用[212Pb/203Pb]-Pentixather靶向CXCR4可显著提高小细胞肺癌患者的总生存率

Keegan A Christensen, MELISSA A Fath, Jordan T Ewald, Claudia Robles-Planells, Stephen A Graves, Spenser S Johnson, Zeb R Zacharias, Jon C. D. Houtman, M. Sue O'Dorisio, Michael K Schultz, Bryan G. Allen, Muhammad Furqan, Yusuf Menda, Dijie Liu, Douglas R Spitz
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引用次数: 0

摘要

简介小细胞肺癌(SCLC)的5年总生存率仅为7%。C-X-C 趋化因子受体 4 (CXCR4)是治疗药物的一个极具吸引力的靶点,它在 SCLC 中高度表达,并可通过使用治疗对 212Pb/203Pb 与 pentixather 靶向。我们对[212Pb/203Pb]-pentixather 可安全有效地用于 SCLC 异种移植模型的成像和治疗这一假设进行了测试。结果:对注射了[203Pb]-pentixather的肿瘤小鼠进行的SPECT/CT成像和生物分布研究表明,肿瘤中的摄取依赖于CXCR4,放射性配体在肾脏和肝脏中蓄积。剂量测定计算估计了肿瘤和正常组织对[212Pb]-pentixather的摄取量。对 SCLC 异种移植物(DMS273 和 H69AR)进行[212Pb]-pentixather 处理(37-111 kBq/g)可显著延长生存期并延缓肿瘤生长。用[212Pb]-pentixather(37-111 kBq/g)治疗移植了人类 hCD34+ 骨髓的 NSG 小鼠时,在治疗后 13-18 天的外周血全血细胞计数(CBC)中观察到明显的细胞减少现象,这种现象在第 28-31 天消失。在第 28-31 天,这些动物骨髓造血干细胞的流式细胞术显示,人类造血标志物 CD45(hCD45+)的频率明显降低,骨髓中的鼠类 CD45+(mCD45+)系重组。结论[203Pb]-pentixather可用于对表达CXCR4的SCLC异种进行成像,用α发射体[212Pb]-pentixather治疗可显著延长SCLC异种的中位总生存期。与 hCD45+ 骨髓相比,[212Pb]-pentixather 治疗 28-31 天后,在接种了人类骨髓的 NSG 小鼠中检测到明显更多的 mCD45+ 骨髓再填充。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Targeting CXCR4 with [212Pb/203Pb]-Pentixather Significantly Increases Overall Survival in Small Cell Lung Cancer
Introduction: Small cell lung cancer (SCLC) has a 7% 5-year overall survival. C-X-C chemokine receptor 4 (CXCR4), an attractive target for theranostic agents, is highly expressed in SCLCs, and can be targeted with pentixather using the theranostic pair 212Pb/203Pb. The hypothesis that [212Pb/203Pb]-pentixather can be used safely and effectively for imaging and therapy in SCLC in xenograft models was tested. Results: SPECT/CT imaging and biodistribution studies of tumor bearing mice injected with [203Pb]-pentixather demonstrated CXCR4-dependent uptake in tumors and accumulation of radioligand in kidneys and livers. Dosimetry calculations estimated [212Pb]-pentixather uptake in tumor and normal tissue. [212Pb]-pentixather treatment (37-111 kBq/g) of SCLC xenografts (DMS273 and H69AR) significantly prolonged survival and delayed tumor growth. When NSG mice grafted with human hCD34+ bone marrow were treated with [212Pb]-pentixather (37-111 kBq/g), significant cytopenias were observed in peripheral blood complete blood counts (CBCs) at 13-18 days post treatment which resolved by day 28-31. Flow cytometry of bone marrow hematopeotic stem cells in these animals at day 28-31 demonstrated a significantly reduced frequency of the human hematopoietic marker CD45 (hCD45+) and reconstitution of the bone marrow with murine CD45+ (mCD45+) lineages. Conclusions: [203Pb]-pentixather can be used to image CXCR4 expressing SCLC xenografts and treatment with alpha emitter [212Pb]-pentixather significantly prolongs SCLC xenograft median overall survival. Significantly greater mCD45+ bone marrow repopulation was detected in NSG mice engrafted with human bone marrow 28-31 days following [212Pb]-pentixather treatment, relative to hCD45+ bone marrow.
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