Precise protein assembly of array structures

Yang, Guang; Wu, Libin; Chen, Guosong; Jiang, Ming

doi:10.1039/c6cc04190f

Cited by 28 publications

(19 citation statements)

References 74 publications

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“…[1] In nature, proteins self-assemble into different structures in nano-or micrometer scale with highly ordered patterns, [2] forexample, virus capsids, [3] actin filaments, [4] microtubules, [5] and bacteria S-layers [6] .T hese attractive structures have stimulated strong motivation for programming proteins into various nanoobjects, [7] including oligomers, [8a,b] zero-dimensional (0D) nanocages, [8b,c] 1D fibers, [9] nanotubes, [10] 2D nanosheets, [11] nanorings, [12] and 3D frameworks [13] . [1] In nature, proteins self-assemble into different structures in nano-or micrometer scale with highly ordered patterns, [2] forexample, virus capsids, [3] actin filaments, [4] microtubules, [5] and bacteria S-layers [6] .T hese attractive structures have stimulated strong motivation for programming proteins into various nanoobjects, [7] including oligomers, [8a,b] zero-dimensional (0D) nanocages, [8b,c] 1D fibers, [9] nanotubes, [10] 2D nanosheets, [11] nanorings, [12] and 3D frameworks [13] .…”

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“…These results introduce an easy strategy to control the assembly structure and dimension, whichcould shed light on controlled protein assembly.Proteins are remarkable building blocks for the fabrication of different functional materials because of their enormous structural complexity and intrinsic functions. [1] In nature, proteins self-assemble into different structures in nano-or micrometer scale with highly ordered patterns, [2] forexample, virus capsids, [3] actin filaments, [4] microtubules, [5] and bacteria S-layers [6] .T hese attractive structures have stimulated strong motivation for programming proteins into various nanoobjects, [7] including oligomers, [8a,b] zero-dimensional (0D) nanocages, [8b,c] 1D fibers, [9] nanotubes, [10] 2D nanosheets, [11] nanorings, [12] and 3D frameworks [13] .…”

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Highly Ordered Self‐Assembly of Native Proteins into 1D, 2D, and 3D Structures Modulated by the Tether Length of Assembly‐Inducing Ligands

et al. 2017

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In nature, proteins self-assemble into various structures with different dimensions. To construct these nanostructures in laboratories, normally proteins with different symmetries are selected. However, most of these approaches are engineering-intensive and highly dependent on the accuracy of the protein design. Herein, we report that a simple native protein LecA assembles into one-dimensional nanoribbons and nanowires, two-dimensional nanosheets, and three-dimensional layered structures controlled mainly by small-molecule assembly-inducing ligands RnG (n=1, 2, 3, 4, 5) with varying numbers of ethylene oxide repeating units. To understand the formation mechanism of the different morphologies controlled by the small-molecule structure, molecular simulations were performed from microscopic and mesoscopic view, which presented a clear relationship between the molecular structure of the ligands and the assembled patterns. These results introduce an easy strategy to control the assembly structure and dimension, which could shed light on controlled protein assembly.

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Highly Ordered Self‐Assembly of Native Proteins into 1D, 2D, and 3D Structures Modulated by the Tether Length of Assembly‐Inducing Ligands

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“…Recently, hierarchical organization of protein assemblies into array structures has gained the interest of researchers. Electrostatic interactions, metal-ligand interactions, molecular recognition and protein-protein interactions are known to drive this hierarchical self-assembly [77] and CCMV [78], P22 [79] and ferritin [80] nanocages have been incorporated in crystalline structures and metamaterials. Combining this hierarchical organization with protein nanocage-based nanoreactors can give rise to array structures that incorporate various catalytic functions with high level of positional control.…”

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Self-assembled nanoreactors based on peptides and proteins

Timmermans

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2018

Current Opinion in Colloid & Interface Science

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“…However, most natural proteins could be treated as colloidal particles without canonical interacting motifs for precise organization . To achieve regular protein packing structures in the laboratory, intensively engineered proteins with well‐selected geometry and symmetry are always employed to control protein–protein interactions (PPIs), which highly depend on the accuracy of the protein design .…”

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confidence: 99%

Highly Ordered Self‐Assembly of Native Proteins into 1D, 2D, and 3D Structures Modulated by the Tether Length of Assembly‐Inducing Ligands

et al. 2017

Self Cite

View full text Add to dashboard Cite

In nature, proteins self‐assemble into various structures with different dimensions. To construct these nanostructures in laboratories, normally proteins with different symmetries are selected. However, most of these approaches are engineering‐intensive and highly dependent on the accuracy of the protein design. Herein, we report that a simple native protein LecA assembles into one‐dimensional nanoribbons and nanowires, two‐dimensional nanosheets, and three‐dimensional layered structures controlled mainly by small‐molecule assembly‐inducing ligands RnG (n=1, 2, 3, 4, 5) with varying numbers of ethylene oxide repeating units. To understand the formation mechanism of the different morphologies controlled by the small‐molecule structure, molecular simulations were performed from microscopic and mesoscopic view, which presented a clear relationship between the molecular structure of the ligands and the assembled patterns. These results introduce an easy strategy to control the assembly structure and dimension, which could shed light on controlled protein assembly.

show abstract

Precise protein assembly of array structures

Cited by 28 publications

References 74 publications

Highly Ordered Self‐Assembly of Native Proteins into 1D, 2D, and 3D Structures Modulated by the Tether Length of Assembly‐Inducing Ligands

Highly Ordered Self‐Assembly of Native Proteins into 1D, 2D, and 3D Structures Modulated by the Tether Length of Assembly‐Inducing Ligands

Self-assembled nanoreactors based on peptides and proteins

Highly Ordered Self‐Assembly of Native Proteins into 1D, 2D, and 3D Structures Modulated by the Tether Length of Assembly‐Inducing Ligands

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