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Dead cells in melanoma tumors provide abundant antigen for targeted delivery of ionizing radiation by a mAb to melanin

机译:黑色素瘤肿瘤中的死细胞提供了丰富的抗原可通过mAb定向释放电离辐射至黑色素

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摘要

Melanoma is a cancer with a rising incidence, and metastatic disease is almost always lethal. We investigated the feasibility of targeting melanin, an intracellular melanocyte pigment, to deliver cytotoxic radiation to human melanoma cells in vivo by using a melanin-binding mAb (6D2). Nude mice bearing MNT1 pigmented human melanoma tumors were treated with mAb 6D2 labeled with 1.5 mCi (1 Ci = 37 GBq) of the β-emitter 188-Rhenium (188Re) and manifested inhibition of tumor growth and prolonged survival. mAb 6D2 bound tumor melanin and demonstrated no crossreactivity with normal melanized tissues in black mice. The mechanism of melanin targeting involved Ab binding to extracellular melanin released during tumor cell turnover or to dying cells with permeable membranes. In this approach, the cytotoxic radiation emanating from labeled Ab bound to melanin is presumably delivered by “crossfire” effect to the adjacent viable tumor cells. Our results establish the feasibility of targeting melanin released from dead melanoma cells in tumors with radiolabeled Abs to achieve a therapeutic effect. In contrast to conventional tumor antigens, melanin is insoluble, resistant to degradation, and can be expected to accumulate in targeted tissues, suggesting that the efficacy of therapy could increase with each subsequent treatment cycle.
机译:黑色素瘤是一种发病率不断上升的癌症,而转移性疾病几乎总是致命的。我们研究了靶向黑色素(一种细胞内黑色素细胞色素)通过使用黑色素结合mAb(6D2)在体内向人黑色素瘤细胞传递细胞毒性辐射的可行性。用标记有1.5 mCi(1 Ci = 37 GBq)的β-发射体188- <( 188 Re)的mAb 6D2处理带有MNT1色素性黑色素瘤的裸鼠。延长生存期。 mAb 6D2结合肿瘤黑色素,在黑色小鼠中与正常黑色素化组织无交叉反应。黑色素靶向机制涉及抗体结合肿瘤细胞更新期间释放的细胞外黑色素或具有可渗透膜的垂死细胞。在这种方法中,由标记的与黑色素结合的Ab发出的细胞毒性辐射大概是通过“交火”效应传递到相邻的存活肿瘤细胞上的。我们的结果确立了用放射性标记的Abs靶向从死去的黑色素瘤细胞中释放的黑色素达到治疗效果的可行性。与常规的肿瘤抗原相反,黑色素不溶,对降解具有抗性,并且可以预期在靶组织中蓄积,这表明治疗的功效可能随随后的每个治疗周期而增加。

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