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使用新型抗氧化型巨噬细胞移动抑制因子/人血清球蛋白双特异性抗体ON105进行的预靶向放射免疫疗法在小鼠癌症模型中导致显著的肿瘤消退。

Pretargeted radioimmunotherapy with the novel anti-oxMIF/HSG bispecific antibody ON105 results in significant tumor regression in murine models of cancer.

作者信息

Puchol Tarazona Alejandro A, Schinagl Alexander, Mirkina Irina, Rossmueller Gregor, Kerschbaumer Randolf J, Bachmann Friedmund, Thiele Michael

机构信息

OncoOne Research & Development GmbH, Vienna, Austria.

OncoOne Research & Development GmbH, Austria.

出版信息

Mol Cancer Ther. 2024 Jun 5. doi: 10.1158/1535-7163.MCT-24-0083.

DOI:10.1158/1535-7163.MCT-24-0083
PMID:38833646
Abstract

Radioimmunotherapy (RIT) uses mAbs to deliver radionuclides to cancer cells or the tumor microenvironment and has shown promise in treating localized and diffuse tumors. While RIT agents have gained FDA/EMA approval for certain hematological malignancies, effectiveness of RIT in treating solid tumors remains limited. Here we present PreTarg-it®, a novel approach for pretargeted radioimmunotherapy, providing optimized delivery of payloads in a two-step regimen. The effectiveness of PreTarg-it® is demonstrated by a powerful combination of ON105, a novel bispecific antibody against both oxMIF and the histamine-succinyl-glycyl (HSG) hapten, as the first component and the radioactively labeled DOTA-di-HSG peptide as the second component in murine models of cancer. Mice bearing either subcutaneous mouse colorectal CT26 or human pancreatic CFPAC-1 tumors received an intravenous injection of ON105. After ON105 had accumulated in the tumor and cleared from circulation to approximately 1-3% of its peak concentration, 177Lu-DOTA-di-HSG peptide was administered. A single PreTarg-it® treatment cycle resulted in tumor regression when mice bearing CT26 tumors were given the highest treatment dose with a pretargeting delay of three days. Administered with a 5-day interval, the highest dose arrested tumor growth in both CT26 syngrafts and CFPAC-1 xenografts. In all cases, the highest treatment dose resulted in 100% survival at the study endpoint whereas the control cohorts showed 0% and 60% survival in the CT26 and CFPAC-1 models, respectively. Therefore, PreTarg-it® holds potential as a novel and potent therapy for patients with hard-to-treat solid tumors such as pancreatic cancer, as well as those with late-stage malignancies.

摘要

放射免疫疗法(RIT)利用单克隆抗体将放射性核素递送至癌细胞或肿瘤微环境,在治疗局部和弥漫性肿瘤方面显示出前景。虽然RIT药物已获得美国食品药品监督管理局(FDA)/欧洲药品管理局(EMA)对某些血液系统恶性肿瘤的批准,但RIT在治疗实体瘤方面的有效性仍然有限。在此,我们介绍PreTarg-it®,一种用于预靶向放射免疫疗法的新方法,在两步方案中实现了有效载荷的优化递送。PreTarg-it®的有效性通过一种强大的组合得以证明,即在癌症小鼠模型中,第一步使用新型双特异性抗体ON105(一种针对氧化巨噬细胞移动抑制因子(oxMIF)和组胺 - 琥珀酰 - 甘氨酰(HSG)半抗原的双特异性抗体),第二步使用放射性标记的DOTA - 二 - HSG肽。携带皮下小鼠结肠直肠癌CT26或人胰腺CFPAC - 1肿瘤的小鼠接受静脉注射ON105。在ON105在肿瘤中积累并从循环中清除至其峰值浓度的约1 - 3%后,给予177Lu - DOTA - 二 - HSG肽。当携带CT26肿瘤的小鼠接受最高治疗剂量且预靶向延迟三天时,单个PreTarg-it®治疗周期导致肿瘤消退。以5天间隔给药时,最高剂量使CT26同基因移植瘤和CFPAC - 1异种移植瘤的肿瘤生长停滞。在所有情况下,最高治疗剂量在研究终点时导致100%存活,而对照队列在CT26和CFPAC - 1模型中的存活率分别为0%和60%。因此,PreTarg-it®作为一种针对胰腺癌等难以治疗的实体瘤患者以及晚期恶性肿瘤患者的新型有效疗法具有潜力。

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