy (RPT) administration, and dosimetric guidance to the bone marrow is required to limit toxicity.

METHODS AND MATERIALS

Female neu/N transgenic mice (MMTV-neu) were intravenously injected with 0 to 16.65 kBq of the alpha-particle emitter labeled antibody, Ac-DOTA-7.16.4, and euthanized at 1 to 9 days after treatment. Complete blood counts were performed. Femurs and tibias were collected, and bone marrow was isolated from 1 femur and tibia and counted for radioactivity. Contralateral intact femurs were fixed, decalcified, and assessed by histology. Marrow cellularity was the biologic endpoint selected for RBE2 determination. For the reference radiation, both femurs of the mice were photon irradiated with 0 to 5 Gy using a small animal radiation research platform.

RESULTS

Response as measured by cellularity for the alpha-particle emitter RPT (αRPT) RPT and the external beam radiation therapy were linear and linear quadratic, respectively, as a function of absorbed dose. The resulting dose-independent RBE2 for bone marrow was 6.

CONCLUSIONS

As αRPT gains prominence, preclinical studies evaluating RBE in vivo will be important in relating to human experience with beta-particle emitter RPT. Such normal tissue RBE evaluations will help mitigate unexpected toxicity in αRPT.

摘要

目的

在本研究中,我们测定了用α粒子发射体锕225(Ac)标记的抗HER2/neu抗体对骨髓的剂量无关相对生物学效应(RBE2)。血液学毒性通常是放射性药物治疗(RPT)给药的结果,因此需要对骨髓进行剂量测定指导以限制毒性。

方法和材料

给雌性neu/N转基因小鼠(MMTV-neu)静脉注射0至16.65 kBq的α粒子发射体标记抗体Ac-DOTA-7.16.4,并在治疗后1至9天实施安乐死。进行全血细胞计数。收集股骨和胫骨,从1根股骨和胫骨中分离出骨髓并计数放射性。对侧完整股骨进行固定、脱钙并通过组织学评估。骨髓细胞密度是选择用于测定RBE2的生物学终点。对于参考辐射,使用小动物辐射研究平台对小鼠的双侧股骨进行0至5 Gy的光子照射。

结果

通过细胞密度测量的α粒子发射体RPT(αRPT)和外照射放疗的反应分别是吸收剂量的线性函数和线性二次函数。由此得出的骨髓剂量无关RBE2为6。

结论

随着αRPT的日益突出,评估体内RBE的临床前研究对于关联人类使用β粒子发射体RPT的经验将很重要。此类正常组织RBE评估将有助于减轻αRPT中意外的毒性。

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