Literature DB >> 29642033

Partitioning and Enhanced Self-Assembly of Actin in Polypeptide Coacervates.

Patrick M McCall1, Samanvaya Srivastava2, Sarah L Perry3, David R Kovar4, Margaret L Gardel5, Matthew V Tirrell6.   

Abstract

Biomolecules exist and function in cellular microenvironments that control their spatial organization, local concentration, and biochemical reactivity. Due to the complexity of native cytoplasm, the development of artificial bioreactors and cellular mimics to compartmentalize, concentrate, and control the local physico-chemical properties is of great interest. Here, we employ self-assembling polypeptide coacervates to explore the partitioning of the ubiquitous cytoskeletal protein actin into liquid polymer-rich droplets. We find that actin spontaneously partitions into coacervate droplets and is enriched by up to ∼30-fold. Actin polymerizes into micrometer-long filaments and, in contrast to the globular protein BSA, these filaments localize predominately to the droplet periphery. We observe up to a 50-fold enhancement in the actin filament assembly rate inside coacervate droplets, consistent with the enrichment of actin within the coacervate phase. Together these results suggest that coacervates can serve as a versatile platform in which to localize and enrich biomolecules to study their reactivity in physiological environments.
Copyright © 2018. Published by Elsevier Inc.

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Year:  2018        PMID: 29642033      PMCID: PMC5954293          DOI: 10.1016/j.bpj.2018.02.020

Source DB:  PubMed          Journal:  Biophys J        ISSN: 0006-3495            Impact factor:   4.033


  44 in total

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Journal:  Adv Colloid Interface Sci       Date:  2016-09-06       Impact factor: 12.984

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Authors:  Scott D Hansen; J Bradley Zuchero; R Dyche Mullins
Journal:  Methods Mol Biol       Date:  2013

8.  Selective Uptake and Refolding of Globular Proteins in Coacervate Microdroplets.

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  13 in total

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4.  Charge-Based Separation of Proteins Using Polyelectrolyte Complexes as Models for Membraneless Organelles.

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5.  Therapeutics-how to treat phase separation-associated diseases.

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6.  Temperature-Responsive Peptide-Nucleotide Coacervates.

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7.  Impact of wet-dry cycling on the phase behavior and compartmentalization properties of complex coacervates.

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8.  Drops and fibers - how biomolecular condensates and cytoskeletal filaments influence each other.

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9.  Polyelectrolyte Complex Coacervation across a Broad Range of Charge Densities.

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10.  Sustained enzymatic activity and flow in crowded protein droplets.

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