Laboratory of Nano- and Translational Medicine, Carolina Center for Cancer Nanotechnology Excellence, Carolina Institute of Nanomedicine, University of North Carolina at Chapel Hill , Chapel Hill, North Carolina 27599, United States.
Department of Radiation Oncology, Lineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill , Chapel Hill, North Carolina 27599, United States.
ACS Nano. 2018 Feb 27;12(2):1544-1563. doi: 10.1021/acsnano.7b08122. Epub 2018 Jan 26.
Non-Hodgkin lymphoma (NHL) is one of the most common types of hematologic malignancies. Pretargeted radioimmunotherapy (PRIT), the sequential administration of a bispecific antibody-based primary tumor-targeting component followed by a radionucleotide-labeled treatment effector, has been developed to improve the treatment efficacy and to reduce the side effects of conventional RIT. Despite the preclinical success of PRIT, clinical trials revealed that the immunogenicity of the bispecific antibody as well as the presence of competing endogenous effector molecules often compromised the treatment. One strategy to improve PRIT is to utilize bio-orthogonal ligation reactions to minimize immunogenicity and improve targeting. Herein, we report a translatable pretargeted nanoradioimmunotherapy strategy for the treatment of NHL. This pretargeting system is composed of a dibenzylcyclooctyne (DBCO)-functionalized anti-CD20 antibody (α-CD20) tumor-targeting component and an azide- and yttrium-90-(Y) dual-functionalized dendrimer. The physicochemical properties of both pretargeting components have been extensively studied. We demonstrated that an optimized dual-functionalized dendrimer can undergo rapid strain-promoted azide-alkyne cycloaddition with the DBCO-functionalized α-CD20 at the physiological conditions. The treatment effector in our pretargeting system can not only selectively deliver radionucleotides to the target tumor cells but also increase the complement-dependent cytotoxicity of α-CD20 and thus enhance the antitumor effects, as justified by comprehensive in vitro and in vivo studies in mouse NHL xenograft and disseminated models.
非霍奇金淋巴瘤(NHL)是最常见的血液恶性肿瘤之一。前靶向放射免疫疗法(PRIT)是一种将基于双特异性抗体的原发性肿瘤靶向成分与放射性核素标记的治疗效应物顺序给予的方法,旨在提高治疗效果并降低常规 RIT 的副作用。尽管 PRIT 的临床前研究取得了成功,但临床试验表明,双特异性抗体的免疫原性以及内源性竞争效应分子的存在常常会影响治疗效果。提高 PRIT 的一种策略是利用生物正交连接反应来最小化免疫原性并提高靶向性。在此,我们报告了一种用于 NHL 治疗的可转化的前靶向纳米放射免疫疗法策略。该前靶向系统由二苄基环辛炔(DBCO)功能化抗 CD20 抗体(α-CD20)肿瘤靶向成分和叠氮化物和钇-90(Y)双功能化树枝状大分子组成。这两种前靶向成分的理化性质都得到了广泛的研究。我们证明,优化后的双功能化树枝状大分子可以在生理条件下与 DBCO 功能化的 α-CD20 快速进行应变促进的叠氮化物-炔烃环加成反应。我们前靶向系统中的治疗效应物不仅可以选择性地将放射性核素递送到靶肿瘤细胞,还可以增加 α-CD20 的补体依赖性细胞毒性,从而增强抗肿瘤作用,这在小鼠 NHL 异种移植和播散模型的综合体外和体内研究中得到了证实。