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识别表皮生长因子受体的配体和抗体导向蓖麻毒素A链缀合物的毒性

Toxicity of ligand and antibody-directed ricin A-chain conjugates recognizing the epidermal growth factor receptor.

作者信息

Vollmar A M, Banker D E, Mendelsohn J, Herschman H R

出版信息

J Cell Physiol. 1987 Jun;131(3):418-25. doi: 10.1002/jcp.1041310314.

Abstract

Approximately equal amounts of 125I-mAb 225 (a monoclonal antibody recognizing the human epidermal growth factor receptor) and 125I-labeled epidermal growth factor (125I-EGF) were bound by HeLa cells. However, these two EGF receptor binding moieties had different fates after binding. Sixty percent of cell-associated 125I-EGF was internalized. The majority of internalized 125I was released from the cell within 2 hr. In contrast, whereas only 30% of bound 125I-mAb 225 was internalized by HeLa cells, the internalized radioactivity remained cell-associated. EGF and mAb 225 were used to construct ricin A-chain (RTA) conjugates. The two chimeric molecules, EGF-RTA and mAb 225-RTA, were equally toxic to human HeLa cells. EGF-RTA was also toxic to murine 3T3 cells. In contrast, mAb 225-RTA was not toxic to 3T3 cells, consistent with the human EGF-receptor specificity of mAb 225. Neither conjugate was cytotoxic to EGF receptor-deficient 3T3-NR6 cells. Rapidity and potency of protein synthesis inhibition of HeLa cells were equivalent for the two chimeric conjugates, as was the degree to which colony-forming ability was reduced. However, ammonium chloride enhanced the toxicity of EGF-RTA but not mAb 225-RTA, suggesting that the two toxic chimeric toxins--like the unconjugated receptor-binding moieties--are processed differently by HeLa cells.

摘要

等量的125I标记的单克隆抗体225(一种识别人类表皮生长因子受体的单克隆抗体)和125I标记的表皮生长因子(125I-EGF)被HeLa细胞结合。然而,这两种表皮生长因子受体结合部分在结合后有着不同的命运。60%与细胞结合的125I-EGF被内化。大部分内化的125I在2小时内从细胞中释放出来。相比之下,虽然只有30%结合的125I-单克隆抗体225被HeLa细胞内化,但内化的放射性仍与细胞相关。表皮生长因子(EGF)和单克隆抗体225被用于构建蓖麻毒素A链(RTA)偶联物。两种嵌合分子,EGF-RTA和单克隆抗体225-RTA,对人类HeLa细胞具有同等毒性。EGF-RTA对鼠3T3细胞也有毒性。相比之下,单克隆抗体225-RTA对3T3细胞无毒,这与单克隆抗体225对人类表皮生长因子受体的特异性一致。两种偶联物对表皮生长因子受体缺陷的3T3-NR6细胞均无细胞毒性。两种嵌合偶联物对HeLa细胞蛋白质合成抑制的速度和效力相当,对集落形成能力降低的程度也相当。然而,氯化铵增强了EGF-RTA的毒性,但没有增强单克隆抗体225-RTA的毒性,这表明这两种有毒的嵌合毒素——与未偶联的受体结合部分一样——在HeLa细胞中的处理方式不同。

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