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α-取代残基在β-肽12-螺旋中的容纳:扩展折叠体支架可用的取代模式范围。

Accommodation of alpha-substituted residues in the beta-peptide 12-helix: expanding the range of substitution patterns available to a foldamer scaffold.

作者信息

Park Jin-Seong, Lee Hee-Seung, Lai Jonathan R, Kim Byeong Moon, Gellman Samuel H

机构信息

School of Chemistry, College of Natural Sciences, Seoul National University, Seoul 151-742, Korea.

出版信息

J Am Chem Soc. 2003 Jul 16;125(28):8539-45. doi: 10.1021/ja034180z.

DOI:10.1021/ja034180z
PMID:12848561
Abstract

Beta-amino acid oligomers composed exclusively of homochiral trans-2-aminocyclopentanecarboxylic acid (ACPC) residues and/or related pyrrolidine-based residues are known to favor a specific helical secondary structure that is defined by 12-membered ring C=O(i)- -H-N(i+3) hydrogen bonds ("12-helix"). The 12-helix is structurally similar to the familiar alpha-helix and therefore represents a source of potential alpha-helix-mimics. The 12-helix will be most useful in this regard if this conformational scaffold can be employed to arrange specific sets of protein-like side chains in space. Here we examine whether the 12-helix tolerates insertion of acyclic beta-amino acid residues bearing a substituent in the alpha-position ("beta(2)-residues"). Seventeen homologous beta-peptide heptamers have been prepared in which one to four beta(2)-residues reside among ACPC and/or pyrrolidine residues. Circular dichroism comparisons suggest that beta(2)-residues have a lower 12-helical propensity than do residues preorganized by a five-membered ring, as expected, but that beta-peptides containing beta(2)-residues at one or two of the seven positions retain a significant preference for 12-helix formation. These results indicate that a limited number of beta(2)-residues can be used to introduce side chains at specific positions along the surface of a 12-helix.

摘要

仅由同手性反式-2-氨基环戊烷羧酸(ACPC)残基和/或相关的基于吡咯烷的残基组成的β-氨基酸低聚物,已知有利于一种特定的螺旋二级结构,该结构由12元环C=O(i)- -H-N(i+3)氢键(“12-螺旋”)定义。12-螺旋在结构上与常见的α-螺旋相似,因此是潜在的α-螺旋模拟物的来源。如果这种构象支架可用于在空间中排列特定的类蛋白质侧链组,那么12-螺旋在这方面将最有用。在这里,我们研究12-螺旋是否能容忍在α-位带有取代基的无环β-氨基酸残基(“β(2)-残基”)的插入。已经制备了十七种同源的β-肽七聚体,其中一到四个β(2)-残基存在于ACPC和/或吡咯烷残基之间。圆二色性比较表明,正如预期的那样,β(2)-残基的12-螺旋倾向低于由五元环预组织的残基,但在七个位置中的一或两个位置含有β(2)-残基的β-肽对12-螺旋形成仍有显著偏好。这些结果表明,有限数量的β(2)-残基可用于在12-螺旋表面的特定位置引入侧链。

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