Nitrogen isotopic analyses by isotope-ratio-monitoring gas chromatography / mass spectrometry

Amino acids containing natural-abundance levels of ¹⁵N were derivatized and analyzed isotopically using a technique in which individual compounds are separated by gas chromatography, combusted on-line, and the product stream sent directly to an isotope-ratio mass spectrometer. For samples of N₂ gas, standard deviations of ratio measurement were better than 0.1‰ (Units for δ are parts per thousand or per million (‰).) for samples larger than 400 pmol and better than 0.5‰ for samples larger than 25 pmol (0.1‰ ¹⁵N is equivalent to 0.00004 atom % ¹⁵N). Results duplicated those of conventional, batchwise analyses to within 0.05‰. For combustion of organic compounds yielding CO₂/N₂ ratios between 14 and 28, in particular for N-acetyl n-propyl derivatives of amino acids, δ values were within 0.25‰ of results obtained using conventional techniques and standard deviations were better than 0.35‰. Pooled data for measurements of all amino acids produced an accuracy and precision of 0.04 and 0.23‰, respectively, when 2 mnol of each amino acid was injected on column and 20% of the stream of combustion products was delivered to the mass spectrometer.     

The convergent syntheses of pyrazinyl and quinoxalinyl phenylmethanones from 2-lithio pyrazines and quinoxalines

Pyrazines and quinoxalines bearing 2-substituents that direct ortho metalation reacted with lithium 2,2,6,6-tetramethylpiperidide to produce 2-substituted-3-lithiopyrazines and quinoxalines. These lithio reagents reacted with N-methoxy-N-methylbenzamide to give good to moderate yields of 3-substituted pyrazinyl or quinoxalinylphenylmethanones. The 3-methylthio substituents of some ketone products were oxidized to methylsulfonyl groups that were susceptible to nucleophilic displacement.     

Transient absorption spectra of 2-hydroxybenzophenone photostabilizers

Transient absorption spectra (400–600 nm) of 2-hydroxybenzophenone and the methyl methacrylate copolymer of 2-hydroxy, 3-allyl, 4,4'-dimethoxybenzophenone following 355 nm excitation (7–480 ps delay) are reported. A short-lived, 435 nm transient (τ ≈ 10 ps in CH₂Cl₂) for both molecules is assigned to the lowest excited singlet before internal proton transfer. Weaker, broad T-T absorption is observed after 480 ps.     

The Combination of Gas Chromatography With Mass Spectrometry

Abstract

The coupling of the techniques of gas chromatography and mass spectrometry has provided the chemist with one of his most powerful analytical methods. The analysis of such diverse substances as fuels, air pollutants, food flavors, smokes, protein hydrolyzates, pesticides, lipid extracts, etc. may all require the separation and identification of the components of extremely complex mixtures.     

Assessment of angiogenesis: implications for ultrasound imaging

In this paper, the fundamentals of tumor angiogenesis and the implications for ultrasound imaging will be described. Twenty-eight athymic nude mice were implanted with the human melanoma cell lines DB-1 or MW-9 (14 mice/group). Ultrasound contrast agents were injected in the tail veins. Power Doppler and pulse inversion harmonic imaging (PI-HI) was performed (in real time and intermittently). Ultrasound results were compared to immunohistochemical stains for endothelial cells (CD31), vascular endothelial growth factor (VEGF), and cyclooxygenase-2 (COX-2). Linear regression analysis indicated statistically significant correlations between percent area stained with COX-2 and with VEGF relative to power Doppler (p<0.05) and intermittent PI-HI (p<0.05) measures of tumor neovascularity in the MW-9 and the DB-1 mice, respectively. Preliminary results from a human trial of the anti-angiogenic drug Angiostatin (Entremed, Rockville, MD) showed tumor volumes increased in two patients, while the vascularity remained virtually unchanged. Conversely, in three patients with diminished tumor volumes vascularity increased by 38%. In conclusion, contrast enhanced ultrasound imaging of tumor neovascularity may provide noninvasive markers of angiogenesis and may become a useful tool for monitoring anti-angiogenic therapies in vivo.     

Surface-enhanced vibrational investigation of adsorbed analgesics

Adsorption properties of acetylsalicylic acid (AA), ibuprofen and acetaminophen deposited from volatile solvents with varying protic/aprotic properties on vacuum-evaporated silver films were characterized using surface-enhanced infrared absorption (SEIRA) and surface-enhanced Raman spectroscopy (SERS). SERS preferentially enhances monolayer Raman shifts, while SEIRA can enhance the infrared absorbance of the monolayer and multilayers. To our best knowledge, this is the first reported study of these molecules using a combination of SERS/SEIRA. SERS revealed that AA and ibuprofen adsorbed ionically in monolayers, independent of the deposition solvents used in the process. SEIRA experiments showed that AA multilayers condensed molecularly using a deposition solvent with polar bonds. However, when an alkane deposition solvent with non-polar bonds such as n-heptane was used, AA adsorbed as acetylsalicylate ions in the first few multilayers, while ibuprofen always adsorbed as the free acid in the multilayer. These ionization trends depend upon the affinity of AA and ibuprofen for the underlying silver film. TPD experiments on silver powders further demonstrated that ibuprofen affinity for silver was less than AA. Furthermore, SEIRA indicated that acetaminophen adsorbed as multilayers of metastable polymorphs using protic or polar aprotic deposition solvents. Protic deposition solvents gave higher quality SERS spectra of an acetaminophen monolayer in comparison to polar aprotic deposition solvents. Such studies could find significant applications in biochemical and nanotechnology processes such as drug delivery, catalysis, and tissue engineering and will contribute to the understanding of the impact and fate of analgesics released into the environment.