靶向系统性放射治疗联合 scVEGF/177Lu 可导致肿瘤血管持续破坏和肿瘤内细胞凋亡。
Targeted systemic radiotherapy with scVEGF/177Lu leads to sustained disruption of the tumor vasculature and intratumoral apoptosis.
机构信息
Department of Radiology/MIPS, Stanford University, Palo Alto, California, USA.
出版信息
J Nucl Med. 2011 Oct;52(10):1630-7. doi: 10.2967/jnumed.111.091629. Epub 2011 Sep 2.
UNLABELLED
Tumor vessels abundantly express receptors for vascular endothelial growth factor (VEGF), despite treatment with conventional or antiangiogenic drugs. We wished to determine whether the high levels of VEGF receptor (VEGFR) within the tumor vasculature could be leveraged for intracellular delivery of therapeutically significant doses of scVEGF/(177)Lu, a novel radiopharmaceutical based on a recombinant single-chain (sc) derivative of VEGF, in orthotopic breast cancer models.
METHODS
scVEGF-PEG (polyethylene gycol)-DOTA conjugates containing 2.0-, 3.4-, or 5.0-kDa PEG linkers site-specifically conjugated to a cysteine-containing tag (Cys-tag) in scVEGF were radiolabeled with (177)Lu (scVEGF/(177)Lu) for in vivo studies. Human MDA231luc and mouse 4T1luc cell lines were injected orthotopically to establish breast carcinoma tumors in immunodeficient and immunocompetent hosts, respectively. The effects of scVEGF/(177)Lu were defined by analysis of changes in tumor growth and immunohistochemical staining for the endothelial markers CD31 and VEGFR-2 and terminal deoxynucleotidyl transferase-mediated dUTP nick-end labeling (TUNEL) staining for intratumoral apoptosis.
RESULTS
Biodistribution assays and dosimetric calculations established that scVEGF/(177)Lu with a 3.4-kDa PEG linker delivered the highest dose of radiation to tumors (69.9 cGy/MBq/g of tissue) and the lowest dose to the kidneys (33.3 cGy/MBq/organ). Total doses below 40 MBq/mouse of scVEGF/(177)Lu did not affect renal function, and 3 divided doses of 6.3 MBq/mouse or a bolus dose of 18.9 MBq/mouse induced only transient lymphopenia and weight loss (<10% baseline weight). In mice with orthotopic mammary breast carcinoma, intravenous injections of well-tolerated bolus and fractionated doses of scVEGF/(177)Lu in the range from 6.3 to 18.9 MBq/mouse (25-76 MBq/m(2)) resulted in dose-dependent tumor growth inhibition. Immunohistochemical analysis of tumors at 4-5 wk after single injections of scVEGF/(177)Lu indicated dose-dependent regression of tumor vasculature and widespread intratumoral apoptosis. A single dose of 7.4 MBq/mouse of scVEGF/(177)Lu given before a course of bevacizumab or sunitinib treatment enhanced the antiangiogenic effects of both drugs.
CONCLUSION
Selective targeting of VEGFR in tumor vasculature with well-tolerated doses of scVEGF/(177)Lu is effective in orthotopic breast cancer models. As high levels of VEGFR expression in the tumor vasculature are a common feature in a variety of cancers, targeting tumor angiogenesis with scVEGF/(177)Lu warrants further exploration.
目的
尽管常规或抗血管生成药物治疗,但肿瘤血管大量表达血管内皮生长因子(VEGF)受体。我们希望确定肿瘤血管中 VEGFR 的高表达水平是否可以用于细胞内递送至治疗相关剂量的 scVEGF/(177)Lu,scVEGF/(177)Lu 是一种基于 VEGF 重组单链(sc)衍生物的新型放射性药物。
方法
scVEGF-PEG(聚乙二醇)-DOTA 缀合物含有 2.0、3.4 或 5.0 kDa PEG 接头,特异性连接到 scVEGF 中的半胱氨酸标签(Cys-tag)上,用(177)Lu 标记(scVEGF/(177)Lu)用于体内研究。人 MDA231luc 和小鼠 4T1luc 细胞系分别通过原位注射建立乳腺癌肿瘤,分别在免疫缺陷和免疫活性宿主中。通过分析肿瘤生长变化、内皮标志物 CD31 和 VEGFR-2 的免疫组织化学染色以及肿瘤内细胞凋亡的末端脱氧核苷酸转移酶介导的 dUTP 缺口末端标记(TUNEL)染色来定义 scVEGF/(177)Lu 的作用。
结果
生物分布测定和剂量计算确定,具有 3.4 kDa PEG 接头的 scVEGF/(177)Lu 向肿瘤提供最高剂量的辐射(69.9 cGy/MBq/g 组织),向肾脏提供最低剂量(33.3 cGy/MBq/器官)。低于 40 MBq/小鼠的 scVEGF/(177)Lu 总剂量不影响肾功能,6.3 MBq/小鼠的 3 个等分剂量或 18.9 MBq/小鼠的单次剂量仅引起短暂的淋巴细胞减少和体重减轻(<10%基线体重)。在患有原位乳腺乳腺癌的小鼠中,静脉内注射耐受良好的 scVEGF/(177)Lu 单次和分次剂量范围为 6.3 至 18.9 MBq/小鼠(25-76 MBq/m(2))导致肿瘤生长抑制呈剂量依赖性。scVEGF/(177)Lu 单次注射后 4-5 周对肿瘤进行的免疫组织化学分析表明,肿瘤血管呈剂量依赖性消退,广泛发生肿瘤内细胞凋亡。在贝伐单抗或舒尼替尼治疗前给予 7.4 MBq/小鼠的 scVEGF/(177)Lu 单剂量可增强这两种药物的抗血管生成作用。
结论
用耐受良好的 scVEGF/(177)Lu 剂量选择性靶向 VEGFR 在原位乳腺癌模型中是有效的。由于肿瘤血管中 VEGFR 的高表达水平是多种癌症的共同特征,因此用 scVEGF/(177)Lu 靶向肿瘤血管生成值得进一步探索。
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