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兰瑞肽自组装形成纳米管的分子起源:一种突变方法

Molecular origin of the self-assembly of lanreotide into nanotubes: a mutational approach.

作者信息

Valéry Céline, Pouget Emilie, Pandit Anjali, Verbavatz Jean-Marc, Bordes Luc, Boisdé Isabelle, Cherif-Cheikh Roland, Artzner Franck, Paternostre Maité

机构信息

Ipsen Pharma, 08980 Sant Feliu de Llobregat, Barcelona, Spain.

出版信息

Biophys J. 2008 Mar 1;94(5):1782-95. doi: 10.1529/biophysj.107.108175. Epub 2007 Nov 9.

Abstract

Lanreotide, a synthetic, therapeutic octapeptide analog of somatostatin, self-assembles in water into perfectly hollow and monodisperse (24-nm wide) nanotubes. Lanreotide is a cyclic octapeptide that contains three aromatic residues. The molecular packing of the peptide in the walls of a nanotube has recently been characterized, indicating four hierarchical levels of organization. This is a fascinating example of spontaneous self-organization, very similar to the formation of the gas vesicle walls of Halobacterium halobium. However, this unique peptide self-assembly raises important questions about its molecular origin. We adopted a directed mutation approach to determine the molecular parameters driving the formation of such a remarkable peptide architecture. We have modified the conformation by opening the cycle and by changing the conformation of a Lys residue, and we have also mutated the aromatic side chains of the peptide. We show that three parameters are essential for the formation of lanreotide nanotubes: i), the specificity of two of the three aromatic side chains, ii), the spatial arrangement of the hydrophilic and hydrophobic residues, and iii), the aromatic side chain in the beta-turn of the molecule. When these molecular characteristics are modified, either the peptides lose their self-assembling capability or they form less-ordered architectures, such as amyloid fibers and curved lamellae. Thus we have determined key elements of the molecular origins of lanreotide nanotube formation.

摘要

兰瑞肽是一种合成的生长抑素治疗性八肽类似物,在水中自组装成完美的中空且单分散(宽24纳米)的纳米管。兰瑞肽是一种环状八肽,含有三个芳香族残基。最近已对纳米管壁中该肽的分子堆积进行了表征,表明存在四个层次的组织水平。这是自发自组装的一个引人入胜的例子,与嗜盐菌的气荚膜壁的形成非常相似。然而,这种独特的肽自组装引发了关于其分子起源的重要问题。我们采用定向突变方法来确定驱动形成这种非凡肽结构的分子参数。我们通过打开环和改变赖氨酸残基的构象来改变构象,并且我们还对该肽的芳香族侧链进行了突变。我们表明,三个参数对于兰瑞肽纳米管的形成至关重要:i)三个芳香族侧链中的两个的特异性,ii)亲水和疏水残基的空间排列,以及iii)分子β-转角中的芳香族侧链。当这些分子特征被改变时,要么肽失去其自组装能力,要么它们形成无序程度较低的结构,如淀粉样纤维和弯曲薄片。因此,我们已经确定了兰瑞肽纳米管形成的分子起源的关键要素。

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