Self‐Assembly of Differently Shaped Protein–Polymer Conjugates through Modification of the Bioconjugation Site

Huang, Aaron; Olsen, Bradley D.

doi:10.1002/marc.201500744

Cited by 12 publications

(22 citation statements)

References 31 publications

(61 reference statements)

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“…These proteins were then used to synthesize bioconjugates via site-specific bioconjugation chemistry using thiol-maleimide coupling (Scheme 1). In addition to these six conjugates, structural data of conjugates of reduced charged Sso7d (rcSso7d), 45 human heart myoglobin (HMb), 44 human immunoglobulin G (IgG), 43 mCherry, 51 and EGFP 52 from other studies were compared to identify trends in how the properties of each protein affects the quality of ordering and general self-assembly behavior of protein–polymer bioconjugates. For the six bioconjugates in this study as well as the referenced bioconjugates, the weight fraction of protein and polymer was kept roughly symmetric except in the case of IgG, where the mass of the protein was too large to form a symmetric conjugate.…”

Section: Results and Discussionmentioning

confidence: 99%

“…These C ODT values are considerably higher than for EGFP and mCherry, which have C ODT values as low as 30 wt %. 40,51,52 Additionally, 3 of the proteins exhibit ODT temperatures ( T ODT values) at concentrations of 40 and 45 wt %: HTPI transitions from the disordered phase to a hexagonal phase, and both DFPaseN and BSA transition from disordered to lamellar phases. These transitions are likely due to desolvation of the polymer resulting in phase separation as the water partitions to the protein domains.…”

Section: Results and Discussionmentioning

confidence: 99%

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Predicting Protein–Polymer Block Copolymer Self-Assembly from Protein Properties

et al. 2019

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Protein–polymer bioconjugate self-assembly has attracted a great deal of attention as a method to fabricate protein nanomaterials in solution and the solid state. To identify protein properties that affect phase behavior in protein–polymer block copolymers, a library of 15 unique protein-b-poly(N-isopropylacrylamide) (PNIPAM) copolymers comprising 11 different proteins was compiled and analyzed. Many attributes of phase behavior are found to be similar among all studied bioconjugates regardless of protein properties, such as formation of micellar phases at high temperature and low concentration, lamellar ordering with increasing temperature, and disordering at high concentration, but several key protein-dependent trends are also observed. In particular, hexagonal phases are only observed for proteins within the molar mass range 20–36 kDa, where ordering quality is also significantly enhanced. While ordering is generally found to improve with increasing molecular weight outside of this range, most large bioconjugates exhibited weaker than predicted assembly, which is attributed to chain entanglement with increasing polymer molecular weight. Additionally, order–disorder transition boundaries are found to be largely uncorrelated to protein size and quality of ordering. However, the primary finding is that bioconjugate ordering can be accurately predicted using only protein molecular weight and percentage of residues contained within β sheets. This model provides a basis for designing protein–PNIPAM bioconjugates that exhibit well-defined self-assembly and a modeling framework that can generalize to other bioconjugate chemistries.

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Section: Results and Discussionmentioning

confidence: 99%

Section: Results and Discussionmentioning

confidence: 99%

Predicting Protein–Polymer Block Copolymer Self-Assembly from Protein Properties

et al. 2019

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“…Recently, we have reported the topological effects on the self-assembly of globular protein-coil protein fusion proteins 22,39 and protein polymer block copolymers. 40 In this work, changing the elastin-like polypeptide (ELP) tails from the N to C termini of mCherry has no impact on the ability to form well-ordered nanostructures. 39 On the other hand, a bola fusion protein, which has two ELP tails on both N and C termini of mCherry, showed a lower order-disorder transition concentration than the linear fusion protein, which has one EPL tail on the N terminus of mCherry.…”

Section: Introductionmentioning

confidence: 90%

“…However, differences in domain spacing were observed, suggesting changes in protein orientation within the lamellar phase. 40 The protein-polymer block copolymer approach is a promising approach to expand the capability to obtain topological designs and functional designs. To obtain well-defined bioconjugates, site-specific modification is one of the most important tools.…”

Section: Introductionmentioning

confidence: 99%

Topology effects on protein–polymer block copolymer self-assembly

Suguri

Olsen

2019

Polym. Chem.

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“…Therefore, affinity approaches (biotin-streptavidin binding, cofactor reconstitution) ( Boerakker et al, 2006 ), or site-selective covalent polymer conjugation are used. As usual, the conjugation approach affects the stability of the micelle and the protein orientation ( Huang and Olsen, 2016 ). In a recent example, enzyme-poly( N -(2-hydroxypropyl) methacrylate)) (PHPMA) conjugates were self-assembled through polymerization-induced coassembly (PICA) approach.…”

Section: Enzyme-polymer Hybridsmentioning

confidence: 99%

Tunable Polymeric Scaffolds for Enzyme Immobilization

Rodriguez‐Abetxuko

Sánchez-deAlcázar

Muñumer

et al. 2020

Front. Bioeng. Biotechnol.

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The number of methodologies for the immobilization of enzymes using polymeric supports is continuously growing due to the developments in the fields of biotechnology, polymer chemistry, and nanotechnology in the last years. Despite being excellent catalysts, enzymes are very sensitive molecules and can undergo denaturation beyond their natural environment. For overcoming this issue, polymer chemistry offers a wealth of opportunities for the successful combination of enzymes with versatile natural or synthetic polymers. The fabrication of functional, stable, and robust biocatalytic hybrid materials (nanoparticles, capsules, hydrogels, or films) has been proven advantageous for several applications such as biomedicine, organic synthesis, biosensing, and bioremediation. In this review, supported with recent examples of enzyme-protein hybrids, we provide an overview of the methods used to combine both macromolecules, as well as the future directions and the main challenges that are currently being tackled in this field.

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Self‐Assembly of Differently Shaped Protein–Polymer Conjugates through Modification of the Bioconjugation Site

Cited by 12 publications

References 31 publications

Predicting Protein–Polymer Block Copolymer Self-Assembly from Protein Properties

Predicting Protein–Polymer Block Copolymer Self-Assembly from Protein Properties

Topology effects on protein–polymer block copolymer self-assembly

Tunable Polymeric Scaffolds for Enzyme Immobilization

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