RESUMEN
We present novel means to hyperpolarize deuterium nuclei in 13CD2 groups at cryogenic temperatures. The method is based on cross-polarization from 1H to 13C and does not require any radio-frequency fields applied to the deuterium nuclei. After rapid dissolution, a new class of long-lived spin states can be detected indirectly by 13C NMR in solution. These long-lived states result from a sextet-triplet imbalance (STI) that involves the two equivalent deuterons with spin I = 1. An STI has similar properties as a triplet-singlet imbalance that can occur in systems with two equivalent I = 12 spins. Although the lifetimes TSTI are shorter than T1(Cz), they can exceed the life-time T1(Dz) of deuterium Zeeman magnetization by a factor of more than 20.
RESUMEN
The development of biocompatible hyperpolarized media is a crucial step towards application of hyperpolarization in vivo. This article describes the achievement of 1% hyperpolarization of 3-amino-1,2,4-triazine protons in water using the parahydrogen induced polarization technique based on signal amplification by reversible exchange (SABRE). Polarization was achieved in less than 1 min.
RESUMEN
Hyperpolarization methods are used in NMR to overcome its inherent sensitivity problem. Herein, the biologically relevant target nicotinamide is polarized by the hyperpolarization technique signal amplification by reversible exchange. We illustrate how the polarization transfer field, and the concentrations of parahydrogen, the polarization-transfer-catalyst and substrate can be used to maximize signal amplification by reversible exchange effectiveness by reference to the first-order spin system of this target. The catalyst is shown to be crucial in this process, first by facilitating the transfer of hyperpolarization from parahydrogen to nicotinamide and then by depleting the resulting polarized states through further interaction. The 15 longitudinal one, two, three and four spin order terms produced are rigorously identified and quantified using an automated flow apparatus in conjunction with NMR pulse sequences based on the only parahydrogen spectroscopy protocol. The rates of build-up of these terms were shown to follow the order four~three > two > single spin; this order parallels their rates of relaxation. The result of these competing effects is that the less-efficiently formed single-spin order terms dominate at the point of measurement with the two-spin terms having amplitudes that are an order of magnitude lower. We also complete further measurements to demonstrate that (13)C NMR spectra can be readily collected where the long-lived quaternary (13)C signals appear with significant intensity. These are improved upon by using INEPT. In summary, we dissect the complexity of this method, highlighting its benefits to the NMR community and its applicability for high-sensitivity magnetic resonance imaging detection in the future.
Asunto(s)
Análisis de Inyección de Flujo/instrumentación , Hidrógeno/química , Espectroscopía de Resonancia Magnética/instrumentación , Microquímica/instrumentación , Técnicas de Sonda Molecular/instrumentación , Niacinamida/análisis , Niacinamida/química , Diseño de Equipo , Análisis de Falla de EquipoRESUMEN
Hyperpolarization produces nuclear spin polarization that is several orders of magnitude larger than that achieved at thermal equilibrium thus providing extraordinary contrast and sensitivity. As a parahydrogen induced polarization (PHIP) technique that does not require chemical modification of the substrate to polarize, Signal Amplification by Reversible Exchange (SABRE) has attracted a lot of attention. Using a prototype parahydrogen polarizer, we polarize two drugs used in the treatment of tuberculosis, namely pyrazinamide and isoniazid. We examine this approach in four solvents, methanol-d4, methanol, ethanol and DMSO and optimize the polarization transfer magnetic field strength, the temperature as well as intensity and duration of hydrogen bubbling to achieve the best overall signal enhancement and hence hyperpolarization level.
Asunto(s)
Antituberculosos/química , Isoniazida/química , Espectroscopía de Resonancia Magnética/métodos , Pirazinamida/química , Campos Electromagnéticos , Hidrógeno/química , SolventesRESUMEN
While the characterization of materials by NMR is hugely important in the physical and biological sciences, it also plays a vital role in medical imaging. This success is all the more impressive because of the inherently low sensitivity of the method. We establish here that [Ir(H)(2)(IMes)(py)(3)]Cl undergoes both pyridine (py) loss as well as the reductive elimination of H(2). These reversible processes bring para-H(2) and py into contact in a magnetically coupled environment, delivering an 8100-fold increase in (1)H NMR signal strength relative to non-hyperpolarized py at 3 T. An apparatus that facilitates signal averaging has been built to demonstrate that the efficiency of this process is controlled by the strength of the magnetic field experienced by the complex during the magnetization transfer step. Thermodynamic and kinetic data combined with DFT calculations reveal the involvement of [Ir(H)(2)(η(2)-H(2))(IMes)(py)(2)](+), an unlikely yet key intermediate in the reaction. Deuterium labeling yields an additional 60% improvement in signal, an observation that offers insight into strategies for optimizing this approach.
Asunto(s)
Compuestos Heterocíclicos/química , Hidrógeno/química , Iridio/química , Catálisis , Espectroscopía de Resonancia Magnética , Magnetismo , Modelos MolecularesRESUMEN
The phosphido-substituted triruthenium cluster Ru(3)(CO)(9)(mu-H)(micro-PPh(2)) is shown to react with H(2) to form the trihydride cluster Ru(3)(CO)(9)(H)(mu-H)(2)(mu-PPh(2)), which undergoes a number of re-arrangement reactions on heating to yield other phosphido-substituted triruthenium clusters. In the presence of alkyne substrates, heating the system leads to catalytic hydrogenation via CO loss and the formation of a Ru(3)(eta(2)-PhC[double bond, length as m-dash]CHPh)(CO)(8)(micro-H)(PHPh(2)) resting state, in a reaction affected by the polarity of the solvent. No mononuclear fragments are observed in the catalytic transformation, confirming directly that the phosphido ligand is able to exert a stabilising influence on the cluster core.
RESUMEN
Reaction of [RhCl(PPh3)2]2 with parahydrogen revealed that the binuclear dihydride [Rh(H)2(PPh3)2mu-Cl)2Rh(PPh3)2] and the tetrahydride complex [Rh(H)2(PPh3)2(mu-Cl)]2 are readily formed. While magnetisation transfer from free H2 into both the hydride resonances of the tetrahydride and [Rh(H)2Cl(PPh3)3] is observable, neither transfer into [Rh(H)2(PPh3)2(mu-Cl)2Rh(PPh3)2] nor transfer between the two binuclear complexes is seen. Consequently [Rh(H)2(PPh3)2(mu-Cl)]2 and [Rh(H)2(PPh3)2(mu-Cl)2Rh(PPh3)2] are not connected on the NMR timescale by simple elimination or addition of H2. The rapid exchange of free H2 into the tetrahydride proceeds via reversible halide bridge rupture and the formation of [Rh(H)2(PPh3)2(mu-Cl)RhCl(H)2(PPh3)2]. When these reactions are examined in CD2Cl2, the formation of the solvent complex [Rh(H)2(PPh3)2(mu-Cl)2Rh(CD2Cl2)(PPh3)] and the deactivation products [Rh(Cl)(H)PPh3)2(mu-Cl)(mu-H)Rh(Cl)(H)PPh3)2] and [Rh(Cl)(H)(CD2Cl2)(PPh3)(mu-Cl)(mu-H)Rh(Cl)(H)PPh3)2] is indicated. In the presence of an alkene and parahydrogen, signals corresponding to binuclear complexes of the type [Rh(H)2(PPh3)2(mu-Cl)(2)(Rh)(PPh3)(alkene)] are detected. These complexes undergo intramolecular hydride interchange in a process that is independent of the concentration of styrene and catalyst and involves halide bridge rupture, followed by rotation about the remaining Rh-Cl bridge, and bridge re-establishment. This process is facilitated by electron rich alkenes. Magnetisation transfer from the hydride ligands of these complexes into the alkyl group of the hydrogenation product is also observed. Hydrogenation is proposed to proceed via binuclear complex fragmentation and trapping of the resultant intermediate [RhCl(H)2PPh3)2] by the alkene. Studies on a number of other binuclear dihydride complexes including [(H)(Cl)Rh(PMe3)2(mu-H)(mu-Cl)Rh(CO)(PMe3)], [(H)2Rh(PMe3)2(mu-Cl)2Rh(CO)(PMe3)] and [HRh(PMe3)2(mu-H)(mu-Cl)2Rh(CO)(PMe3)] reveal that such species are able to play a similar role in hydrogenation catalysis. When the analogous iodide complexes [RhIPPh3)2]2 and [RhI(PPh3)3] are examined, [Rh(H)2(PPh3)2(mu-I)2Rh(PPh3)2], [Rh(H)2(PPh3)2(mu-I)]2 and [Rh(H)2I(PPh3)3] are observed in addition to the corresponding binuclear alkene-dihydride products. The higher initial activity of these precursors is offset by the formation of the trirhodium phosphide bridged deactivation product, [[(H)(PPh3)Rh(mu-H)(mu-I)(mu-PPh2)Rh(H)(PPh3)](mu-I)2Rh(H)2PPh3)2]
RESUMEN
In this study we report the application of continuous-wave (CW) electron paramagnetic resonance (EPR) constant-time spectral spatial imaging (CTSSI) for in vivo oxymetry. 2D and 3D SSI studies of a phantom and live mice were carried out using projection reconstruction (PR) and constant-time (CT) modalities using a CW-EPR spectrometer/imager operating at 300 MHz frequency. Distortion of line shape, which is inherent in the PR method, was minimized by the CTSSI modality. It was also found that CTSSI offers improved noise reduction, restores a smoother line shape, and gives high convergence of estimated values. Spatial resolution was also improved by CTSSI, although fundamental spectral line-width broadening was observed. Although additional corrections are required for accurate estimations of spectral line width, CTSSI was able to demonstrate distinct differences in oxygen tension between a tumor and the normal legs of a C3H mouse. The PR method, on the other hand, was unable to make such a distinction unequivocally with the triarylmethyl spin probes. CTSSI promises to be a more suitable method for quantitative in vivo oxymetric studies using radiofrequency EPR imaging (EPRI).
Asunto(s)
Espectroscopía de Resonancia por Spin del Electrón , Procesamiento de Imagen Asistido por Computador , Neoplasias Experimentales/diagnóstico , Oximetría , Animales , Femenino , Ratones , Ratones Endogámicos C3H , Fantasmas de ImagenRESUMEN
The reactivity of the cluster family [Ru(3)(CO)(12-x)(L)(x)] (in which L=PMe(3), PMe(2)Ph, PPh(3) and PCy(3), x=1-3) towards hydrogen is described. When x=2, three isomers of [Ru(3)(H)(mu-H)(CO)(9)(L)(2)] are formed, which differ in the arrangement of their equatorial phosphines. Kinetic studies reveal the presence of intra- and inter-isomer exchange processes with activation parameters and solvent effects indicating the involvement of ruthenium-ruthenium bond heterolysis and CO loss, respectively. When x=3, reaction with H(2) proceeds to form identical products to those found with x=2, while when x=1 a single isomer of [Ru(3)(H)(mu-H)(CO)(10)(L)] is formed. Species [Ru(3)(H)(mu-H)(CO)(9)(L)(2)] have been shown to play a kinetically significant role in the hydrogenation of an alkyne substrate through initial CO loss, with rates of H(2) transfer being explicitly determined for each isomer. A less significant secondary reaction involving loss of L yields a detectable product that contains both a pendant vinyl unit and a bridging hydride ligand. Competing pathways that involve fragmentation to form [Ru(H)(2)(CO)(2)(L)(alkyne)] are also observed and shown to be favoured by nonpolar solvents. Kinetic data reveal that catalysis based on [Ru(3)(CO)(10)(PPh(3))(2)] is the most efficient although [Ru(3)(H)(mu-H)(CO)(9)(PMe(3))(2)] corresponds to the most active of the detected intermediates.
RESUMEN
Low temperature in-situ UV irradiation of toluene solutions containing bis(alkene)rhodium complexes and parahydrogen in conjunction with NMR monitoring enables the characterisation of unstable eta 2-solvent complexes and dihydrogen activation products.
RESUMEN
This study describes the use of the single-point imaging (SPI) modality, also known as constant-time imaging (CTI), in radiofrequency (RF) Fourier transform (FT) electron paramagnetic resonance (EPR). The SPI technique, commonly used for high-resolution solid-state nuclear magnetic resonance (NMR) imaging, has been successfully applied to 2D and 3D RF-FT-EPR imaging of phantoms containing narrow-line EPR spin probes. The SPI scheme is essentially a phase-encoding technique that operates by acquiring a single data point in the free induction decay (FID) after a fixed delay (phase-encoding time), following the pulsed RF excitation, in the presence of static magnetic field gradients. Since the phase-encoding time remains constant for a given image data set, the spectral information is automatically deconvolved, providing well-resolved pure spatial images. Therefore, images obtained using SPI are artifact-free and the resolution is not significantly limited by the line width, compared to the images obtained using the conventional filtered back-projection (FBP) scheme, suggesting that the SPI modality may have advantages for EPR imaging of large objects. In this work the advantages and limitations of SPI as compared to FBP are investigated by imaging suitable phantom objects. Although SPI takes longer to perform than the FBP method, optimization of the data collection scheme may increase the temporal resolution, rendering this technique suitable for in vivo studies. Spectral information can also be extracted from a series of SPI images that are generated as a function of the delay from the excitation pulse.