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Preparation of Recombinant Protein A‐Lymphotoxin Chimeric Protein and Its Antitumor Effects in Mice

机译:重组蛋白A-Lymphotoxin嵌合蛋白的制备及其在小鼠中的抗肿瘤作用

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摘要

We have investigated the in vivo function of a chimeric protein constructed by recombinant DNA techniques. The behavior and antitumor activity of a protein A‐lymphotoxin chimera (ALT) was examined on a murine tumor in mice in comparison with ammo‐terminal 19 amino acid‐deleted lymphotoxin (dLT), Seven‐week‐old male BALB/c mice were implanted intradermally with Meth‐A fibrosarcoma on day 0. ALT and dLT caused tumor regression, hemorrhagic necrosis and complete regression in a dose‐related way when each agent was given intratumorally 5 times (days 5–9). The ratio of the median effective doses for complete tumor regression was 1.6 between ALT and dLT on a molar basis. ALT caused tumor regression and body weight loss when given intravenously on the same schedule. Biodistribution studies with 125I‐labeled ALT and dLT demonstrated that, after intratumoral administration, ALT was retained longer in the administered site and was cleared more slowly from the mouse body than dLT. These findings suggest that a protein A‐lymphotoxin chimeric protein expresses both antitumor activity similar to that of lymphotoxin and characteristic in vivo behavior of the fused protein A portion.
机译:我们已经研究了通过重组DNA技术构建的嵌合蛋白的体内功能。与具有19个氨基酸末端的氨基末端的淋巴毒素(dLT)相比,在小鼠的小鼠肿瘤上检测了A-淋巴毒素嵌合体(ALT)的行为和抗肿瘤活性,其中7周龄的雄性BALB / c小鼠在第0天皮内植入Meth-A纤维肉瘤。当每种药物在瘤内给予5次时(第5-9天),ALT和dLT以剂量相关的方式引起肿瘤消退,出血性坏死和完全消退。完全肿瘤消退的中位有效剂量比在ALT和dLT之间为1.6。当按相同的时间表静脉注射时,ALT导致肿瘤消退和体重减轻。用 125 I标记的ALT和dLT进行的生物分布研究表明,瘤内给药后,ALT在给药部位的保留时间更长,并且从小鼠体内清除的速度比dLT慢。这些发现表明,蛋白A-淋巴毒素嵌合蛋白既表达与淋巴毒素相似的抗肿瘤活性,又表达融合蛋白A部分的体内特征。

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