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蓖麻毒素对体外蛋白质合成的抑制作用。核糖体作为毒素的作用靶点。

Inhibition by ricin of protein synthesis in vitro. Ribosomes as the target of the toxin.

作者信息

Montanaro L, Sperti S, Stirpe F

出版信息

Biochem J. 1973 Nov;136(3):677-83. doi: 10.1042/bj1360677.

Abstract
  1. Ricin (a toxic protein from the seeds of Ricinus communis) is a powerful inhibitor of the poly(U)-directed incorporation of phenylalanine into polypeptides catalysed by isolated rat liver ribosomes and elongation factors 1 and 2 (EF 1 and EF 2). The inhibition can be largely overcome by increasing the concentration of ribosomes. 2. The toxin does not affect the binding of phenylalanyl-tRNA to ribosomes catalysed by EF 1, nor does it inhibit the puromycin reaction used as a test for peptide-bond formation catalysed by ribosomes. 3. Ricin inhibits the ribosome-linked GTP hydrolysis catalysed by EF 2. 4. Ribosomes treated with ricin and washed through sucrose gradients containing 0.6m-NH(4)Cl are functionally inactive in those assay systems that are sensitive to the presence of added toxin. 5. It is suggested that ricin brings about an irreversible modification of ribosomes which impairs their ability to interact with EF 2. Since ricin inhibits at a molar concentration much lower than that of ribosomes it probably acts catalytically. No added cofactor is necessary for the inhibitory action of the toxin.
摘要
  1. 蓖麻毒素(一种从蓖麻种子中提取的有毒蛋白质)是一种强大的抑制剂,可抑制由分离的大鼠肝脏核糖体以及延伸因子1和2(EF 1和EF 2)催化的聚(U)指导的苯丙氨酸掺入多肽的过程。通过增加核糖体的浓度,这种抑制作用在很大程度上可以被克服。2. 该毒素不影响由EF 1催化的苯丙氨酰 - tRNA与核糖体的结合,也不抑制用作核糖体催化的肽键形成测试的嘌呤霉素反应。3. 蓖麻毒素抑制由EF 2催化的核糖体连接的GTP水解。4. 用蓖麻毒素处理并通过含有0.6m - NH(4)Cl的蔗糖梯度洗涤的核糖体,在那些对添加毒素的存在敏感的测定系统中功能失活。5. 有人提出,蓖麻毒素会对核糖体进行不可逆的修饰,从而损害其与EF 2相互作用的能力。由于蓖麻毒素在比核糖体低得多的摩尔浓度下就能产生抑制作用,所以它可能起催化作用。毒素的抑制作用不需要添加辅助因子。

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Site of action of ricin on the ribosome.蓖麻毒素在核糖体上的作用位点。
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本文引用的文献

4
Ricin - a potent inhibitor of protein synthesis.蓖麻毒素——一种强大的蛋白质合成抑制剂。
FEBS Lett. 1972 Feb 15;20(3):327-329. doi: 10.1016/0014-5793(72)80098-x.
5
Studies on the toxic action of ricin.蓖麻毒素的毒性作用研究。
Proc Soc Exp Biol Med. 1966 Mar;121(3):685-91. doi: 10.3181/00379727-121-30861.

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