Nuclear magnetic resonance identification process

Although relaxation measurements have been widely used in nuclear magnetic resonance studies of solid catalysts and adsorbed molecules, they have not found such favor in similar ESR work. Relaxation phenomena, however, do play a very important role in any magnetic resonance experiment, whether or not this aspect of the problem is studied. In fact, the temperature at which most ESR experiments are conducted is dictated by the relaxation process. Furthermore, even qualitative data on relaxation times can be used as supporting evidence in the identification of a paramagnetic species. 

Nuclear magnetic resonance traditionally has had low sensitivity and spectral resolution. It can provide rigorous quantification of analytes, but not accurate qualitative identification. Individual resonances may be sensitive to the chemical and physical environment of the molecule, which then requires appropriate preparation of samples. The process also has little dynamic range, in contrast to GC-MS. 

Control analyses rely on the use of appropriate procedures or measurements assuring the identity of the materials involved in each step of the manufacturing process from receipt of raw materials to delivery of the finished products. NIR spectroscopy is an advantageous alternative to wet chemical methods and instrumental techniques such as IR, Raman and nuclear magnetic resonance (NMR) spectroscopies for positive identification. 

Nuclear magnetic resonance (NMR) spectroscopy is a most effective and significant method for observing the structure and dynamics of polymer chains both in solution and in the solid state [1]. Undoubtedly the widest application of NMR spectroscopy is in the field of structure determination. The identification of certain atoms or groups in a molecule as well as their position relative to each other can be obtained by one-, two-, and three-dimensional NMR. Of importance to polymerization of vinyl monomers is the orientation of each vinyl monomer unit to the growing chain tacticity. The time scale involved in NMR measurements makes it possible to study certain rate processes, including chemical reaction rates. Other applications are isomerism, internal relaxation, conformational analysis, and tautomerism. 

Use of an integrated system incorporating CCC separation, PDA detector, and LC-MS proved to be a valuable tool in the rapid identification of known compounds from microbial extracts.6 This collection of analytical data has enabled us to make exploratory use of advanced data analysis methods to enhance the identification process. For example, from the UV absorbance maxima and molecular weight for the active compound(s) present in a fraction, a list of potential structural matches from a natural products database (e.g., Berdy Bioactive Natural Products Database, Dictionary of Natural Products by Chapman and Hall, etc.) can be generated. Subsequently, the identity of metabolite(s) was ascertained by acquiring a proton nuclear magnetic resonance ( H-NMR) spectrum. 

Several spectroscopic techniques, namely, Ultraviolet-Visible Spectroscopy (UV-Vis), Infrared (IR), Nuclear Magnetic Resonance (NMR), etc., have been used for understanding the mechanism of solvent-extraction processes and identification of extracted species. Berthon et al. reviewed the use of NMR techniques in solvent-extraction studies for monoamides, malonamides, picolinamides, and TBP (116, 117). NMR spectroscopy was used as a tool to identify the structural parameters that control selectivity and efficiency of extraction of metal ions. 13C NMR relaxation-time data were used to determine the distances between the carbon atoms of the monoamide ligands and the actinides centers. The II, 2H, and 13C NMR spectra analysis of the solvent organic phases indicated malonamide dimer formation at low concentrations. However, at higher ligand concentrations, micelle formation was observed. NMR studies were also used to understand nitric acid extraction mechanisms. Before obtaining conformational information from 13C relaxation times, the stoichiometries of the... 

The refinement or creation of new approaches may result in the elimination of existing activities. For example, the structure confirmation of newly synthesized lead compounds traditionally involved an extensive use of nuclear magnetic resonance (NMR). Once reliable LC/MS methodologies became available and their performance was benchmarked, they were soon accepted as an exclusive method for the rapid structure confirmation of lead compounds at an earlier stage of the lead identification process. 

G. J. Lehr, T. L. Barry, G. Petzinger, G. M. Hanna, S. W. Zito, Isolation and identification of process impurities in trimethoprim drug substance by high-performance liquid chromatography, atmospheric pressure chemical ionization liquid chro-matography/mass spectrometry and nuclear magnetic resonance spectroscopy, J. Pharm. Biomed. Anal. 19 (1999), 373-389. 

This multidisciplinary team approach toward impurity identification was successfully applied to the identification of this impurity. Each and every discipline played a very important role. Without SPE enrichment to remove the drug substance from the impurities, the impurity could not be purified by preparative HPLC. The novel acidic degradation study of the impurity provided very valuable information of the structure of the impurity. Mass spectrometry and nuclear magnetic resonance spectroscopy were the ultimate tools in this structure elucidation. Furthermore, the formation mechanisms were concluded by a careful examination of the process. 

All phases of analytical development are ideally supported by chemical separation techniques such as HPLC, TLC, GC, SFC, and CE. HPLC continues to be the primary method of analysis throughout the pharmaceutical development process. Although HPLC is limited in its ability to separate more than 15-20 components in a single analysis, and variations in columns and instrumentation manufacturer to manufacturer complicate transfer of methods, HPLC can readily be implemented to meet ICH requirements for method performance. For early-phase methods, HPLC can be coupled dynamically to mass and nuclear magnetic resonance spectrometers to facilitate the identification of unknown impurities. In later phases, HPLC can be implemented in a fully automated format as a high-throughput method for release and stability testing. 

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