Literature DB >> 22475325

Cationic spacer arm design strategy for control of antimicrobial activity and conformation of amphiphilic methacrylate random copolymers.

Edmund F Palermo1, Satyavani Vemparala, Kenichi Kuroda.   

Abstract

Antimicrobial and hemolytic activities of amphiphilic random copolymers were modulated by the structure of the cationic side chain spacer arms, including 2-aminoethylene, 4-aminobutylene, and 6-aminohexylene groups. Cationic amphiphilic random copolymers with ethyl methacrylate (EMA) comonomer were prepared with a range of comonomer fractions, and the library of copolymers was screened for antimicrobial and hemolytic activities. Copolymers with 4-aminobutylene cationic side chains showed an order of magnitude enhancement in their antimicrobial activity relative to those with 2-aminoethylene spacer arms, without causing adverse hemolysis. When the spacer arms were further elongated to hexylene, the copolymers displayed potent antimicrobial and hemolytic activities. The 4-aminobutylene side chain appears to be the optimal spacer arm length for maximal antimicrobial potency and minimal hemolysis, when combined with hydrophobic ethylmethacrylate in a roughly 70/30 ratio. The copolymers displayed relatively rapid bactericidal kinetics and broad-spectrum activity against a panel of Gram-positive and Gram-negative bacteria. The effect of the spacer arms on the polymer conformation in the membrane-bound state was investigated by molecular dynamics simulations. The polymer backbones adopt an extended chain conformation, parallel to the membrane surface. A facially amphiphilic conformation at the membrane surface was observed, with the primary ammonium groups localized at the lipid phoshophate region and the nonpolar side chains of EMA comonomers buried in the hydrophobic membrane environment. This study demonstrates that the antimicrobial activity and molecular conformation of amphiphilic methacrylate random copolymers can be modulated by adjustment of cationic side chain spacer arms.

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Year:  2012        PMID: 22475325     DOI: 10.1021/bm300342u

Source DB:  PubMed          Journal:  Biomacromolecules        ISSN: 1525-7797            Impact factor:   6.988


  31 in total

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4.  Molecular design, structures, and activity of antimicrobial peptide-mimetic polymers.

Authors:  Haruko Takahashi; Edmund F Palermo; Kazuma Yasuhara; Gregory A Caputo; Kenichi Kuroda
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Review 5.  Amphiphilic macromolecules on cell membranes: from protective layers to controlled permeabilization.

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7.  Self-assembled cationic amphiphiles as antimicrobial peptides mimics: Role of hydrophobicity, linkage type, and assembly state.

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8.  An Investigation into Rigidity-Activity Relationships in BisQAC Amphiphilic Antiseptics.

Authors:  Renee C Kontos; Stephanie A Schallenhammer; Brian S Bentley; Kelly R Morrison; Javier A Feliciano; Julia A Tasca; Anna R Kaplan; Mark W Bezpalko; W Scott Kassel; William M Wuest; Kevin P C Minbiole
Journal:  ChemMedChem       Date:  2018-12-18       Impact factor: 3.466

9.  Decoupling the Functional Roles of Cationic and Hydrophobic Groups in the Antimicrobial and Hemolytic Activities of Methacrylate Random Copolymers.

Authors:  Hamid Mortazavian; Leanna L Foster; Rajani Bhat; Shyrie Patel; Kenichi Kuroda
Journal:  Biomacromolecules       Date:  2018-10-26       Impact factor: 6.988

10.  Two interdependent mechanisms of antimicrobial activity allow for efficient killing in nylon-3-based polymeric mimics of innate immunity peptides.

Authors:  Michelle W Lee; Saswata Chakraborty; Nathan W Schmidt; Rajan Murgai; Samuel H Gellman; Gerard C L Wong
Journal:  Biochim Biophys Acta       Date:  2014-04-14
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