Literature DB >> 17911256

Control of electrostatic interactions between F-actin and genetically modified lysozyme in aqueous media.

Lori K Sanders1, Wujing Xian, Camilo Guáqueta, Michael J Strohman, Chuck R Vrasich, Erik Luijten, Gerard C L Wong.   

Abstract

The aim for deterministic control of the interactions between macroions in aqueous media has motivated widespread experimental and theoretical work. Although it has been well established that like-charged macromolecules can aggregate under the influence of oppositely charged condensing agents, the specific conditions for the stability of such aggregates can only be determined empirically. We examine these conditions, which involve an interplay of electrostatic and osmotic effects, by using a well defined model system composed of F-actin, an anionic rod-like polyelectrolyte, and lysozyme, a cationic globular protein with a charge that can be genetically modified. The structure and stability of actin-lysozyme complexes for different lysozyme charge mutants and salt concentrations are examined by using synchrotron x-ray scattering and molecular dynamics simulations. We provide evidence that supports a structural transition from columnar arrangements of F-actin held together by arrays of lysozyme at the threefold interstitial sites of the actin sublattice to marginally stable complexes in which lysozyme resides at twofold bridging sites between actin. The reduced stability arises from strongly reduced partitioning of salt between the complex and the surrounding solution. Changes in the stability of actin-lysozyme complexes are of biomedical interest because their formation has been reported to contribute to the persistence of airway infections in cystic fibrosis by sequestering antimicrobials such as lysozyme. We present x-ray microscopy results that argue for the existence of actin-lysozyme complexes in cystic fibrosis sputum and demonstrate that, for a wide range of salt conditions, charge-reduced lysozyme is not sequestered in ordered complexes while retaining its bacterial killing activity.

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Year:  2007        PMID: 17911256      PMCID: PMC2042150          DOI: 10.1073/pnas.0705898104

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


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  25 in total

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2.  Improved siRNA delivery efficiency via solvent-induced condensation of micellar nanoparticles.

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Review 3.  Polyelectrolyte properties of filamentous biopolymers and their consequences in biological fluids.

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Authors:  Hui Wei; Zidong Wang; Jiong Zhang; Stephen House; Yi-Gui Gao; Limin Yang; Howard Robinson; Li Huey Tan; Hang Xing; Changjun Hou; Ian M Robertson; Jian-Min Zuo; Yi Lu
Journal:  Nat Nanotechnol       Date:  2011-01-30       Impact factor: 39.213

5.  Plasmid-templated shape control of condensed DNA-block copolymer nanoparticles.

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Review 6.  Modulation of toll-like receptor signaling by antimicrobial peptides.

Authors:  Ernest Y Lee; Michelle W Lee; Gerard C L Wong
Journal:  Semin Cell Dev Biol       Date:  2018-02-12       Impact factor: 7.727

7.  Polycation induced actin bundles.

Authors:  Andras Muhlrad; Elena E Grintsevich; Emil Reisler
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Authors:  Nathan W Schmidt; Fan Jin; Roberto Lande; Tine Curk; Wujing Xian; Calvin Lee; Loredana Frasca; Daan Frenkel; Jure Dobnikar; Michel Gilliet; Gerard C L Wong
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10.  Two interdependent mechanisms of antimicrobial activity allow for efficient killing in nylon-3-based polymeric mimics of innate immunity peptides.

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