Comprehensive analysis of drugs of abuse in urine using disposable pipette extraction.

The extraction of basic, acidic, and neutral drugs of abuse from a low volume of urine (0.2 mL) using disposable pipette extraction (DPX) is described. DPX is a solid-phase extraction device that uses loosely contained sorbent inside a pipette tip fitted with a screen. This device provides faster extraction times because conditioning steps are not required. In this study, the DPX used a modified divinyl benzene sorbent containing both cation-exchange and reversed-phase mechanisms that facilitates the retention of basic and acidic/neutral drugs, respectively. With this device, a comprehensive method of analysis was developed for a diverse group of drugs and drug classes in urine including amphetamines, opiates, cocaine and its metabolites, tetrahydrocannabinol metabolite, tricyclic antidepressants, meperidine, methadone, and phencyclidine. Recoveries of the majority of drugs analyzed were 90% or greater with relative standard deviations of less than 10%. Additional validation involved the analysis of urine specimens previously analyzed by a local forensic toxicology laboratory.

MALDI-TOF/TOF CID study of poly(alpha-methylstyrene) fragmentation reactions.

MALDI-TOF/TOF CID experiments are reported for hydroxylated poly(alpha-methylstyrene) precursor ions (PAMS: m/z 1,445.9 (n = 10), 2,036.3 (n = 15), 2,626.7 (n = 20), 3,217.1 (n = 25), and 3,807.5 (n = 30), where the number of repeat units n corresponds to the oligomer mass numbers). The influences of structure, molecular weight, and kinetic energy on degradation mechanisms were examined to test the generality of our multi-chain fragmentation model developed for polystyrene. Our results indicate that poly(alpha-methylstyrene) free radicals are formed initially through multiple chain breaks and subsequently undergo a variety of depolymerization reactions to yield predominantly monomer and dimer species; the intensity of each species depends on the effective kinetic energy selected for the CID process. Each depolymerization mechanism is presented in detail with experimental and computational data to justify/rationalize the process and its kinetic energy dependence. These processes show the complex interrelationships between the various pathways along with preferred production of tertiary radicals, which suppresses the appearance of primary radicals. Additionally, Py-GC/MS experimental data are presented to allow a comparison of the multimolecular free radical reactions in pyrolysis with the unimolecular fragmentation reactions of MS/MS.

Matrix-assisted laser desorption/ionization-time-of-flight/time-of-flight collision-induced dissociation study of poly(p-phenylenediamine terephthalamide) fragmentation reactions.

MALDI-TOF/TOF collision-induced dissociation (CID) experiments are reported on model poly(p-phenylenediamine terephthalamide) (PPD-T) polymers, revealing a variety of synthesis reaction products. Diamine-terminated oligomers were the major product of synthesis using excess amine, and di-carboxylic acid oligomers were the major product for excess acid. Structures of major reaction products were confirmed by CID fragmentation studies, along with detailed studies of MS/MS decomposition pathways. Apparent fracture of the phenylcarbonyl bond was the major fragmentation pathway (independent of end groups), resulting from initial NHCO bond cleavage with subsequent CO loss. Hydrogen-transfer reactions play an important role in fragmentation, involving both cross-chain abstraction of NH hydrogen and long-range H-transfer. End-group and main-chain modifications produce fingerprint CID fragmentation patterns that can be used to identify end groups and branching patterns; the structure of an unanticipated synthesis product was established using CID. The effect of synthesis conditions on polymer composition was studied using the analysis of variance, specifically, the amine-to-acid ratio used and post-synthesis addition of CaO. Of particular interest is oligomer end-group modification by the solvent (N-methyl pyrrolidone) induced by addition of CaO.

A MALDI-TOF MS study of oligomeric poly(m-phenyleneisophthalamide).

MALDI-TOF MS was used to study the end-group distribution of a series of poly(m-phenyleneisophthalamide) oligomers which were synthesized using various mole percent ratios of diamine to diacid chloride (90:10, 80:20, 70:30, 60:40, 50:50, 40:60, 30:70, 20:80, and 10:90) to clarify results obtained in previous work published in this journal. Oligomers synthesized with excess diamine or excess diacid chloride were found to contain abundances of amine or carboxylate end groups, respectively, as expected. Oligomers synthesized with equal molar ratios of reactants produced cyclic species which were also found in a previous publication as an oligomer in commercially produced, high molecular mass Nomex.