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Folding and activity of hybrid sequence disulfide-stabilized peptides.

机译:杂合序列二硫键稳定肽的折叠和活性。

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摘要

Peptides have been synthesized that have hybrid sequences, partially derived from the bee venom peptide apamin and partially from the S peptide of ribonuclease A. The hybrid peptides were demonstrated by NMR spectroscopy to fold, forming the same disulfides and basic three-dimensional structure as native apamin, containing a beta-turn and an alpha-helix. These hybrids were active in complementing S protein, reactivating nuclease activity. In addition, the hybrid peptide was effective in inducing antibodies that cross-react with the RNase, without conjugation to a carrier protein. The stability of the folded structure of this peptide suggests that it should be possible to elicit antibodies that will react not only with a specific sequence, but also with a specific secondary structure. Hybrid sequence peptides also provide opportunities to study separately nucleation and propagation steps in formation of secondary structure. We show that in S peptide the alpha-helix does not end abruptly but rather terminates gradually over four or five residues. In general, these hybrid sequence peptides, which fold predictably because of disulfide bond formation, can provide opportunities for examining structure-function relationships for many biologically active sequences.
机译:已经合成了具有杂合序列的肽,该杂合序列部分来源于蜂毒肽apamin和部分来源于核糖核酸酶A的S肽。通过NMR光谱证明了杂合肽折叠,形成了与天然相同的二硫键和基本三维结构含有β-转角和α-螺旋的木瓜蛋白酶。这些杂种在补充S蛋白,激活核酸酶活性方面具有活性。另外,杂合肽可有效诱导与RNA酶交叉反应的抗体,而不与载体蛋白缀合。该肽的折叠结构的稳定性表明,应该有可能引发不仅与特定序列反应而且与特定二级结构反应的抗体。杂合序列肽还提供了分别研究二级结构形成中的成核和繁殖步骤的机会。我们显示,在S肽中,α-螺旋不会突然终止,而是会在四个或五个残基上逐渐终止。通常,这些杂合序列肽由于二硫键的形成而可预测地折叠,可以为检查许多生物学活性序列的结构-功能关系提供机会。

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