PSMA 靶向锕-225 缀合物(225Ac-Macropa-Pelgifatamab)的临床前疗效:用于前列腺癌的靶向 α 治疗。
Preclinical Efficacy of a PSMA-Targeted Actinium-225 Conjugate (225Ac-Macropa-Pelgifatamab): A Targeted Alpha Therapy for Prostate Cancer.
机构信息
Bayer AG, Berlin, Germany.
Bayer AS, Oslo, Norway.
出版信息
Clin Cancer Res. 2024 Jun 3;30(11):2531-2544. doi: 10.1158/1078-0432.CCR-23-3746.
PURPOSE
Initially, prostate cancer responds to hormone therapy, but eventually resistance develops. Beta emitter-based prostate-specific membrane antigen (PSMA)-targeted radionuclide therapy is approved for the treatment of metastatic castration-resistant prostate cancer. Here we introduce a targeted alpha therapy (TAT) consisting of the PSMA antibody pelgifatamab covalently linked to a macropa chelator and labeled with actinium-225 and compare its efficacy and tolerability with other TATs.
EXPERIMENTAL DESIGN
The in vitro characteristics and in vivo biodistribution, antitumor efficacy, and tolerability of 225Ac-macropa-pelgifatamab (225Ac-pelgi) and other TATs were investigated in cell line- and patient-derived prostate cancer xenograft models. The antitumor efficacy of 225Ac-pelgi was also investigated in combination with the androgen receptor inhibitor darolutamide.
RESULTS
Actinium-225-labeling of 225Ac-pelgi was efficient already at room temperature. Potent in vitro cytotoxicity was seen in PSMA-expressing (LNCaP, MDA-PCa-2b, and C4-2) but not in PSMA-negative (PC-3 and DU-145) cell lines. High tumor accumulation was seen for both 225Ac-pelgi and 225Ac-DOTA-pelgi in the MDA-PCa-2b xenograft model. In the C4-2 xenograft model, 225Ac-pelgi showed enhanced antitumor efficacy with a T/Cvolume (treatment/control) ratio of 0.10 compared with 225Ac-DOTA-pelgi, 225Ac-DOTA-J591, and 227Th-HOPO-pelgifatamab (227Th-pelgi; all at 300 kBq/kg) with T/Cvolume ratios of 0.37, 0.39, and 0.33, respectively. 225Ac-pelgi was less myelosuppressive than 227Th-pelgi. 225Ac-pelgi showed dose-dependent treatment efficacy in the patient-derived KuCaP-1 model and strong combination potential with darolutamide in both cell line- (22Rv1) and patient-derived (ST1273) xenograft models.
CONCLUSIONS
These results provide a strong rationale to investigate 225Ac-pelgi in patients with prostate cancer. A clinical phase I study has been initiated (NCT06052306).
目的
前列腺癌最初对激素治疗有反应,但最终会产生耐药性。基于β发射体的前列腺特异性膜抗原(PSMA)靶向放射性核素疗法已被批准用于治疗转移性去势抵抗性前列腺癌。本文介绍了一种由 PSMA 抗体 pelgifatamab 与大环配体共价连接,并与锕-225 标记的靶向 α 治疗(TAT),并将其疗效和耐受性与其他 TAT 进行比较。
实验设计
在细胞系和患者来源的前列腺癌异种移植模型中,研究了 225Ac- macropa-pelgifatamab(225Ac-pelgi)和其他 TAT 的体外特性、体内分布、抗肿瘤疗效和耐受性。还研究了 225Ac-pelgi 与雄激素受体抑制剂达洛鲁胺联合应用的抗肿瘤疗效。
结果
225Ac-pelgi 在室温下的放射性标记效率已经很高。在 PSMA 表达(LNCaP、MDA-PCa-2b 和 C4-2)而非 PSMA 阴性(PC-3 和 DU-145)细胞系中观察到强烈的体外细胞毒性。在 MDA-PCa-2b 异种移植模型中,225Ac-pelgi 和 225Ac-DOTA-pelgi 均有较高的肿瘤摄取。在 C4-2 异种移植模型中,与 225Ac-DOTA-pelgi、225Ac-DOTA-J591 和 227Th-HOPO-pelgifatamab(227Th-pelgi;均为 300 kBq/kg)相比,225Ac-pelgi 的 T/C 体积(治疗/对照)比值为 0.10,具有增强的抗肿瘤疗效,分别为 0.37、0.39 和 0.33。与 227Th-pelgi 相比,225Ac-pelgi 的骨髓抑制作用较小。在患者来源的 KuCaP-1 模型中,225Ac-pelgi 表现出剂量依赖性的治疗效果,并在细胞系(22Rv1)和患者来源(ST1273)异种移植模型中与达洛鲁胺具有强烈的联合潜力。
结论
这些结果为在前列腺癌患者中研究 225Ac-pelgi 提供了强有力的依据。一项临床 I 期研究已经启动(NCT06052306)。
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