Liposome-Mediated Cellular Delivery of Active gp91phox

Background Gp91phox is a transmembrane protein and the catalytic core of the NADPH oxidase complex of neutrophils. Lack of this protein causes chronic granulomatous disease (CGD), a rare genetic disorder characterized by severe and recurrent infections due to the incapacity of phagocytes to kill microorganisms. Methodology Here we optimize a prokaryotic cell-free expression system to produce integral mammalian membrane proteins. Conclusions Using this system, we over-express truncated forms of the gp91phox protein under soluble form in the presence of detergents or lipids resulting in active proteins with a “native-like” conformation. All the proteins exhibit diaphorase activity in the presence of cytosolic factors (p67phox, p47phox, p40phox and Rac) and arachidonic acid. We also produce proteoliposomes containing gp91phox protein and demonstrate that these proteins exhibit activities similar to their cellular counterpart. The proteoliposomes induce rapid cellular delivery and relocation of recombinant gp91phox proteins to the plasma membrane. Our data support the concept of cell-free expression technology for producing recombinant proteoliposomes and their use for functional and structural studies or protein therapy by complementing deficient cells in gp91phox protein.

• Publication year

  2007

• Venue

  PLoS ONE

• Publication date

  2007-09-12

• Fields of study

  Biology, Medicine, Chemistry

• Identifiers
  DOI 10.1371/journal.pone.0000856PMID 17848987PMCID 1955831
• External record

  Open on Semantic Scholar

• Source metadata

  Semantic Scholar, PubMed

• No claims are published for this paper.

• No concepts are published for this paper.

• Chronic granulomatous disease

  2010cited by this paper
• Structural genomics on membrane proteins: comparison of more than 100 GPCRs in 3 expression systems

  2007cited by this paper
• NOX family NADPH oxidases: not just in mammals.

  2007cited by this paper
• Cell-free production of G protein-coupled receptors for functional and structural studies.

  2007cited by this paper
• Regulation of phagocyte NADPH oxidase activity: identification of two cytochrome b558 activation states

  2007cited by this paper
• New insights into the membrane topology of the phagocyte NADPH oxidase: characterization of an anti-gp91-phox conformational monoclonal antibody.

  2007cited by this paper
• Production of membrane proteins using cell–free expression systems

  2007cited by this paper
• Reprint of "Cell-free production of G protein-coupled receptors for functional and structural studies" [J. Struct. Biol. 158 (2007) 482-493].

  2007cited by this paper
• Assessing the antifungal activity, pharmacokinetics, and tissue distribution of amphotericin B following the administration of Abelcet and AmBisome in combination with caspofungin to rats infected with Aspergillus fumigatus.

  2007cited by this paper
• Leu505 of Nox2 is crucial for optimal p67phox‐dependent activation of the flavocytochrome b558 during phagocytic NADPH oxidase assembly

  2007cited by this paper
• Optimizing targeted gene delivery: Chemical modification of viral vectors and synthesis of artificial virus vector systems

  2006cited by this paper
• Analysis of Human Phagocyte Flavocytochrome b558 by Mass Spectrometry*

  2006cited by this paper
• Typical and atypical trafficking pathways of Ad5 penton base recombinant protein: implications for gene transfer

  2006cited by this paper
• Cell‐free expression as an emerging technique for the large scale production of integral membrane protein

  2006cited by this paper
• Deletion Mutagenesis of p22phox Subunit of Flavocytochrome b558

  2006cited by this paper
• Assembly of the phagocyte NADPH oxidase complex: chimeric constructs derived from the cytosolic components as tools for exploring structure‐function relationships

  2006influential reference
• Understanding recombinant expression of membrane proteins.

  2006cited by this paper
• A simple strategy towards membrane protein purification and crystallization.

  2006cited by this paper
• Recent approaches to intracellular delivery of drugs and DNA and organelle targeting.

  2006cited by this paper
• Correction of X-linked chronic granulomatous disease by gene therapy, augmented by insertional activation of MDS1-EVI1, PRDM16 or SETBP1

  2006influential reference
• The C‐terminal flavin domain of gp91phox bound to plasma membranes of granulocyte‐like X‐CGD PLB‐985 cells is sufficient to anchor cytosolic oxidase components and support NADPH oxidase‐associated diaphorase activity independent of cytosolic phospholipase A2 regulation

  2006cited by this paper
• Expression of G protein coupled receptors in a cell-free translational system using detergents and thioredoxin-fusion vectors.

  2005cited by this paper
• Temporal targeting of tumour cells and neovasculature with a nanoscale delivery system

  2005cited by this paper
• Functional expression of eukaryotic membrane proteins in Lactococcus lactis

  2005cited by this paper
• Evaluation of two anti-gp91phox antibodies as immunoprobes for Nox family proteins: mAb 54.1 recognizes recombinant full-length Nox2, Nox3 and the C-terminal domains of Nox1-4 and cross-reacts with GRP 58.

  2005cited by this paper
• Crystallization of a mammalian membrane protein overexpressed in Saccharomyces cerevisiae.

  2005cited by this paper
• Dual Role of Rac in the Assembly of NADPH Oxidase, Tethering to the Membrane and Activation of p67phox

  2004cited by this paper
• Site-Specific Inhibitors of NADPH Oxidase Activity and Structural Probes of Flavocytochrome b: Characterization of Six Monoclonal Antibodies to the p22phox Subunit1

  2004cited by this paper
• Assembly of the phagocyte NADPH oxidase

  2004cited by this paper
• Cell-free synthesis of a functional ion channel in the absence of a membrane and in the presence of detergent.

  2004cited by this paper
• Efficient delivery of DNA to dendritic cells mediated by influenza virosomes.

  2004cited by this paper
• Activation of the flavoprotein domain of gp91phox upon interaction with N-terminal p67phox (1-210) and the Rac complex.

  2004cited by this paper
• In vitro synthesis of fully functional EmrE, a multidrug transporter, and study of its oligomeric state.

  2004cited by this paper
• Chronic granulomatous disease.

  2003cited by this paper
• Changing the Conformation State of Cytochrome b558 Initiates NADPH Oxidase Activation

  2003cited by this paper
• Membrane proteins: functional and structural studies using reconstituted proteoliposomes and 2-D crystals.

  2002cited by this paper
• Exploration of the diaphorase activity of neutrophil NADPH oxidase.

  2002cited by this paper
• The superoxide-generating NADPH oxidase: structural aspects and activation mechanism

  2002influential reference
• NADPH oxidase of Epstein-Barr-virus immortalized B lymphocytes. Effect of cytochrome b(558) glycosylation.

  2001cited by this paper
• Tumor targeting using anti-her2 immunoliposomes.

  2001cited by this paper
• Characterization of the flavoprotein domain of gp91phox which has NADPH diaphorase activity.

  2001influential reference
• Pharmacodynamics of insulin in polyethylene glycol-coated liposomes.

  1999cited by this paper
• Analysis of glycosylation sites on gp91phox, the flavocytochrome of the NADPH oxidase, by site-directed mutagenesis and translation in vitro.

  1997cited by this paper
• Superoxide production by cytochrome b559. Mechanism of cytosol-independent activation.

  1994cited by this paper
• The superoxide-generating system of human neutrophils possesses a novel diaphorase activity. Evidence for distinct regulation of electron flow within NADPH oxidase by p67-phox and p47-phox.

  1994influential reference
• Production of recombinant cytochrome b558 allows reconstitution of the phagocyte NADPH oxidase solely from recombinant proteins.

  1993cited by this paper
• Generation of Superoxide by purified and relipidated cytochrome b 559 in the absence of cytosolic activators

  1993cited by this paper

• Cell-free protein synthesis and vesicle systems for programmable therapeutic manufacturing and delivery

  2025cites this paper
• Delivery of trans-membrane proteins by liposomes; The effect of liposome size and formulation technique on the efficiency of protein delivery.

  2021cites this paper
• Neutrophil: Methods and Protocols

  2020cites this paper
• Cell-Free NADPH Oxidase Activation Assays: A Triumph of Reductionism.

  2020cites this paper
• A new functional membrane protein microarray based on tethered phospholipid bilayers.

  2018cites this paper
• Liposome-chaperoned cell-free synthesis for the design of proteoliposomes: Implications for therapeutic delivery.

  2018cites this paper
• Long-term observational studies of chronic granulomatous disease

  2018cites this paper
• New Tethered Phospholipid Bilayers Integrating Functional G-Protein-Coupled Receptor Membrane Proteins.

  2017cites this paper
• Therapeutic effects of proteoliposomes on X-linked chronic granulomatous disease: proof of concept using macrophages differentiated from patient-specific induced pluripotent stem cells

  2017influential citation
• Functional characterization of p7 viroporin from hepatitis C virus produced in a cell-free expression system.

  2016cites this paper
• Nouveaux modèles d’étude de la Granulomatose Septique Chronique grâce aux cellules souches pluripotentes induites – Application au développement de la thérapie protéique

  2015cites this paper
• Reconstitution of Ion Channels in a Lipid Bilayer in a Microfluidic Device using Cell-Free Protein Synthesis

  2015cites this paper
• CRISPR-mediated genotypic and phenotypic correction of a chronic granulomatous disease mutation in human iPS cells

  2015cites this paper
• Recombinant form of mammalian gp91(phox) is active in the absence of p22(phox).

  2014cites this paper
• Primary immunodeficiency disease (PID) is a disorder caused by an inherited flaw in the immune system. PIDs are mainly seen in children and are characterized by recurrent and severe infections with susceptibility to unusual organisms. The infections

  2014cites this paper
• Neutrophil Methods and Protocols

  2014cites this paper
• Membrane Protein Quality Control in Cell-Free Expression Systems: Tools, Strategies and Case Studies

  2014cites this paper
• Membrane protein synthesis in cell‐free systems: From bio‐mimetic systems to bio‐membranes

  2014cites this paper
• Cell-free expression of GPCRs: the endothelin system

  2014cites this paper
• Recombinant Human Melatonin Receptor MT1 Isolated in Mixed Detergents Shows Pharmacology Similar to That in Mammalian Cell Membranes

  2014cites this paper
• Cell-free NADPH oxidase activation assays: "in vitro veritas".

  2014influential citation
• Modulation de l’activité du flavocytochrome b₅₅₈ : étude fonctionnelle

  2014influential citation
• Co-translational association of cell-free expressed membrane proteins with supplied lipid bilayers

  2013cites this paper
• Recombinant Nox4 cytosolic domain produced by a cell or cell-free base systems exhibits constitutive diaphorase activity.

  2012cites this paper
• Cell-free membrane protein expression for solid-state NMR.

  2012cites this paper
• Functional analysis of membranous Fo-a subunit of F1Fo-ATP synthase by in vitro protein synthesis.

  2012cites this paper
• Characterization of co-translationally formed nanodisc complexes with small multidrug transporters, proteorhodopsin and with the E. coli MraY translocase.

  2012cites this paper
• Développement et applications de protocoles de synthèse in vitro du canal mécanosensible bactérien à large conductance, pour son étude structurale par résonance magnétique nucléaire en phase solide

  2011cites this paper
• New insight into the Nox4 subcellular localization in HEK293 cells: first monoclonal antibodies against Nox4.

  2011cites this paper
• Advances in cell-free protein synthesis for the functional and structural analysis of membrane proteins.

  2011cites this paper
• NADPH oxydase Nox4 : structure/fonction protéomique recombinante et approche immunologique

  2011influential citation
• Characterization of superoxide overproduction by the D-Loop(Nox4)-Nox2 cytochrome b(558) in phagocytes-Differential sensitivity to calcium and phosphorylation events.

  2011cites this paper
• Coupled cell-free synthesis and lipid vesicle insertion of a functional oligomeric channel MscL MscL does not need the insertase YidC for insertion in vitro.

  2011cites this paper
• Characterization of the Cell-penetrating Properties of the Epstein-Barr Virus ZEBRA trans-Activator*

  2010cites this paper
• Binding modules alter the activity of chimeric cellulases: Effects of biomass pretreatment and enzyme source

  2010cites this paper
• Single-step production of functional OEP24 proteoliposomes.

  2010cites this paper
• Expression of functional mammal flavocytochrome b(558) in yeast: comparison with improved insect cell system.

  2010cites this paper
• Production of functional bacteriorhodopsin by an Escherichia coli cell‐free protein synthesis system supplemented with steroid detergent and lipid

  2009cites this paper
• Régulation de l'activité NADPH oxydase phagocytaire : mécanismes moléculaires de la super-activité oxydase du cytochrome b558 D-loopNox4-Nox2

  2009cites this paper
• Production of recombinant proteoliposomes for therapeutic uses.

  2009cites this paper
• Ex Vivo Gene Therapy Approaches for the Treatment of Globoid Cell Leukodystrophy

  2009cites this paper
• Membrane protein expression: no cells required.

  2009cites this paper
• A Bacterial Cell‐Free Expression System to Produce Membrane Proteins and Proteoliposomes: From cDNA to Functional Assay

  2008cites this paper
• Liposomes-mediated delivery of pro-apoptotic therapeutic membrane proteins.

  2008cites this paper
• Training proteoliposomes containing membrane proteins with the aid of a cell-free synthesis system proteic

  2007cites this paper