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Featured researches published by Adam O. Barden.


Inorganic Chemistry | 2008

Metal-assisted in situ formation of a tridentate acetylacetone ligand for complexation of fac-Re(CO)3+ for radiopharmaceutical applications.

Paul D. Benny; Glenn A. Fugate; Adam O. Barden; Jennifer E. Morley; Elsa Silva-Lopez; Brendan Twamley

Reaction of [NEt4]2[ReBr3(CO)3] with 2,4-pentanedione (acac) yields a complex of the type fac-Re(acac)(OH2)(CO)3 (1) under aqueous conditions. 1 was further reacted with a monodentate ligand (pyridine) to yield a fac-Re(acac)(pyridine)(CO)3 complex (2). Complex 1 was found to react with primary amines to generate a Schiff base (imine) in aqueous solutions. When a mixed-nitrogen donor bidentate ligand, 2-(2-aminoethyl)pyridine, that has different coordination affinities for fac-Re(acac)(OH2)(CO)3 was utilized, a unique tridentate ligand was formed in situ utilizing a metal-assisted Schiff base formation to yield a complex fac-Re(CO)3(3[(2-phenylethyl)imino]-2-pentanone) (3). Tridentate ligand formation was found to occur only with the Re-coordinated acac ligand. Reactions of acac with fac-Re(CO)3Br(2-(2-aminoethyl)pyridine) (4) or a mixture of [NEt4]2[ReBr3(CO)3], acac, and 2-(2-aminoethyl)pyridine did not yield the formation of complex 3 in water.


Journal of the American Chemical Society | 2017

Single-Protein Tracking Reveals That NADPH Mediates the Insertion of Cytochrome P450 Reductase into a Biomimetic of the Endoplasmic Reticulum

Carlo Barnaba; Michael J. Martinez; Evan Taylor; Adam O. Barden; James A. Brozik

Cytochrome P450 reductase (CPR) is the redox partner for most human cytochrome P450 enzymes. It is also believed that CPR is an integral membrane protein exclusively. Herein, we report that, contrary to this belief, CPR can exist as a peripheral membrane protein in the absence of NADPH and will transition to an integral membrane protein in the presence of stoichiometric amounts of NADPH or greater. All experiments were performed in a solid-supported cushioned lipid bilayer that closely matched the chemical composition of the human endoplasmic reticulum and served as an ER biomimetic. The phase characteristics and fluidity of the ER biomimetic was characterized with fluorescence micrographs and temperature-dependent fluorescence recovery after photobleaching. The interactions of CPR with the ER biomimetic were directly observed by tracking single CPR molecules using time-lapse single-molecule fluorescence imaging and subsequent analysis of tracks. These studies revealed dramatic changes in diffusion coefficient and the degree of partitioning of CPR as a function of NADPH concentration.


Journal of Physical Chemistry B | 2016

Substrate Dependent Native Luminescence from Cytochromes P450 3A4, 2C9, and P450cam.

Carlo Barnaba; Sara C. Humphreys; Adam O. Barden; Jeffrey P. Jones; James A. Brozik

Metalloporphyrin containing proteins, such as cytochrome P450, play a key role in biological systems. The spectroscopic properties of metalloporphyrins have been a subject of intense interest and intense debate for over 50 years. Iron-porphyrins are usually believed to be nonfluorescent. Herein we report that, contrary to this belief, cytochrome P450 heme groups luminesce with enough intensity to be of use in the characterization of these enzymes. To confirm that the emission is from the heme, we destroyed the heme by titration with cumene hydroperoxide and measured the changes in emission upon titration with compounds known to bind to the distal face of the heme in two human cytochrome P450 enzymes, known as CYP3A4 and CYP2C9. The titration curves gave spectral dissociation constants that were not significantly different from those reported using the Soret UV/vis absorbance changes. We have tentatively assigned the broad luminescence at ∼500 nm to a (1)ππ* → gs fluorescence and the structured luminescence above 600 nm to a (3)ππ* → gs phosphorescence. These assignments are not associated with the Q-band, and are in violation of Kashas rule. To illustrate the utility of the emission, we measured spectral dissociation constants for testosterone binding to P450 3A4 in bilayers formed on glass coverslips, a measurement that would be very difficult to make using absorption spectroscopy. Complementary experiments were carried out with water-soluble P450cam.


Chemistry and Physics of Lipids | 2014

Conditions for liposome adsorption and bilayer formation on BSA passivated solid supports

Elsa Silva-Lopez; Lance E. Edens; Adam O. Barden; David Keller; James A. Brozik

Planar solid supported lipid membranes that include an intervening bovine serum albumen (BSA) cushion can greatly reduce undesirable interactions between reconstituted membrane proteins and the underlying substrate. These hetero-self-assemblies reduce frictional coupling by shielding reconstituted membrane proteins from the strong surface charge of the underlying substrate, thereby preventing them from strongly sticking to the substrate themselves. The motivation for this work is to describe the conditions necessary for liposome adsorption and bilayer formation on these hetero-self-assemblies. Described here are experiments that show that the state of BSA is critically important to whether a lipid bilayer is formed or intact liposomes are adsorbed to the BSA passivated surface. It is shown that a smooth layer of native BSA will readily promote lipid bilayer formation while BSA that has been denatured either chemically or by heat will not. Atomic force microscopy (AFM) and fluorescence microscopy was used to characterize the surfaces of native, heat denatured, and chemically reduced BSA. The mobility of several zwitterionic and negatively charged lipid combinations has been measured using fluorescence recovery after photobleaching (FRAP). From these measurements diffusion constants and percent recoveries have been determined and tabulated. The effect of high concentrations of beta-mercaptoethanol (β-ME) on liposome formation as well as bilayer formation was also explored.


Bioorganic & Medicinal Chemistry Letters | 2013

Near native binding of a fluorescent serotonin conjugate to serotonin type 3 receptors.

Elsa Silva-Lopez; Adam O. Barden; James A. Brozik

Described is the synthesis of 5-hydroxytryptamine-tetramethylrhodamine (5HT*); an indole nitrogen linked fluorescent conjugate of serotonin. Through a series fluorescence quenching experiments and experiments in the presence of a known competitive antagonist (Granisetron), it was shown that 5HT* specifically binds to purified homo-pentameric type-3 human serotonin receptors (5HT(3A)). The measured dissociation constant and Hill coefficient are K(d) = 83 ± 3 nM and n = 3.1 ± 0.3, respectively which is indicative of multi-ligand binding and cooperativity similar to that of unconjugated serotonin.


Neuropharmacology | 2015

Tracking individual membrane proteins and their biochemistry: The power of direct observation.

Adam O. Barden; Adam S. Goler; Sara C. Humphreys; Samaneh Tabatabaei; Martin Lochner; Marc-David Ruepp; Thomas Jack; Jonathan Simonin; Andrew J. Thompson; Jeffrey P. Jones; James A. Brozik


Biophysical Journal | 2017

Single Protein Tracking of P450-Reductase in an Endoplasmic Reticulum Biomimetic Reveals a NADPH Dependent Interaction with the Membrane

James A. Brozik; Carlo Barnaba; Adam O. Barden; Linda Agyen; Sean L. Sheridan


Biophysical Journal | 2017

Single Molecule Kinetic Measurements and Hidden Markov Models for P2X1 Receptors

James A. Brozik; Adam O. Barden; Ashish Bhattari; Brian N. Webb; Andrew J. Thompson


The FASEB Journal | 2015

Deconvoluting the Dance: Cytochrome P450 Interaction Mapping via Super-Resolution Imaging

Sara C. Humphreys; Adam O. Barden; Carlo Barnaba; James A. Brozik; Jeffrey P. Jones


Biophysical Journal | 2015

Super-Resolution Imaging and Single Particle Tracking of Serotonin 5HT3A Receptor in Biomimetic Membranes

Adam O. Barden; Adam S. Goler; James A. Brozik

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James A. Brozik

Washington State University

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Carlo Barnaba

Washington State University

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Jeffrey P. Jones

Washington State University

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Sara C. Humphreys

Washington State University

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Elsa Silva-Lopez

Washington State University

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Adam S. Goler

Washington State University

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Ashish Bhattari

Washington State University

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Brian N. Webb

Washington State University

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