Spatial Distribution and Solvent Polarity-Triggered Release of a Polypeptide Incorporated into Invertible Micellar Assemblies

Yanxiong Pan; Oksana Zholobko; Hui Li; Jing Jin; Jinlian Hu; Bingcan Chen; Andriy Voronov; Zhongyu Yang

doi:10.1021/acsami.9b22435

Spatial Distribution and Solvent Polarity-Triggered Release of a Polypeptide Incorporated into Invertible Micellar Assemblies

ACS Appl Mater Interfaces. 2020 Mar 11;12(10):12075-12082. doi: 10.1021/acsami.9b22435. Epub 2020 Feb 26.

Authors

Yanxiong Pan¹, Oksana Zholobko², Hui Li³, Jing Jin⁴, Jinlian Hu⁵, Bingcan Chen³, Andriy Voronov², Zhongyu Yang¹

Affiliations

¹ Department of Chemistry and Biochemistry, North Dakota State University, Fargo, North Dakota 58102, United States.
² Coatings and Polymeric Materials Department, North Dakota State University, Fargo, North Dakota 58108, United States.
³ Department of Plant Sciences, North Dakota State University, Fargo, North Dakota 58102, United States.
⁴ Magnetic Resonance Center, Boston College, Chestnut Hill, Massachusetts 02467, United States.
⁵ Institute of Textiles and Clothing, The Hong Kong Polytechnic University, Hong Kong 999077, China.

PMID: 32057221
DOI: 10.1021/acsami.9b22435

Abstract

Extracting, stabilizing, or delivering biomacromolecules such as proteins and peptides in organic phases have potential applications in biocatalysis, protein extraction, and food antioxidation. However, most current delivery/stabilization platforms face various limitations such as protein/peptide molecular size, platform stability/reusability, and/or potential damage to the cargos. A potential solution to these problems is micellar self-assemblies from amphiphilic invertible polymers, which have recently been demonstrated to be powerful as molecular hosts to deliver both small molecular drugs and functional polypeptides in the aqueous phase. To better understand the function of biomacromolecules and predict the usefulness of the formed invertible micellar assemblies (IMAs) as biomacromolecular hosts in organic phases, it is critical to characterize the spatial distribution, structure, and dynamics of biomacromolecules in the IMA including those upon release. However, the background signals of the IMAs limit the application of most peptide characterization approaches. In this work, we overcome the technical barriers by using site-directed spin labeling electron paramagnetic resonance to probe the spatial arrangement and release of a model, the hemagglutinin (HA) peptide, in the IMAs formed from two different amphiphilic invertible polymers. By site-specifically probing three residues along the peptide chain, for the first time, we depict the possible spatial distribution of HA within the IMAs. By triggering the disassembly of the IMAs with a thermodynamically good solvent (in this study, acetone), we detailed the stability of IMAs in toluene and the peptide release conditions once the polarity of the medium changes. Our findings are important for the application of peptides/proteins at the polar-nonpolar interface or using this interface to extract or deliver biomacromolecules. Our work also demonstrates the power of SDSL-EPR on probing peptide or micelle dynamics, which can be generalized to understand proteins or other biomacromolecules in micellar polymer assemblies in varied applications.

Keywords: EPR spectroscopy; invertible micellar assemblies; peptide dynamics; peptide release; site-directed spin labeling.

MeSH terms

Drug Delivery Systems / methods*
Electron Spin Resonance Spectroscopy
Hemagglutinins / chemistry
Hydrophobic and Hydrophilic Interactions
Micelles*
Peptides / chemistry*
Peptides / pharmacokinetics
Polymers / chemistry
Solvents / chemistry*
Surface-Active Agents / chemistry*

Substances

Hemagglutinins
Micelles
Peptides
Polymers
Solvents
Surface-Active Agents