Literature DB >> 21628584

Structural plasticity of a transmembrane peptide allows self-assembly into biologically active nanoparticles.

Sergey G Tarasov1, Vadim Gaponenko, O M Zack Howard, Yuhong Chen, Joost J Oppenheim, Marzena A Dyba, Sriram Subramaniam, Youngshim Lee, Christopher Michejda, Nadya I Tarasova.   

Abstract

Significant efforts have been devoted to the development of nanoparticular delivering systems targeting tumors. However, clinical application of nanoparticles is hampered by insufficient size homogeneity, difficulties in reproducible synthesis and manufacturing, frequent high uptake in the liver, systemic toxicity of the carriers (particularly for inorganic nanoparticles), and insufficient selectivity for tumor cells. We have found that properly modified synthetic analogs of transmembrane domains of membrane proteins can self-assemble into remarkably uniform spherical nanoparticles with innate biological activity. Self-assembly is driven by a structural transition of the peptide that adopts predominantly a beta-hairpin conformation in aqueous solutions, but folds into an alpha-helix upon spontaneous fusion of the nanoparticles with cell membrane. A 24-amino acid peptide corresponding to the second transmembrane helix of the CXCR4 forms self-assembled particles that inhibit CXCR4 function in vitro and hamper CXCR4-dependent tumor metastasis in vivo. Furthermore, such nanoparticles can encapsulate hydrophobic drugs, thus providing a delivery system with the potential for dual biological activity.

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Year:  2011        PMID: 21628584      PMCID: PMC3116420          DOI: 10.1073/pnas.1014598108

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


  30 in total

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6.  Inhibition of G-protein-coupled receptor function by disruption of transmembrane domain interactions.

Authors:  N I Tarasova; W G Rice; C J Michejda
Journal:  J Biol Chem       Date:  1999-12-03       Impact factor: 5.157

7.  Multistage nanoparticle delivery system for deep penetration into tumor tissue.

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Journal:  Proc Natl Acad Sci U S A       Date:  2011-01-18       Impact factor: 11.205

Review 8.  Drug penetration in solid tumours.

Authors:  Andrew I Minchinton; Ian F Tannock
Journal:  Nat Rev Cancer       Date:  2006-08       Impact factor: 60.716

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  18 in total

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Journal:  Curr Pharmacol Rep       Date:  2016-01-04

2.  The structure of monomeric components of self-assembling CXCR4 antagonists determines the architecture of resulting nanostructures.

Authors:  Youngshim Lee; Yuhong Chen; Nadya I Tarasova; Vadim Gaponenko
Journal:  Nanotechnology       Date:  2011-11-23       Impact factor: 3.874

3.  Biased antagonism of CXCR4 avoids antagonist tolerance.

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Journal:  Sci Signal       Date:  2018-10-16       Impact factor: 8.192

4.  Heteromerization of chemokine (C-X-C motif) receptor 4 with α1A/B-adrenergic receptors controls α1-adrenergic receptor function.

Authors:  Abhishek Tripathi; P Geoff Vana; Tanmay S Chavan; Lioubov I Brueggemann; Kenneth L Byron; Nadya I Tarasova; Brian F Volkman; Vadim Gaponenko; Matthias Majetschak
Journal:  Proc Natl Acad Sci U S A       Date:  2015-03-16       Impact factor: 11.205

Review 5.  Biomaterials via peptide assembly: Design, characterization, and application in tissue engineering.

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Journal:  Acta Biomater       Date:  2021-10-25       Impact factor: 8.947

6.  Regulation of the thrombin/protease-activated receptor 1 axis by chemokine (CXC motif) receptor 4.

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7.  Novel peptide nanoparticle-biased antagonist of CCR3 blocks eosinophil recruitment and airway hyperresponsiveness.

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8.  Characterization of heteromeric complexes between chemokine (C-X-C motif) receptor 4 and α1-adrenergic receptors utilizing intermolecular bioluminescence resonance energy transfer assays.

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Authors:  Xiaoyun Su; Jing Zhang; Roderick I Mackie; Isaac K O Cann
Journal:  PLoS One       Date:  2012-08-27       Impact factor: 3.240

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