抗 MUC1-C 抗体偶联纳米颗粒增强分次放射治疗的疗效。

Anti-MUC1-C Antibody-Conjugated Nanoparticles Potentiate the Efficacy of Fractionated Radiation Therapy.

机构信息

Dana-Farber Cancer Institute, Department of Medical Oncology, Harvard Medical School, Boston, Massachusetts; Centre Paul Strauss, Strasbourg, France.

Dana-Farber Cancer Institute, Department of Medical Oncology, Harvard Medical School, Boston, Massachusetts.

出版信息

Int J Radiat Oncol Biol Phys. 2020 Dec 1;108(5):1380-1389. doi: 10.1016/j.ijrobp.2020.06.069. Epub 2020 Jul 4.

DOI:10.1016/j.ijrobp.2020.06.069

PMID:32634545

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7680267/

Abstract

PURPOSE

Heavy-metal chelators and inorganic nanoparticles (NPs) have been examined as potential radioenhancers to increase the efficacy of external beam radiation therapy for various cancers. Most of these agents have, unfortunately, displayed relatively poor pharmacokinetic properties, which limit the percentage of injected dose (%ID/g) that localizes to tumors and which shorten the window for effective radiation enhancement due to rapid tumor washout.

METHODS AND MATERIALS

To address these challenges, we sought to conjugate gadolinium-based ultrasmall (<5 nm) NPs to an antibody directed against the oncogenic MUC1-C subunit that is overexpressed on the surface of many different human cancer types. The binding of the anti-MUC1-C antibody 3D1 to MUC1-C on the surface of a cancer cell is associated with its internalization and, thereby, to effective intracellular delivery of the antibody-associated payload, promoting its effective tumor retention. As such, we examined whether systemically administered anti-MUC1-C antibody-conjugated, gadolinium-based NPs (anti-MUC1-C/NPs) could accumulate within cell-line xenograft models of MUC1-C-expressing (H460) lung and (E0771) breast cancers to improve the efficacy of radiation therapy (XRT).

RESULTS

The %ID/g of anti-MUC1-C/NPs that accumulated within tumors was found to be similar to that of their unconjugated counterparts (6.6 ± 1.4 vs 5.9 ± 1.7 %ID/g, respectively). Importantly, the anti-MUC1-C/NPs demonstrated prolonged retention in in vivo tumor microenvironments; as a result, the radiation boost was maintained during the course of fractionated therapy (3 × 5.2 Gy). We found that by administering anti-MUC1-C/NPs with XRT, it was possible to significantly augment tumor growth inhibition and to prolong the animals' overall survival (46.2 ± 3.1 days) compared with the administration of control NPs with XRT (31.1 ± 2.4 days) or with XRT alone (27.3 ± 1.6 days; P < .01, log-rank).

CONCLUSIONS

These findings suggest that anti-MUC1-C/NPs could be used to enhance the effectiveness of radiation therapy and potentially to improve clinical outcomes.

摘要

目的

重金属螯合剂和无机纳米粒子（NPs）已被研究为潜在的放射增敏剂，以提高各种癌症的外束放射治疗的疗效。不幸的是，这些药物中的大多数表现出相对较差的药代动力学特性，这限制了注射剂量的百分比（%ID/g）定位到肿瘤，并由于肿瘤快速清除而缩短了有效的放射增强窗口。

方法和材料

为了解决这些挑战，我们试图将基于镧系元素的超小（<5nm）NPs 与针对在许多不同人类癌症类型表面过度表达的致癌 MUC1-C 亚基的抗体偶联。针对癌细胞表面 MUC1-C 的抗 MUC1-C 抗体 3D1 的结合与它的内化有关，从而促进了抗体相关有效载荷的有效细胞内递呈，促进其有效的肿瘤保留。因此，我们研究了全身性给予抗 MUC1-C 抗体偶联的基于镧系元素的 NPs（抗 MUC1-C/NPs）是否可以在表达 MUC1-C 的细胞系异种移植模型（H460）肺癌和（E0771）乳腺癌中积累，以提高放射治疗（XRT）的疗效。

结果

发现抗 MUC1-C/NPs 在肿瘤中积累的%ID/g 与未偶联的类似物相似（分别为 6.6±1.4%ID/g 和 5.9±1.7%ID/g）。重要的是，抗 MUC1-C/NPs 在体内肿瘤微环境中表现出延长的保留；结果，在分次治疗（3×5.2Gy）过程中维持了放射增敏作用。我们发现，通过给予 XRT 联合抗 MUC1-C/NPs，可以显著抑制肿瘤生长，并延长动物的总生存期（46.2±3.1 天），与给予 XRT 联合对照 NPs（31.1±2.4 天）或单独给予 XRT（27.3±1.6 天）相比（P<.01，对数秩）。