Comparative Radioimmunotherapy of Experimental Melanoma with Novel Humanized Antibody to Melanin Labeled with 213Bismuth and 177Lutetium

被引:21
作者
Allen, Kevin J. H. [1 ]
Jiao, Rubin [1 ]
Malo, Mackenzie E. [1 ]
Frank, Connor [1 ]
Fisher, Darrell R. [2 ]
Rickles, David [3 ]
Dadachova, Ekaterina [1 ]
机构
[1] Univ Saskatchewan, Coll Pharm & Nutr, Saskatoon, SK S7N 5E5, Canada
[2] Verst Med Phys & Radiat Safety, Richland, WA 99354 USA
[3] RadImmune Therapeut, Tarrytown, NY 10591 USA
关键词
radioimmunotherapy; humanized antibody; melanin; B16-F10; melanoma; 213Bismuth; 177Lutetium; IPILIMUMAB; RADIATION; SURVIVAL; CELLS;
D O I
10.3390/pharmaceutics11070348
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Melanoma is a cancer with increasing incidence and there is a need for alternatives to immunotherapy within effective approaches to treatment of metastatic melanoma. We performed comparative radioimmunotherapy (RIT) of experimental B16-F10 melanoma with novel humanized IgG to melanin h8C3 labeled with a beta emitter, Lu-177, and an alpha-emitter, Bi-213, as well as biodistribution, microSPECT/CT imaging, and mouse and human dosimetry calculations. microSPECT/CT imaging showed that a humanized antibody that targets free melanin in the tumor microenvironment had high tumor uptake in B16F10 murine melanoma in C57Bl/6 mice, with little to no uptake in naturally melanized tissues. Extrapolation of the mouse dosimetry data to an adult human demonstrated that doses delivered to major organs and the whole body by Lu-177-h8C3 would be approximately two times higher than those delivered by Bi-213-h8C3, while the doses to the tumor would be almost similar. RIT results indicated that Bi-213-h8C3 was more effective in slowing down the tumor growth than Lu-177-h8C3, while both radiolabeled antibodies did not produce significant hematologic or systemic side effects. We concluded that h8C3 antibody labeled with Bi-213 is a promising reagent for translation into a clinical trial in patients with metastatic melanoma.
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页数:11
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