Phosphorus-31 NMRspectroscopy is ananalytical chemistry technique that usesnuclear magnetic resonance (NMR) to studychemical compounds that containphosphorus. Phosphorus is commonly found inorganic compounds and coordination complexes (asphosphines), making it useful to measure31- NMR spectra routinely. Solution31P-NMR is one of the more routine NMR techniques because31P has anisotopic abundance of 100% and a relatively highgyromagnetic ratio. The31P nucleus also has aspin of1/2, making spectra relatively easy to interpret. The only other highly sensitive NMR-active nuclei spin1/2 that are monoisotopic (or nearly so) are1H and19F.[1][a]
With a gyromagnetic ratio 40.5% of that for1H,31P-NMR signals are observed near 202 MHz on an 11.7-Tesla magnet (used for 500 MHz1H-NMR measurements). Chemical shifts are typically referenced to 85%phosphoric acid, which is assigned the chemical shift of 0, and appear at positive values (downfield of the standard).[2] Due to the inconsistentnuclear Overhauser effect, integrations are not useful.[2] Most often, spectra are recorded with protonsdecoupled.
31P-NMR spectroscopy is useful to assay purity and to assign structures of phosphorus-containing compounds because these signals are well resolved and often occur at characteristic frequencies. Chemical shifts and coupling constants span a large range but sometimes are not readily predictable. TheGutmann-Beckett method uses Et3PO in conjunction with31P-NMR spectroscopy to assess the Lewis acidity of molecular species.
The ordinary range of chemical shifts ranges from about δ250 to −δ250, which is much wider than typical for1H-NMR. Unlike1H-NMR spectroscopy, but similar to most other nuclei,31P-NMR shifts are primarily not determined by the magnitude of the diamagnetic shielding, but are dominated by the so-called paramagnetic shielding tensor (unrelated toparamagnetism). The paramagnetic shielding tensor, σp, includes terms that describe the radial expansion (related to charge), energies ofexcited states, and bond overlap. Illustrative of the effects lead to big changes in chemical shifts, the chemical shifts of the twophosphate esters (MeO)3PO (δ2.1) and (t-BuO)3PO (δ-13.3). More dramatic are the shifts for phosphine derivatives H3P (δ-240), (CH3)3P (δ-62), (i-Pr)3P (δ20), and (t-Bu)3P (δ61.9).[3]
One-bondcoupling is illustrated by PH3 where J(P,H) is 189 Hz. Two-bond couplings, e.g.PCH are an order of magnitude smaller. The situation for phosphorus-carbon couplings are more complicated since the two-bond couplings are often larger than one-bond couplings. The J(13C,31P) values for triphenylphosphine are respectively −12.5, 19.6, 6.8, and 0.3 for one-, two-, three-, and four-bond couplings.[4]
The convention surrounding31P-NMR (and other nuclei) changed convention in 1975: "The dimensionless scale should be defined as positive in the high frequency (low field) direction."[5] Therefore, note that manuscripts published before 1976 will generally have the opposite sign.
31P-NMR spectroscopy is widely used for studies ofphospholipid bilayers and biological membranes in native conditions. The analysis[6] of31P-NMR spectra of lipids could provide a wide range of information about lipid bilayer packing,phase transitions (gel phase, physiological liquid crystal phase, ripple phases, non bilayer phases), lipid head group orientation/dynamics, and elastic properties of pure lipid bilayer and as a result of binding of proteins and other biomolecules.
In addition, a specific N-H...(O)-P experiment (INEPT transfer using three-bond scalar coupling3JN-P~5 Hz) could provide a direct information about formation ofhydrogen bonds between amine protons of protein to phosphate of lipid headgroups, which is useful in studies of protein/membrane interactions.