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Two Saporin-Containing Immunotoxins Specific for CD20 and CD22 Show Different Behavior in Killing Lymphoma Cells

机译:CD20和CD22特有的两种含Saporin的免疫毒素在杀死淋巴瘤细胞中表现出不同的行为

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摘要

Immunotoxins (ITs) are hybrid proteins combining the binding specificity of antibodies with the cytocidal properties of toxins. They represent a promising approach to lymphoma therapy. The cytotoxicity of two immunotoxins obtained by chemical conjugation of the plant toxin saporin-S6 with the anti-CD20 chimeric antibody rituximab and the anti-CD22 murine antibody OM124 were evaluated on the CD20-/CD22-positive cell line Raji. Both ITs showed strong cytotoxicity for Raji cells, but the anti-CD22 IT was two logs more efficient in killing, probably because of its faster internalization. The anti-CD22 IT gave slower but greater caspase activation than the anti-CD20 IT. The cytotoxic effect of both immunotoxins can be partially prevented by either the pan-caspase inhibitor Z-VAD or the necroptosis inhibitor necrostatin-1. Oxidative stress seems to be involved in the cell killing activity of anti-CD20 IT, as demonstrated by the protective role of the H2O2 scavenger catalase, but not in that of anti-CD22 IT. Moreover, the IT toxicity can be augmented by the contemporary administration of other chemotherapeutic drugs, such as PS-341, MG-132, and fludarabine. These results contribute to the understanding of the immunotoxin mechanism of action that is required for their clinical use, either alone or in combination with other drugs.
机译:免疫毒素(IT)是结合抗体的结合特异性和毒素的杀细胞特性的杂合蛋白。它们代表了一种有前途的淋巴瘤治疗方法。在CD20- / CD22阳性细胞系Raji上评估了通过将植物毒素saporin-S6与抗CD20嵌合抗体利妥昔单抗和抗CD22鼠抗体OM124化学偶联而获得的两种免疫毒素的细胞毒性。两种IT对Raji细胞均显示出强大的细胞毒性,但抗CD22 IT的杀伤效率要高两个对数,这可能是因为其更快的内在化。与抗CD20 IT相比,抗CD22 IT的半胱天冬酶活化较慢,但更大。泛半胱天冬酶抑制剂Z-VAD或坏死病抑制剂necrostatin-1可以部分预防两种免疫毒素的细胞毒性作用。氧化应激似乎与抗CD20 IT的细胞杀伤活性有关,如过氧化氢过氧化氢过氧化氢酶的保护作用所证明的,但抗CD22 IT却没有。此外,可以通过当代施用其他化学治疗药物(例如PS-341,MG-132和氟达拉滨)来增强IT毒性。这些结果有助于理解其临床用途所需要的免疫毒素作用机理,无论是单独使用还是与其他药物联合使用。

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