Cutting-edge LC–MS/MS applications in clinical mass spectrometry: Focusing on analysis of drugs and metabolites

In recent years, liquid chromatography with tandem mass spectrometry (LC–MS/MS) has become a fundamental technology in clinical practice. In Japan, the LC–MS/MS system is used in many large hospitals. It has become popular among pharmacists and laboratory technicians. LC–MS/MS has some advantages in terms of accuracy, speed, and comprehensiveness compared to conventional automated chemical testing equipment. However, LC–MS/MS is by no means a universal method, and it is necessary to understand its characteristics before using it. In the field of therapeutic drug monitoring (TDM), there is an issue with linearity in comprehensive measurement; however, ion-abundance adjustment methods, such as in-source collision-induced dissociation, have been proposed as a solution to this problem. The development of a biomarker analysis includes search, identification, and quantification, and it is necessary to select an appropriate mass spectrometric method for each step. In this paper, we review cutting-edge technologies that can expand the performance of LC–MS/MS in the clinical field and consider current issues and future prospects.     

Homogeneous poly(L‐lactic acid)/chitosan blended films

This work reports an optimized and simple methodology for the preparation of poly(L‐lactic) acid/chitosan (CHT) blends by solvent casting based on the use of a common solvent: hexafluor‐2‐propanol. Films with different component fractions were successfully prepared and did not show visible phase separation. Such biodegradable films have potential to be used in distinct biomedical and environmental applications. The composition effect on film wettability and morphology was investigated by contact angle measurements and scanning electron microscopy. Swelling measurements were also conducted. The composition effect on their thermal properties was analyzed by differential scanning calorimetry. It was found that crystallization is almost suppressed for CHT fractions above 50%. The film miscibility as a function of their composition was evaluated by optical microscopy and Fourier transform infrared spectroscopy imaging. These results evidenced the good miscibility at the microscopic level of the blends. The viscoelastic behavior of the developed films was also studied for the first time by dynamical mechanical analysis (DMA) in an unconventional way: their mechanical properties were measured while they were immersed in gradient compositions of water/ethanol mixtures. This allowed to analyze the glass transition dynamics of the CHT fraction, which would not be possible with conventional DMA tests. DMA temperature scans were also conducted. Copyright © 2014 John Wiley & Sons, Ltd.     

Multifunctionalized CMCht/PAMAM Dendrimer Nanoparticles Modulate the Cellular Uptake by Astrocytes and Oligodendrocytes in Primary Cultures of Glial Cells

The efficiency of the treatments involving CNS disorders is commonly diminished by the toxicity, reduced stability and lack of targeting of the administered neuroactive compounds. In this study, we have successfully multifunctionalized CMCht/PAMAM dendrimer nanoparticles by coupling the CD11b antibody and loading MP into the nanoparticles. The modification of the new antibody‐conjugated nanoparticles was confirmed by S‐TEM observation and ¹H NMR and FTIR spectroscopy. Cytotoxicity assays revealed that the conjugates did not affect the viability of both primary cultures of glial and microglial cells. Trace analyses of FITC‐labelled nanoparticles revealed that the uptake of antibody‐conjugated nanoparticles was conserved in microglial cells but significantly decreased in astrocytes and oligodendrocytes. Thus, this study demonstrates that antibody conjugation contributes to a modulation of the internalization of these nanocarriers by different cell types, which might be of relevance for specific targeting of CNS cell populations.

     

Iron complexes of (e)- and (z)-1,2-dichlorodisilenes

Novel disilene-iron complexes [(E)- (1E) and (Z)-(eta2-R3SiClSi=SiClSiR3)Fe(CO)4 (1Z), SiR3 = tBu2MeSi] were synthesized by the reaction of the corresponding tetrachlorodisilane with an excess amount of K2Fe(CO)4, and the structures of 1E and 1Z were determined by X-ray crystallography. These complexes constitute not only the first transition-metal complexes with E,Z-isomerism but also the first complexes with halogen-substituted disilene ligands. The initial formation of 1Z during the synthetic reaction and the slow one-way isomerization of 1Z to 1E are rationalized by the intervention of the corresponding silylene complex (R3SiCl2Si)(R3Si)Si=Fe(CO)4.     

Promotion effects of optical antipodes on the formation of helical fibrils: chiral perfluorinated gelators

A chiral gelator, RR- or SS-N,N'-diperfluorooctanoyl-1,2-diaminocyclohexane, gelated racemic 2-butanol. The gel was most stable at the racemic mixture, its stability lowered with the increase in the optical purity of the gelator. Notably, characteristic helically coiled fibrils were formed in the narrow region of enantiomer excess (ee = 0.2-0.4). Promotion effects of the antipodal enantiomers are proposed.     

Long tethers binding redox centers to polymer backbones enhance electron transport in enzyme "Wiring" hydrogels

A redox hydrogel with an apparent electron diffusion coefficient (D(app)) of (5.8 +/- 0.5) x 10(-)(6) cm(2) s(-)(1) is described. The order of magnitude increase in D(app) relative to previously studied redox hydrogels results from the tethering of redox centers to the backbone of the cross-linked redox polymer backbone through 13 atom spacer arms. The long and flexible tethers allow the redox centers to sweep electrons from large-volume elements and to collect electrons of glucose oxidase efficiently. The spacer arms make the collection of electrons from glucose oxidase so efficient that glucose is electrooxidized already at -0.36 V versus Ag/AgCl, the reversible potential of the redox potential of the FAD/FADH(2) centers of the enzyme at pH 7.2. The limiting current density of 1.15 mA cm(-)(2) is reached at a potential as low as -0.1 V versus Ag/AgCl. The novel redox center of the polymer is a tris-dialkylated N,N'-biimidazole Os(2+/3+) complex. Its redox potential, -0.195 V versus Ag/AgCl, is 0.8 V reducing relative to that of Os(bpy)(2+/3+), its 2,2'-bipyridine analogue.     

Oxygen is electroreduced to water on a "wired" enzyme electrode at a lesser overpotential than on platinum

The first enzyme-based catalyst that is superior to platinum in the four-electron electroreduction of oxygen to water is reported. The smooth Pt cathode reached half and 90% of the mass transport-limited current density at respective overpotentials of -0.4 and -0.58 V in 0.5 M sulfuric acid, and only at even higher overpotentials in pH 7.2 phosphate buffer. In contrast, the smooth "wired" bilirubin oxidase cathode reached half and 90% of the mass transport-limited current density at respective overpotentials as low as -0.2 and -0.25 V. The mass transport-limited current density for the smooth "wired" enzyme cathode in PBS was twice that with smooth Pt in 0.5 M sulfuric acid. Under 1 atm O2 pressure, O2 was electroreduced to water on a polished carbon cathode, coated with the "wired" BOD film, in pH 7.2 saline buffer (PBS) at an overpotential of -0.31 V at a current density of 9.5 mA cm-2. At the same overpotential, the current density of the polished platinum cathode in 0.5 M H2SO4 was 16-fold lower, only 0.6 mA cm-2.     

Marked difference in singlet-chemiexcitation efficiency between syn-anti isomers of spiro[1,2-dioxetane-3,1′-dihydroisobenzofuran] for intramolecular charge-transfer-induced decomposition

Spiro[1,2-dioxetane-3,1′-dihydroisobenzofuran] syn-3 bearing a hydroxy group at the 6-position (as a model syn-rotamer of parent dioxetane 4 bearing a 3-hydroxyphenyl group) and its isomer anti-3 (as a model anti-rotamer of 4) were synthesized. When these spiro-dioxetanes were treated with tetrabutylammonium fluoride (TBAF) in DMSO, anti-3 emitted light with high efficiency (Φ^CL = 0.41), while the respective value for syn-3 was only 1/10 for anti-3. This significant difference in Φ^CL between syn-3 and anti-3 was attributed to the difference in their singlet-chemiexcitation efficiencies.     

Synthesis of 3alpha,7alpha,14alpha-trihydroxy-5beta-cholan-24-oic acid: a potential primary bile acid in vertebrates

A method for the synthesis of 3alpha,7alpha,14alpha-trihydroxy-5beta-cholan-24-oic acid which is a possible candidate of bile acid metabolite in vertebrates was developed. The principal reactions involved were 1). stereoselective remote-hydroxylation of methyl ursodeoxycholate diacetate with dimethyldioxirane, 2). site-selective protection at C-3 by tert-butyldimethylsilylation of the resulting 3alpha,7alpha,14alpha-trihydroxy ester, 3). oxidation of the diol with pyridinium dichromate adsorbed on activated alumina, 4). stereoselective reduction of the 7-ketone with zinc borohydride, and 5). cleavage of the protecting group at C-3 with p-toluenesulfonic acid. A facile elimination of the 14alpha-hydroxy group under an acidic or neutral condition is also described. The synthetic reference compound is now available for comparison with unidentified biliary bile acids detected in vertebrate bile.