Abstract
Nuclear magnetic resonance (NMR) spectroscopy is a powerful analytical tool used in modern science and technology. Its novel incarnation, based on measurements of NMR signals without external magnetic fields, provides direct access to intramolecular interactions based on heteronuclear scalar J-coupling. The uniqueness of these interactions makes each zero-field NMR spectrum distinct and useful in chemical fingerprinting. However, the necessity of heteronuclear coupling often results in weak signals due to the low abundance of certain nuclei (e.g., 15N). Hyperpolarization of such compounds may solve the problem. In this work, we investigate molecules with natural isotopic abundance that are polarized using non-hydrogenative parahydrogen-induced polarization. We demonstrate that spectra of hyperpolarized naturally abundant pyridine derivatives can be observed and uniquely identified whether the same substituent is placed at a different position of the pyridine ring or different constituents are placed at the same position. To do so, we constructed an experimental system using a home-built nitrogen vapor condenser, which allows for consistent long-term measurements, crucial for identifying naturally abundant hyperpolarized molecules at a concentration level of ~1 mM. This opens avenues for future chemical detection of naturally abundant compounds using zero-field NMR.
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Introduction
Over the past decade, the zero- and ultralow-field (ZULF) nuclear magnetic resonance (NMR) technique has emerged as a complementary method to conventional high-field (≳1 T) NMR1,2,3,4. Its specific advantage is the ability to directly probe spin-spin interactions in zero field, where the Zeeman interaction, and hence the chemical shift, disappears, and the NMR signals are purely related with J-coupling. In turn, information-rich and chemically specific spectra (the so-called J-spectra)5 of narrow NMR lines (dipolar relaxation and chemical shift anisotropy are strongly suppressed)6,7 enabling high-resolution spectroscopy can be observed. Absence of strong field alleviates the necessity for cryogenic cooling, so that portable and inexpensive ZULF NMR spectrometers can be constructed, prophesizing a new era of NMR research8,9,10.
Since no magnetic field is present during the zero-field NMR measurements, samples need to be spin-polarized prior to the measurements. This can be achieved by remote thermal prepolarization with a permanent magnet located outside of the zero-field (detection) region11. This is a universal approach, providing, however, low sensitivity of the measurements. Alternatively, polarization of the sample can be achieved by application of chemically discerning hyperpolarization methods12,13,14,15 among which para-hydrogen-induced polarization (PHIP) is one of the most promising as it works well at ZULFs16,17,18,19. The resulting PHIP-signal enhancement can be achieved using hydrogenative PHIP20,21,22 or the so-called Signal Amplification by Reversible Exchange (SABRE)23,24,25,26, which is the method used in this work. SABRE employs a reversible interaction between an active iridium-based catalyst (formed from a precatalyst), a substrate (e.g., pyridine), and para-hydrogen (pH2) (Fig. 1). Due to this reversible interaction, a labile complex, containing protons from pH2 and the substrate, is formed. In such a complex, high polarization of pH2 protons is transferred to the molecule of interest through the J-coupling network of the catalyst (see Fig. 1b and d). As the active complex splits up, releasing the molecule into the solution, the structure of the molecule is unchanged while its spin polarization is high.
Observation of ZULF NMR spectra requires existence of heteronuclear J-coupling in the molecule of interest. Hence, low abundance of most spin-1/2 nuclei (e.g., 13C, 15N, 29Si) means that only a small fraction of molecules in the sample generates ZULF NMR signals. To address this problem, expensive isotopic labelling of molecules is needed5, with notable exceptions of molecules containing at least two of such spin-1/2 nuclei as 1H, 19F, and 31P of nearly 100% abundance11,27. The large polarization achieved through SABRE can alleviate the need for isotopically labelled compounds as the efficient sensitization of 1H, 13C, 15N, 19F, 31P, 29Si, etc., nuclei has proven possible with the use of SABRE technique28,29,30.
The SABRE technique is effective for catalytic hyperpolarization of such compounds as pyridine, which is a readily available molecular target now known to produce a high level of polarization31,32. While pyridine is toxic itself, it exhibits derivatives that are reflective of a wide range of pharmaceutical agents that show antimicrobial, antiviral, or anticancer properties33, while several promising biorelevant pyridine derivatives can be hyperpolarized32,34,35,36. The increased interest in the molecule and its derivatives also reflects their potential in magnetic resonance imaging (MRI) as contrast agents. For example, pyridine derivatives (nicotinic acid and nicotinamide) are B3 vitamers and have been hyperpolarized by SABRE to detect conventional NMR/MRI signals37,38. It should be noted that in this context pyridine was studied as a SABRE target not only in conventional NMR but also in ZULF NMR experiments8,17.
Although in zero field both chemical identification5,9 and application of various hyperpolarization methods16,17 have been demonstrated, until now they have not been studied in conjugation with each other. Without doubt, real-world applications of ZULF NMR will require both the ability to work with unaltered samples and to perform chemical identification3. This is the task that we undertake in this work by investigating a group of similar molecules –pyridine derivatives– in their natural isotopic abundance (containing 0.36% of 15N with spin-1/2) using ZULF NMR and SABRE hyperpolarization. We collect hyperpolarized zero-field spectra for natural abundant pyridine derivatives, not yet studied by ZULF NMR, and demonstrate that they can be distinguished by means of their zero-field spectra. This is done by studies of the pyridine derivatives containing the same substituent, at different ring positions, as well as various substituents at the same ring position. Among the different pyridine derivatives, we specifically target nicotinamide, which is the first biomolecule hyperpolarized with SABRE to be measured in zero field. To measure spectra with good signal-to-noise ratio, we develop an experimental system enabling reliable signal averaging. The system is based on a vapor condenser, which ensures a stable sample composition during long-term measurements. This experimental capability allowed for monitoring catalyst activation used in the SABRE process at zero magnetic field. Finally, our experimental results are supported with numerical simulations, which well reproduce all the spectra. This validates our theoretical approach and paves the way toward chemical identification of naturally abundant compounds using zero-field NMR.
Results and discussion
In-situ catalyst activation and long-term signal monitoring with ZULF NMR
A zero-field NMR signal can be used to directly measure the efficiency of polarization transfer during repeated SABRE experiments. Figure 2a presents the ZULF NMR spectrum of pyridine measured at different times after the experiment initiation. As shown, the amplitude of the signal increases with the length of the experiment. Moreover, because the area under the ZULF NMR spectrum (signal intensity) can be used as a quantitative measure of the efficiency of the polarization transfer, Fig. 2b shows the ZULF NMR spectrum of pyridine integrated between 5 and 25 Hz as a function of the time of bubbling pH2 through the solution. For this study, each transient was measured for 6 s, and each resulting data point was averaged over four successive transients. The data presented in Fig. 2b (red points) shows the initial growth of signal intensity over time indicating an improvement in the polarization efficiency. Interestingly, the signal starts at a nonzero value, which indicates operation with a partially activated sample. The results of a similar experiment, starting with a fully activated catalyst, are overlayed in Fig. 2b (blue points). The activation was achieved by purging the sample with a large volume of pH2 (10 min purge with a flow of 300 sccm) before starting the measurement. This, combined with the condenser keeping the sample composition stable over time (see discussion below), results in the detection of hundreds of stable (~2% standard deviation) zero-field NMR signal transients with signal amplitude twice that observed during the first measurement (red points Fig. 2b). As catalyst activation provides stronger zero-field signals, it was used in the subsequent studies of naturally abundant pyridine derivatives.
The data presented in Fig. 2b, as well as spectra of natural abundant molecules presented in the next section, are the result of long-term experiments (tens of minutes of total pH2 bubbling). The constant flow of dry gas can result in the evaporation of an NMR sample, causing changes in spectra and polarization efficiency39. Additionally, when an NMR sample reflects a high concentration of analyte, the evaporation of solvent will cause precipitation. In this case, precipitation can lead to capillary obstruction, resulting in interrupted pH2 bubbling during the SABRE experiment. In our work, a vapor condenser, using a cold nitrogen vapor coolant, was introduced to enable long-term measurement (see Methods sections and Fig. 4). The cold nitrogen vapor in the condenser keeps the top of the NMR tube at a lower controllable temperature, allowing the solvent vapor to recondense and return to the bottom of the tube as liquid (the bottom of the NMR is heated up to ~40 °C, see Methods section). When the condenser temperature is maintained at about 0 °C, a sample of a volume of 0.5 ml can be used to record NMR signals for over 7.5 h (allowing for up to 10 times longer measurement than presented in the following section). Furthermore, increasing the flow of the liquid nitrogen vapor through the condenser would make even longer measurements possible. As shown in Fig. 2b, the use of condenser results in the robustness of the SABRE protocol (same amplitude over time after activation), delivering similar observations over at least 35 min, which is an important observation given the known dependence on the SABRE response on concentration. An alternative method to prolong SABRE experiments, where the gas is presaturated with methanol vapor, has been described in the literature39. Despite the effectiveness of this technique it requires use of extra solvent volume, while controlling the condenser temperature could be viewed as an advantage of the method used in our study.
While the initial investigations on the efficiency of polarization transfer in SABRE were performed with Crabtree’s catalyst, in order to enable the detection of much weaker NMR signals from naturally abundant compounds (presented in the following section), a change was made to the experimental protocol. Commercially available Crabtree’s catalyst was replaced with [IrCl(COD)(IMes)] precatalyst, which is known to yield higher hyperpolarization levels for pyridine and its derivatives (activation process and hyperpolarization mechanism are shown in Fig. 1c, d)40.
Natural abundance SABRE at zero field
Figure 3 presents zero-field NMR spectra of hyperpolarized pyridine derivatives: 3,5-dichloropyridine, 3-methoxypyridine, 4-methoxypyridine, 3-methylpyridine, 4-methylpyridine, and nicotinamide. Due to the need for a heteronuclear coupling, the spectra exclusively correspond to 15N-pyridine, 15N-3,5-dichloropyridine, 15N-3-methoxypyridine, 15N-4-methoxypyridine, 15N-3-methylpyridine, 15N-4-methylpyridine, and 15N-nicotinamide, which are present only at a level of 0.36% due to the 15N abundance. In these molecules, the strongest J-coupling, 2JNH, arises between 15N and the two ortho-protons of the pyridine ring. Thereby, the main peaks observed in the spectra of the molecules appear at 3/2 2JNH, which corresponded to ≈ 15 Hz (indicated by the dashed line in Fig. 3)41. It is clear from these data that, when these dominant J-couplings are similar, the weaker (at least three-bond) hetero- (1H-15N) and homonuclear J-couplings (1H-1H) lead to the modification of the spectra. These modifications are responsible for uniqueness of zero-field NMR spectra and pave avenues for chemical analysis with the technique. It should be noted that analytical calculations of zero-field spectra are only possible in the simplest spin topologies. In a more involved spin system, yet, when the strength of the couplings forms a clear hierarchy, one may implement a perturbative approach to determine the structure of zero-field spectra42. Such calculations can provide more complex, yet analytical formula for shift and splitting of the NMR lines. However, in molecules without such a clear hierarchy, one may not be able to accurately calculate the spectra using perturbation theory approaches. In such a case, the simulations of the spectra may be performed based on numerical diagonalization of the spin Hamiltonian. Although this technique offers the most precise calculation and reproduction of the experimental spectrum, it does not provide simple means for the interpretation of the observed spectra.
We start with the discussion of the 15N-3,5-dichloropyridine spectrum (second spectrum from the top in Fig. 3). In this spectrum, a single line at 15.7 Hz is observed. The line is narrower than the corresponding line in the 15N-pyridine spectrum (top spectrum in Fig. 3) visible at 15.4 Hz. This narrowing is a result of a substitution of two hydrogen atoms by self-decoupled chlorine atoms27, which reduces the number of weak JNH-interactions and limits splitting of the main peak (the splitting is smaller than the resonance width, so its absence manifests as the line narrowing). A similar argument can be made when discussing the 15N-nicotinamide spectrum (third from the top in Fig. 3), where the amide substituent does not have a coupling to a single proton.
Another result of the substitution of hydrogens is a violation of the chemical symmetry of the two ortho-protons, as in 15N-nicotinamide, 15N-3-methoxypyridine, and 15N-3-methylpyridine. The change influences the bonding in these molecules, which leads to the dependence of the J-coupling constant on the position in the molecule. This leads to the appearance of several additional peaks of relatively high amplitude observed in the zero-field spectra around the main line. It should be noted that the lower signal-to-noise ratio seen in the 15N-nicotinamide spectrum compared to other spectra is a consequence of the use of a lower substrate concentration due to its low solubility in methanol. In our study, this issue was partially addressed by using dimethyl sulfoxide (DMSO) as a co-solvent. This particular result demonstrates the use of the SABRE technique to polarize and detect a spectrum of the biomolecule, B3 vitaminer, under zero-field conditions for the first time ever. In a way, this result hints at the possibility of using hyperpolarized nicotinamide for ultralow-field imaging37,43.
When methyl is a substrate in a pyridine-based molecule, additional (weak) J-couplings arise, forming a more complex spin-spin network. This additional interaction leads to splitting of the zero-field NMR lines, and it manifests as broadening of the main peak in both 15N-3-methylpyridine and 15N-4-methylpyridine spectra (Fig. 3). Once again this broadening originates from the inability to resolve splitting of the lines (in simulations, the influence of methyl protons is implemented using a simple line broadening function). On the other hand, narrower lines are observed in the spectra of 15N-3-methoxypyridine and 15N-4-methoxypyridine even though a methoxy group also contains three 1H nuclei. The reason for this is the much weaker (longer-range) J-couplings between 1H nuclei in the methoxy group and 15N compared to those in the methyl group. On the other hand, there was no spectral peak arising from 13C-isotopomers at their natural abundance. This finding might be explained by a reduction in the efficiency of hyperpolarization transfer to 13C in the presence of quadrupolar nuclei (i.e., 14N)44 and the complex spin system of 13C-15N isotopomers resulting in numerous split lines with low peak amplitudes17.
The presented experimental results are supported by the results of numerical simulations of ZULF NMR spectra (Fig. 3b). Such simulations are performed with the J-coupling constants taken from the literature. For more details on the simulation parameters and coupling networks see Supplementary Figure 2 and Supplementary Table 1,2,3,4, while the simulation script is included as Supplementary Data 2. Theoretical model reflects only free ligands (pyridine derivatives) in the solution as T2 of the bound compounds is short making them not detectable with zero-field NMR. All the simulated spectra match experimental results in both the positions and relative amplitudes of the NMR lines (raw data can be found in Supplementary Data 1). The discussion presented in this section shows that each pyridine derivative has either a different spin topology or the spin network is affected by different values of the J-coupling constants between different atoms. Thereby a unique zero-field NMR spectrum is associated with each molecule, demonstrating the ability of application of zero-field NMR for chemical identification. It should be stressed that such identification is possible with samples containing 1–2 M pyridine derivatives at natural abundance of 15N (corresponding to 3.6–7.2 mM of NMR active molecules) by measuring less than 200 transients. This, combined with the robust of the experimental protocol described above, suggests the possibility of SABRE-enhanced ZULF NMR measurements with naturally abundant 15N-compounds at millimolar concentration levels.
Conclusions
In this work, we investigated SABRE-polarization at zero-magnetic field for a range of molecules: pyridine derivatives at their natural isotopic abundance. Using zero-field NMR, we analyzed the molecular spectral patterns and demonstrated their uniqueness with respect to both the substituent and its position. Such identification was performed for the first time using hyperpolarized samples at natural isotopic abundance. Along with the measurements, the experimental setup was constructed, allowing long-term in-situ SABRE experiments performed under zero-field conditions. It enabled studies of the activation of the SABRE catalyst for optimal zero-field hyperpolarization protocol, as well as long-term (many averages) measurements, allowing for the study of compounds at natural isotopic abundance of 15N. A particularly promising extension of the current study is the development of in-situ SABRE-RELAY hyperpolarization for ZULF NMR45. This would expand the range of molecules that could be investigated without the need for expensive labeling. With this we improved the applicability of zero-field NMR spectroscopy as a specific, sensitive, compact, and inexpensive method for chemical and biochemical analysis, paving the way for further applications of the technique in biochemical studies and fundamental-physics investigations (e.g., spin-gravity coupling searches).
Methods
Sample preparation
For monitoring the SABRE-catalyst activation and long-term signal stability check, a sample with 70 mM of 15N-pyridine (CAS#34322-45-7) and 2 mM of Crabtrees’s catalyst, [Ir(COD)(PCy3)(Py)]PF6, (CAS# 64536-78-3) was prepared in 300 μL of methanol.
For the study of naturally abundant 15N-pyridine derivatives, chemicals: pyridine (CAS# 110-86-1), 3,5-dichloropyridine (CAS# 2457-47-8), nicotinamide (CAS# 98-92-0), 3-methoxypyridine (CAS# 7295-76-3), 4-methoxypyridine (CAS# 620-08-6), 3-methylpyridine (CAS# 108-99-6), 4-methylpyridine (CAS# 108-89-4), and methanol (CAS# 67-56-1) were purchased from Sigma-Aldrich and used without further purification. The NMR samples consisted of a 25 mM of air-stable SABRE precatalyst, [IrCl(COD)(IMes)], mixed with 2 M solution of the corresponding pyridine derivatives (except for nicotinamide) were dissolved in 500 μL of methanol. Due to the low solubility of nicotinamide in methanol, a 1 M nicotinamide solution was prepared by addition of 20 μL of DMSO and 480 μL of methanol to 25 mM of the precatalyst.
Para-hydrogen (44% of pH2) was produced by passing pure hydrogen gas through a cold tubing (77 K) filled with an iron (III) oxide catalyst (a home-built para-hydrogen generator). Produced pH2 filled an aluminium cylinder, which was then connected to a bubbling system to expose the NMR sample to the gas. Initially, the precatalyst was activated in Earth’s field by bubbling pH2 through the samples for a few minutes. The change in the sample colour (the sample becoming transparent) was accepted as an indication of catalyst activation. The sample was then placed into the zero-field NMR spectrometer. The SABRE experiments were carried out by bubbling pH2 through sample solutions located in the zero-field region for 6–15 s at a flow rate of ~80 sccm and pressure of 5 bar. After termination of the bubbling, a magnetic-field pulse (π/2 rotation for 1H) was applied and the acquisition of the signal started. For details of the experimental sequence see Supplementary Note 1 and Supplementary Fig. 1.
Zero-field NMR spectrometer
The key components of the ZULF NMR spectrometer (prototype by DM Technologies) used in this work are shown in Fig. 4. Two commercial, ready-to-use Optically-Pumped Magnetometers (OPMs) (QuSpin QZFM) were used for the detection of weak, slowly-oscillating magnetic field, originating from NMR samples. Although the magnetometers could simultaneously detect two components of the field, only one direction per sensor was used. This choice was motivated by a fixed direction of the oscillations of samples’ magnetization at the zero field. The magnetometers were placed in a 3D-printed coil frame and held in the closest position to the NMR sample contained in a 5 mm glass tube. To attenuate external magnetic fields a compact, three-layer mu-metal shield (Twinleaf MS1F) with an additional ferrite innermost layer was used. The magnetometer and the sample during the detection were enclosed inside the shield. An absolute zero field (<0.1 nT) was achieved using a set of magnetic-field coils located inside the shielding. At the same time, additional coils, mounted on the smaller frame closer to the sample, were used to apply DC magnetic-field pulses. The top of the NMR tube was connected to a bubbling system, which used a pair of solenoid valves to control the flow of para-hydrogen through a small capillary submerged in the NMR sample (a more detailed description of the bubbling system and the typical experimental sequence can be found in Supplementary Note 1 and Supplementary Fig. 1). The top of the tube was also enclosed in the vapor condenser, a 3D-printed chamber, that was cooled with liquid nitrogen vapor. This minimized evaporation of the sample. Magnetometer signals were acquired using a 16-bit DAQ card (NI USB-6002), which was also used to generate the experimental sequence, controlling solenoid valves for bubbling, magnetic-field pulses, etc. The experimental sequence was pre-programmed with the use of LabView software that run on a PC. The computer was also used for data acquisition.
Data postprocessing and spectra simulation
Magnetometer data (2000 Sa/s) acquired from two sensors were first de-based using a polynomial fit that subtracted slow drift of the magnetometer signal. Due to the finite bandwidth of the OPMs, the initial 35 ms of the signals were cut off, as the magnetometer response was saturated by the magnetic-field pulse used to generate the NMR signal. The cut points were reconstructed using autoregressive backprediction. Additional exponential apodization was applied to account for non-optimal signal acquisition time (10 s for all experiments) and hence improve the signal-to-noise ratio. Time signals from both OPMs were then Fourier transformed, phase corrected, and combined to produce a final zero-field NMR spectrum. Data post-processing was performed using Wolfram Mathematica.
The experimental spectra are accompanied by the simulation of zero-field NMR spectra based on the numerical diagonalization of the density matrix in the basis of the zero-field Hamiltonian1 and subsequent determination of the magnetization along the sensitive axis of the OPM. Calculations were performed using the high-performance spin simulation library Spintrum46,47, while the form of the density matrix following a magnetic-field pulse was assumed to be proportional to the nuclear polarization created along the sensitive direction of the sensor. This provided an adequate match to the experimental results. The relevant J-coupling constants used in the spectra simulations were taken from the literature and are summarized in Supplementary Tables 1, 2, 3, 4. In addition, line broadening was applied using a decaying single-exponential apodization function to simulated spectra based on experimental results.
Data availability
All raw experimental and simulated NMR spectra are available in Supplementary Data 1.
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Acknowledgements
The authors acknowledge support from the European Union’s Horizon 2020 research and innovation program under the Marie Skłodowska-Curie grant agreement No. 766402. P.P. and S.A. acknowledge the support of a grant from the SciMat Priority Research Area under the Strategic Programme Excellence Initiative at the Jagiellonian University.
Funding
Open Access funding enabled and organized by Projekt DEAL.
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Contributions
P.P., S.A., S.D., and S.P. conceived the experiments. P.P., S.A., and Ł.B. designed and constructed the experimental apparatus. P.P., S.A., and O.B. conducted the experiment(s). P.P, S.A., and O.B. analysed the results. S.D. and S.P contributed to the discussion of the experimental results. All authors contributed to the writing and review of the manuscript.
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Put, P., Alcicek, S., Bondar, O. et al. Detection of pyridine derivatives by SABRE hyperpolarization at zero field. Commun Chem 6, 131 (2023). https://doi.org/10.1038/s42004-023-00928-z
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DOI: https://doi.org/10.1038/s42004-023-00928-z
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