Controlling 1D Nanostructures and Handedness by Polar Residue Chirality of Amphiphilic Peptides

Hai Xu; Kai Qi; Cheng Zong; Jing Deng; Peng Zhou; Xuzhi Hu; Xiaoyue Ma; Dong Wang; Muhan Wang; Jun Zhang; Stephen M. King; Sarah E. Rogers; Jian Ren Lu; Jun Yang; Jiqian Wang

doi:10.1002/smll.202304424

Controlling 1D Nanostructures and Handedness by Polar Residue Chirality of Amphiphilic Peptides

Hai Xu, Kai Qi, Cheng Zong, Jing Deng, Peng Zhou, Xuzhi Hu, Xiaoyue Ma, Dong Wang, Muhan Wang, Jun Zhang, Stephen M. King, Sarah E. Rogers, Jian Ren Lu, Jun Yang, Jiqian Wang

Biological Physics Group

Research output: Contribution to journal › Article › peer-review

Abstract

Peptide assemblies are promising nanomaterials, with their properties and technological applications being highly hinged on their supramolecular architectures. Here, how changing the chirality of the terminal charged residues of an amphiphilic hexapeptide sequence Ac-I4K2-NH2 gives rise to distinct nanostructures and supramolecular handedness is reported. Microscopic imaging and neutron scattering measurements show thin nanofibrils, thick nanofibrils, and wide nanotubes self-assembled from four stereoisomers. Spectroscopic and solid-state nuclear magnetic resonance (NMR) analyses reveal that these isomeric peptides adopt similar anti-parallel β-sheet secondary structures. Further theoretical calculations demonstrate that the chiral alterations of the two C-terminal lysine residues cause the formation of diverse single β-strand conformations, and the final self-assembled nanostructures and handedness are determined by the twisting direction and degree of single β-strands. This work not only lays a useful foundation for the fabrication of diverse peptide nanostructures by manipulating the chirality of specific residues but also provides a framework for predicting the supramolecular structures and handedness of peptide assemblies from single molecule conformations.

Original language	English
Journal	Small
Volume	20
Issue number	5
DOIs	https://doi.org/10.1002/smll.202304424
Publication status	Published - 1 Feb 2024

Keywords

amphiphilic peptides
molecular chirality
nanofibrils
nanotubes
polar residues
supramolecular handedness
theoretical calculations

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10.1002/smll.202304424

I4K2manuscript_15July_2022-yang_Jian Lu_Xu - Small Xu H et al. finalAccepted author manuscript, 4.74 MBLicence: CC BY

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title = "Controlling 1D Nanostructures and Handedness by Polar Residue Chirality of Amphiphilic Peptides",

abstract = "Peptide assemblies are promising nanomaterials, with their properties and technological applications being highly hinged on their supramolecular architectures. Here, how changing the chirality of the terminal charged residues of an amphiphilic hexapeptide sequence Ac-I4K2-NH2 gives rise to distinct nanostructures and supramolecular handedness is reported. Microscopic imaging and neutron scattering measurements show thin nanofibrils, thick nanofibrils, and wide nanotubes self-assembled from four stereoisomers. Spectroscopic and solid-state nuclear magnetic resonance (NMR) analyses reveal that these isomeric peptides adopt similar anti-parallel β-sheet secondary structures. Further theoretical calculations demonstrate that the chiral alterations of the two C-terminal lysine residues cause the formation of diverse single β-strand conformations, and the final self-assembled nanostructures and handedness are determined by the twisting direction and degree of single β-strands. This work not only lays a useful foundation for the fabrication of diverse peptide nanostructures by manipulating the chirality of specific residues but also provides a framework for predicting the supramolecular structures and handedness of peptide assemblies from single molecule conformations.",

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author = "Hai Xu and Kai Qi and Cheng Zong and Jing Deng and Peng Zhou and Xuzhi Hu and Xiaoyue Ma and Dong Wang and Muhan Wang and Jun Zhang and King, {Stephen M.} and Rogers, {Sarah E.} and Lu, {Jian Ren} and Jun Yang and Jiqian Wang",

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AU - Xu, Hai

AU - Qi, Kai

AU - Zong, Cheng

AU - Deng, Jing

AU - Zhou, Peng

AU - Hu, Xuzhi

AU - Ma, Xiaoyue

AU - Wang, Dong

AU - Wang, Muhan

AU - Zhang, Jun

AU - King, Stephen M.

AU - Rogers, Sarah E.

AU - Lu, Jian Ren

AU - Yang, Jun

AU - Wang, Jiqian

PY - 2024/2/1

Y1 - 2024/2/1

N2 - Peptide assemblies are promising nanomaterials, with their properties and technological applications being highly hinged on their supramolecular architectures. Here, how changing the chirality of the terminal charged residues of an amphiphilic hexapeptide sequence Ac-I4K2-NH2 gives rise to distinct nanostructures and supramolecular handedness is reported. Microscopic imaging and neutron scattering measurements show thin nanofibrils, thick nanofibrils, and wide nanotubes self-assembled from four stereoisomers. Spectroscopic and solid-state nuclear magnetic resonance (NMR) analyses reveal that these isomeric peptides adopt similar anti-parallel β-sheet secondary structures. Further theoretical calculations demonstrate that the chiral alterations of the two C-terminal lysine residues cause the formation of diverse single β-strand conformations, and the final self-assembled nanostructures and handedness are determined by the twisting direction and degree of single β-strands. This work not only lays a useful foundation for the fabrication of diverse peptide nanostructures by manipulating the chirality of specific residues but also provides a framework for predicting the supramolecular structures and handedness of peptide assemblies from single molecule conformations.

AB - Peptide assemblies are promising nanomaterials, with their properties and technological applications being highly hinged on their supramolecular architectures. Here, how changing the chirality of the terminal charged residues of an amphiphilic hexapeptide sequence Ac-I4K2-NH2 gives rise to distinct nanostructures and supramolecular handedness is reported. Microscopic imaging and neutron scattering measurements show thin nanofibrils, thick nanofibrils, and wide nanotubes self-assembled from four stereoisomers. Spectroscopic and solid-state nuclear magnetic resonance (NMR) analyses reveal that these isomeric peptides adopt similar anti-parallel β-sheet secondary structures. Further theoretical calculations demonstrate that the chiral alterations of the two C-terminal lysine residues cause the formation of diverse single β-strand conformations, and the final self-assembled nanostructures and handedness are determined by the twisting direction and degree of single β-strands. This work not only lays a useful foundation for the fabrication of diverse peptide nanostructures by manipulating the chirality of specific residues but also provides a framework for predicting the supramolecular structures and handedness of peptide assemblies from single molecule conformations.

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KW - molecular chirality

KW - nanofibrils

KW - nanotubes

KW - polar residues

KW - supramolecular handedness

KW - theoretical calculations

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Controlling 1D Nanostructures and Handedness by Polar Residue Chirality of Amphiphilic Peptides

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