In vivo pharmacodynamic study of contezolid acefosamil, a prodrug of contezolid for oral and intravenous administration.

OBJECTIVES: Contezolid acefosamil is a novel O-acyl phosphoramidate prodrug of contezolid. In the current study, we aimed to systemically evaluate the efficacy of contezolid acefosamil against infections caused by multiple Gram-positive pathogens, and compare the efficacy of the prodrug by oral and intravenous administrations. METHODS: The in vivo pharmacodynamic efficacy of contezolid acefosamil was evaluated in mouse models of systemic (with five S. aureus, three S. pneumoniae and two S. pyogenes bacterial isolates) and thigh (with two S. aureus isolates) infections using linezolid as the reference agent. RESULTS: In both models, contezolid acefosamil administrated either orally or intravenously, demonstrated high antibacterial efficacy similar to linezolid, and the antibacterial efficacy of oral and intravenous contezolid acefosamil were comparable. CONCLUSIONS: The high aqueous solubility and great efficacy of contezolid acefosamil support its clinical development as an injectable and oral antibiotic suitable for serious Gram-positive infections.

Spectroscopic identification of the low-lying electronic states of S2 molecule.

As is well-known, the S2 molecule is a ubiquitous intermediate in the combustion, atmosphere, and interstellar space. The six low-lying bound states of S2 have been characterized via photoelectron velocity map imaging and a high-level multi-reference configuration interaction method with the Davidson correction. Spectroscopic constants have been extracted by fitting the potential energy curves extrapolated to the complete basis set limit with a series of Dunning's correlation-consistent basis sets: aug-cc-pV(Q, 5)Z. The calculated spectroscopic parameters well reproduce the experimental results in this work. On the basis of the theoretical calculations, Franck-Condon simulations are performed to assign six adjacent electronic states, especially for three higher overlapping electronic states (c1Σu -, A'3Δu, and A3Σu +). The dissociation energy De of the S2 - is evaluated to be 4.111 (4) eV in this work, in agreement with the theoretical prediction (4.056 eV).

A comparative study on the bond features in CO, CS, and PbS.

Covalent and noncovalent interactions dominate most compounds in the condensed phase and gas phase. For a classical diatomic molecule CO, it is usually regarded as a triple-bond system with one dative bond. In this work, the photoelectron velocity-map imaging spectra of the CS and PbS anions were first measured. The two interactions have been intuitively understood by a comparative investigation of electrostatic potential (ESP) and bond features in CO, CS, and PbS. It is suggested that both electrostatic and dative covalent interactions compete in CO molecules, while dative covalent interaction prevails in CS molecules and electrostatic interaction dominates in PbS molecules. As a consequence, CO has a very small dipole moment (∼0.1 D) compared to the large dipole moment in CS (>1.8 D) and PbS (>4 D). It is indicated that the electron affinity value increases with the increasing dipole moment in the order of CO < CS < PbS. In addition, intriguing ESP with negative bond-ends and positive bond-cylindrical-surface in CO is also revealed by comparing with that in CS and PbS. In the latter, the two molecules present opposite ESP maps. Molecular orbital analyses indicate surprising participation of Pb 5d orbitals in the Pb-S chemical bonding although Pb belongs to main-group elements. Further bond analyses using electron localization function, natural resonance theory, and bond order methods suggest that covalence is dominant in CS and ionicity is a major component in PbS, but somewhere in between for CO molecules. By a comparative study in this work, the CS molecule is also revealed as a promising ligand molecule for the transition-metal coordination chemical synthesis.

Recombinant expression and biochemical characterization of Mycobacterium tuberculosis 3Fe-4S ferredoxin Rv1786.

Ferredoxins are iron-sulfur protein that mediate electron transfer in cytochrome P450 mono-oxygenase (CYP)-related catalytic reactions in a wide variety of organisms. Rv1786 is a putative ferredoxin, encoded by a gene located downstream of the gene encoding CYP143A1 in the Mycobacterium tuberculosis genome. However, the structure and function of Rv1786 have remained unclear. Here, the recombinant Mtb Rv1786 was expressed, purified as a His-tagged form and characterized with [3Fe-4S] clusters as its cofactors using a series of measurements including SDS-PAGE, western blot, UV/Visible, MALDI-TOF/TOF-MS, and electron paramagnetic resonance spectroscopic analysis. Based on the assessments of surface plasmon resonance (SPR) and steady state kinetic assays, Rv1786 was found to be able to couple with both ferredoxin reductase A (FdrA) and flavoprotein reductase A (FprA) as redox partner, but with a stronger binding to FprA and a better coupling activity to FdrA. Preliminary structural and biochemical characterization of Mtb Rv1786 as a redox partner is presented here.

PRECLINICAL PHARMACOKINETIC ANALYSIS OF (E)-METHYL-4-ARYL-4-OXABUT-2-ENOATE, A NOVEL SER/THR PROTEIN KINASE B INIBITOR, IN RATS.

(E)-Methyl-4-aryl-4-oxabut-2-enoate, designated YH-8, is a novel Serflhr protein kinase B (PknB) inhibitor, which is designed for the treatment of tuberculosis. The aim of this study was to investigate the pharmacokinetics, bioavailability, tissue distribution and excretion characteristics of YH-8 in rats and study its plasma protein binding in vitro. The pharmacokinetic properties were examined after intravenously injected YH-8 at 10 and 20 mg/kg and oral administrated YH-8 at 50, 100 and 200 mg/kg to rats. The concentrations of YH-8 in plasma were determined with LC-MS/MS, with a liquid-liquid extraction. The tissue distribution and urinary, fecal and -biliary excretion patterns of YH-8 were investigated following a single oral dosing of 100 mg/kg. The plasma protein binding rates of YH-8 were determined using ultra-filtration method. After intra- venous and oral administration, YH-8 showed dose-independent pharmacokinetic characteristics, with T(1/2) of approximately 5.5 h and 7.1 h, respectively. The oral absolute bioavailability of YH-8 was relatively low (about 12%). YH-8 was widely distributed in various tissues and showed substantial deposition in intestine, stomach, liver, lung and kidney. The drug was mainly eliminated via fecal excretion and its binding rate with plasma protein was concentration-dependent. In conclusion, this study as first provided the full pharmacokinetic characteristics of YH-8, which would be helpful for its further development and clinical application.

In vivo antibacterial activity of MRX-I, a new oxazolidinone.

MRX-I is a potent oxazolidinone antibiotic against Gram-positive pathogens, including methicillin-resistant Staphylococcus aureus (MRSA), penicillin-resistant Streptococcus pneumoniae (PRSP), penicillin-intermediate S. pneumoniae (PISP), and vancomycin-resistant enterococci (VRE). In this study, the in vivo efficacy of orally administered MRX-I was evaluated using linezolid as a comparator. MRX-I showed the same or better efficacy than linezolid in both systemic and local infection models against the tested strains.

Vibrationally resolved photoelectron imaging of Au3H(-).

We report a combined photoelectron velocity map imaging spectroscopy and density functional theory investigation on the Au3H(-) anion. Transition between the anionic electronic ground state and the neutral electronic ground state is revealed. Vibrationally resolved spectra were recorded at two different photon energies, providing a wealth of spectroscopic information for the electronic ground state of the Au3H. Franck-Condon simulations of the ground-state transition are carried out to assist in the assignment of the vibrationally resolved spectra. The electron affinity and vertical detachment energy of Au3H are measured to be 2.548 ± 0.001 and 2.570 ± 0.001 eV, respectively. Three stretching vibrational modes are determined to be activated upon photodetachment, with the frequencies of 2100 ± 100, 177 ± 10, and 96 ± 10 cm(-1).

Photoelectron imaging and theoretical study on nascent hydrogen bond network in microsolvated clusters of Au- (CH3OH)n (n = 1-5).

We first demonstrate the photoelectron spectroscopic evidence of the transition of two competitive solvation patterns in the Au(-)(CH3OH)n (n = 1-5) clusters. Quantum chemical calculations have been carried out to characterize the geometric structures, energy properties and hydrogen-bonded patterns, and to aid the spectral assignment. It has been found that the nonconventional hydrogen bonds dominate the small clusters (n = 1 and 2), whereas the conventional hydrogen bonds play more and more important role from n = 2 to n = 5. This finding provides concrete hydrogen bond network evolution of Au(-) surrounded by methanol molecules.

An investigation into low-lying electronic states of HCS2 via threshold photoelectron imaging.

Low-energy photoelectron imaging spectra of HCS2(-) are reported for the first time. Vibrationally resolved photodetachment transitions from the ground state of HCS2(-) to the ground state and low-lying excited states of HCS2 are observed. Combined with the ab intio calculations and Franck-Condon simulations, well-resolved vibrational spectra demonstrate definitive evidence for the resolution of the ground-state and excited states of HCS2 radical in the gaseous phase. The ground state and two low-lying excited states of HCS2 radical are assigned as (2)B2, (2)A2, and (2)A1 states, respectively. The adiabatic electron affinity is determined to be 2.910 ± 0.007 eV. And the term energies of the excited states, T0 = 0.451 ± 0.009 eV and 0.553 ± 0.009 eV, are directly measured from the experimental data, respectively. Angular filtering photoelectron spectra are carried out to assist in the spectral band assignment.

Low-energy photoelectron imaging of HS2 anion.

Low-energy photoelectron imaging of HS2 (-) has been investigated, which provides the vibrational frequencies of the ground state as well as the first excited state of HS2. It allows us to determine more accurate electron affinity of HS2, 1.9080 ± 0.0018 eV. Combined with Frank-Condon simulation, the vibrational features have been unveiled related to S-S stretching and S-S-H bending modes for the ground state and S-S stretching, S-S-H bending, and S-H stretching modes for the first excited state. Photoelectron angular distributions are mainly characteristic of electron detachment from two different molecular orbitals (MOs) in HS2 (-). With the aid of accurate electron affinity value of HS2, corresponding thermochemical quantities can be accessed.

Photoelectron imaging and theoretical study on the structure and chemical binding of the mixed-ligand M(I) complexes, [HMSH]⁻ (M = Cu, Ag, and Au).

We have reported a combined photoelectron imaging and theoretical study on gaseous mixed-ligand M(I) complexes of [HMSH](-) (M = Cu, Ag, and Au). With the aid of Franck-Condon simulations, vibrationally resolved photoelectron spectra yield accurate electron affinities of 3.269(6), 3.669(10), and 3.591(6) eV for [HCuSH], [HAgSH], and [HAuSH], respectively. And low-frequency modes are observed: 368(12) cm(-1) for [HCuSH], 286(12) cm(-1) for [HAgSH], and 327(12) cm(-1) for [HAuSH], respectively. Extensive theoretical calculations are performed to aid in the spectral assignments and the calculated values agree well with the experimental observations. Although the S and H atoms have little discrepancy in electronegativity (2.20 for H and 2.54 for S), distinct bonding properties are demonstrated between H-M and M-S bond. It is revealed that there exists significant ionic bonding between M-S in [HMSH](-) (M = Cu, Ag, and Au), while a gradual transition from ionic behavior between H-Cu in [HCuSH](-) to quite strong covalent bonding between H-Au in [HAuSH](-), supported by a variety of chemical bonding analyses.

On the photoelectron velocity-map imaging of lutetium monoxide anion LuO(-).

We report a combined photoelectron velocity-map imaging spectroscopy and density functional theory investigation on lutetium monoxide anion. Transition between the X (1)Σ(+) anion electronic ground state and the neutral X (2)Σ(+) electronic ground state is observed. Vibrationally resolved spectra were obtained at four different photon energies, providing a wealth of spectroscopic information for the electronic ground states of the anionic lutetium monoxide and corresponding neutral species. Franck-Condon simulations of the ground-state transition are performed to assign vibrational structure in the spectra and to assist in identifying the observed spectral bands. The electronic ground state of LuO(-) is found to have a vibrational frequency of 743 ± 10 cm(-1) and an equilibrium bond length of 1.841 Å. The electron affinity of LuO is measured to be 1.624 ± 0.002 eV. The fundamental frequency of ground-state LuO is estimated to be 839 ± 10 cm(-1).

Structure of Au4(0/-1) in the gas phase: A joint geometry relaxed ab initio calculations and vibrationally resolved photoelectron imaging investigation.

We have combined photoelectron velocity-map imaging spectroscopy and high-level ab initio calculations to elucidate the geometries of Au4 (0/-1). Well-resolved ground-state electronic transition was observed in the photoelectron spectrum of Au4 (-) at 446 nm, leading to more accurate electron affinity and vibrational frequencies for the ground state of the neutral Au4 (-). The pure and vibrationally resolved spectra provide definitive experimental evidence for the resolution of the ground-state gold tetramer in the gaseous phase, with the aid of the ab initio calculations and Franck-Condon simulations. The comprehensive comparisons between the experiment and theoretical calculations suggest that the Y-shaped structure is the global minimum for both the neutral and anionic Au4.

Photoelectron velocity-map imaging spectroscopic and theoretical study on the reactivity of the gold atom toward CH3SH, CH3OH, and H2O.

Photoelectron velocity-map imaging spectroscopy has been used to study the reaction of the anionic gold atom with the HR (R = SCH3, OCH3, OH) molecules. The solvated [Au···HR](-) and inserted [HAuR](-) products have been experimentally observed for R = SCH3, whereas only solvated [Au⋯HR](-) products were found for R = OCH3 and OH. This significant difference in the photoelectron spectra suggests the different reactivity of the Au(-) toward the CH3SH, CH3OH, and H2O molecules. Second order Møller-Plesset perturbation theory and coupled-cluster single double triple excitation calculations have been performed to aid the structural assignment of the spectra and to explore the reaction mechanism. Activation energies for the isomerizations of the solvated structures to the inserted ones in the Au(-)∕Au + HR reactions (R = OCH3 and OH) are predicted to be much higher than those for the Au(-)∕Au + CH3SH reactions, supporting the experimental observation. Theoretical calculations provide the evidence that the intriguing [HAuSCH3](-) product may be formed by the attachment of the electron onto the neutral HAuSCH3 species or the isomerization from the anionic [Au···HSCH3](-) one. These findings should be helpful for understanding the feature that the thiols are able to form the staple motifs, whereas CH3OH and H2O are not.

Toxicokinetic study of melamine in the presence and absence of cyanuric acid in rats.

Several lines of evidence show that the nephrotoxic effect of melamine (MEL) in animals is consistent with combined ingestion of MEL and cyanuric acid (CYA). The aim of the present study was to compare the toxicokinetics of MEL in the presence and absence of CYA, and to elucidate the correlation between toxicity and kinetic properties of MEL. Sprague-Dawley rats were administered a single oral dose of MEL (100 mg kg(-1) ) with or without CYA (100 mg kg(-1) ). Plasma and tissue samples were analyzed by liquid chromatography-tandem mass spectrometric (LC-MS/MS) assay. Significant changes in toxicokinetic parameters of MEL such as lower maximum concentration (7.4 ± 3.5 vs 78.0 ± 11.0 µg ml(-1) ) and area under curve (94.9 ± 53.5 vs 295.1 ± 93.7 µg h ml(-1) ), higher plasma elimination half-life (7.0 ± 3.3 vs 2.5 ± 0.3 h) and volume of distribution (11 505.5 ± 5030.3 vs 1312.7 ± 337.7 ml kg(-1) ), as well as significantly higher concentration of MEL in rat kidney (2.96-274.15 vs < 1 µg g(-1) ) were detected in the CYA co-administration group when compared with MEL alone group (P < 0.05). The differences in kinetic parameters between the two groups meant that CYA co-administration could lower absorption, slow excretion and induce tissue accumulation of MEL, which correlated well with the generation and development of renal toxicity. In conclusion, co-administration with CYA leads to the alteration of the kinetic characteristics of MEL, which provides an additional explanation for renal toxicity.

In vivo antibacterial activity of chinfloxacin, a new fluoroquinolone antibiotic.

OBJECTIVES: To evaluate the in vivo antibacterial efficacy of chinfloxacin, a novel fluoroquinolone, in murine systemic and local infection models. METHODS: The efficacy of chinfloxacin in systemic infection was evaluated in a mouse peritonitis model using isolates of methicillin-susceptible Staphylococcus aureus (MSSA, n = 3), methicillin-resistant Staphylococcus aureus (MRSA; n = 1), penicillin-intermediate Streptococcus pneumoniae (PISP; n = 1), penicillin-resistant S. pneumoniae (PRSP; n = 2), vancomycin-susceptible Enterococcus faecalis (VSE; n = 1), vancomycin-resistant E. faecalis (VRE; n = 2), Escherichia coli (n = 3) and Klebsiella pneumoniae (n = 2). The local infections included mouse pulmonary infections caused by penicillin-susceptible S. pneumoniae (PSSP; n = 1), PRSP (n = 1) and K. pneumoniae (n = 2). RESULTS: In the mouse systemic infection model, chinfloxacin demonstrated potent activity against MSSA [50% effective dose (ED(50)) 2.28-4.15 mg/kg], MRSA (ED(50) 14.75 mg/kg), PISP (ED(50) 6.20 mg/kg), PRSP (ED(50) 3.51-5.03 mg/kg), VSE (ED(50) 25.02 mg/kg), VRE (ED(50) 5.18-15.39 mg/kg), E. coli (ED(50) 1.25-1.90 mg/kg) and K. pneumoniae (ED(50) 2.92-8.28 mg/kg). The therapeutic efficacy of chinfloxacin was generally similar to (P > 0.05) that of moxifloxacin, significantly higher (P < 0.01 or P < 0.05) than that of levofloxacin in Gram-positive isolate infections (MSSA, MRSA, PISP, PRSP, VSE and VRE), and less than that of levofloxacin against E. coli and K. pneumoniae infections (P < 0.01). In the mouse pulmonary infection model, chinfloxacin showed potent activity towards S. pneumoniae (higher than levofloxacin and ciprofloxacin) and K. pneumoniae (lower than levofloxacin and similar to or higher than ciprofloxacin) infections. CONCLUSIONS: The results validated the potent efficacy of chinfloxacin in vivo. The high efficacy of chinfloxacin in murine systemic and local infections warrants investigation of its clinical use.

Photoelectron imaging and theoretical calculations of gold-silver hydrides: comparing the characteristics of Au, Ag and H in small clusters.

Structures and electronic properties of the mixed metal hydride anions AuAgH(-), Au(2)AgH(-), AuAg(2)H(-) and their neutrals are studied using anionic photoelectron imaging and theoretical calculations. The three isomers of AuAgH(-) are determined to be linear and those of AuAgH are determined to have C(s) symmetry. The structures of Au(2)AgH(-), AuAg(2)H(-) and their corresponding neutrals are determined to be planar with C(s) or C(2v) symmetries. The vertical detachment energies (VDEs) and adiabatic detachment energies (ADEs) of these anions are reported. Similar to the homonuclear Au(m)(-) and Ag(n)(-) clusters, the metal hydride anions with an even number of valence electrons have higher VDEs than those with an odd number. Variation of the VDEs of these metal hydride anions with interchange of Au, Ag and H (for example Au(m)Ag(n)(-)→ Au(m-1)Ag(n+ 1)(-), or Au(m-1)Ag(n)H(-)) will be shown to be characterized by the electronegativities of Au, Ag and H. The results presented in this study provide important insights into the similar and different characteristics of these three elements in small clusters.

Vibrationally resolved photoelectron imaging of platinum carbonyl anion Pt(CO)(n)- (n = 1-3): experiment and theory.

Photodetachment of platinum carbonyl anions Pt(CO)(n)(-) (n = 1, 3) had been previously investigated using traditional photoelectron spectroscopy (PES) [G. S. Icking-Konert, H. Handschuh, G. Ganteför, and W. Eberhardt, Phys. Rev. Lett. 76, 1047 (1996); B. Chatterjee, F. A. Akin, C. C. Jarrold, and K. Raghavachari, J. Chem. Phys. 119, 10591 (2003)]. Here, we studied Pt(CO)(n)(-) (n = 1-3) using photoelectron velocity-map imaging method and extensive theoretical calculations. Vibrationally resolved spectra from photoelectron imaging experiments allow determination of the electron affinities of Pt(CO)(n), which are 1.196 ± 0.034, 0.930 ± 0.042, and 1.253 ± 0.032 eV for n = 1, 2, and 3, respectively. Two vibrational progressions are resolved for the ground states of Pt(CO) and Pt(CO)(3), while only one is resolved for that of Pt(CO)(2). The frequencies are determined to be 2089 ± 91 and 581 ± 21 cm(-1) for Pt(CO), 2173 ± 115 cm(-1) for Pt(CO)(2) and 2119 ± 88 and 444 ± 18 cm(-1) for Pt(CO)(3). Results from density functional theory and ab initio calculations agreed well with the experimental observations. The spectra were well reproduced by Franck-Condon fitting on the basis of the optimized geometries and the theoretical frequencies. The well-resolved PES also provided valuable benchmarks for various density functionals (B3LYP, BP86, and PW91PW91) for the platinum carbonyls.

Probing the structural and electronic properties of Ag(n)H(-) (n = 1-3) using photoelectron imaging and theoretical calculations.

Structural and electronic properties of silver hydride cluster anions (Ag(n)H(-); n = 1-3) have been explored by combining the negative ion photoelectron imaging spectroscopy and theoretical calculations. The photoelectron spectrum of AgH(-) exhibits transitions from AgH(- 2)Σ(+) to AgH (1)Σ(+) and AgH (3)Σ(+), with the electron affinity (EA) 0.57(3) eV. For Ag(2)H(-), the only observed transition is from Ag(2)H(-) (C(∞v)) (1)Σ(+) to Ag(2)H (C(2v)) (2)A(') and the electron affinity is 2.56(5) eV. Two obvious electron bands are observed in photoelectron imaging of Ag(3)H(-), which are assigned to the transitions from Ag(3)H(-) (C(2v)-T, which means C(2v) geometry with top site hydrogen) (2)B(2) to Ag(3)H (C(2v)-T) (1)A(1) and Ag(3)H (C(2v)-T) (3)B(2). The electron affinity is determined to be 1.61(9) eV. The Ag-H stretching modes in the ground states of AgH and Ag(2)H are experimentally resolved and their frequencies are measured to be 1710(80) and 1650(100) cm(-1), respectively. Aside from the above EAs and the vibrational frequencies, the vertical detachment energies to all ground states and some excited states of Ag(n)H (n = 1-3) are also obtained. Theoretical calculations reproduce the experimental energies quite well, and the results are used to assign the geometries and electronic states for all related species.

In vitro antibacterial activity of chinfloxacin, a new fluoroquinolone antibiotic.

BACKGROUND: Chinfloxacin is a novel synthetic fluoroquinolone with a structure similar to moxifloxacin. The in vitro activity of chinfloxacin was evaluated in the current study. METHOD: Chinfloxacin was tested against a total of 1,739 clinical isolates representing 23 species using the agar dilution method. Studies of bactericidal activity, including minimum bactericidal concentrations (MBC) and time-kill curve determinations, were conducted according to the recommendations of the Clinical and Laboratory Standards Institute. RESULTS: Minimum inhibitory concentrations (MIC)(50)s and MIC(90)s of chinfloxacin were found to be the same or 2-fold lower than those of moxifloxacin against gram-positive isolates except for Streptococcus pyogenes (against which chinfloxacin showed similar MIC(50) as moxifloxacin but 2-fold higher MIC(90)), and the same as or 2-fold higher than those of moxifloxacin against gram-negative isolates. Chinfloxacin showed potent bactericidal activity with MBC/MIC ratios in the range of 1-2 for almost all the isolates tested. Time-kill curves further demonstrated chinfloxacin as a concentration-dependent bactericidal agent usually effective at concentrations of 2 MIC or higher. CONCLUSION: Chinfloxacin showed similar in vitro activity as moxifloxacin.