首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Concept of internal structural controls for evaluation of inactive synthetic peptide analogs: synthesis of Orn1314apamin and its guanidination to an apamin derivative with full neurotoxic activity.
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Concept of internal structural controls for evaluation of inactive synthetic peptide analogs: synthesis of Orn1314apamin and its guanidination to an apamin derivative with full neurotoxic activity.

机译:用于评估非活性合成肽类似物的内部结构控制的概念:Orn1314 apamin的合成及其胍基化为具有完全神经毒性活性的apamin衍生物。

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摘要

The importance of arginine residues 13 and 14 in the bee venom neurotoxin, apamin, was teste by the synthesis of replacement analogs. [13,14-di-Ndelta-trifluoroacetylornithine]Apamin was synthesized by the solid phase method on a benzhydrylamine resin. It was deprotected to [13,14-diornithine]apamin, which was then guanidinated to produce the 4-homoarginine-13,14-diarginine analog, [Har4]apamin. Neither the trifluoroacetylornithine analog nor the ornithine analog produced any detectable symptoms when injected intravenously into mice. However, the synthetic [Har4]apamin exhibited the full neurotoxic activity of native apamin and of [Har4]apamin derived from the natural toxin. This provided an internal structural control for the correctness of the primary structure of the inactive synthetic analogs and strengthened the conclusion that one, or both, of the arginine residues plays an important role in the action of apamin.
机译:蜂毒神经毒素apamin中精氨酸残基13和14的重要性通过合成替代类似物来证明。通过固相法在苯甲基胺树脂上合成了[13,14-二-Ndelta-三氟乙酰鸟氨酸] Apamin。将其脱保护为[13,14-二鸟氨酸] apamin,然后对其进行胍基化处理以生成4-homoarginine-13,14-diarginine类似物[Har4] apamin。当静脉注射入小鼠体内时,三氟乙酰鸟氨酸类似物和鸟氨酸类似物均未产生任何可检测到的症状。但是,合成的[Har4] apamin表现出天然的apaapamin和源自天然毒素的[har4] apamin的全部神经毒性活性。这为无活性合成类似物的一级结构的正确性提供了内部结构控制,并加强了一个结论,即精氨酸残基中的一个或两个都在apapamin作用中起重要作用。

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