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Optimal 13C NMR investigation of intrinsically disordered proteins at 1.2 GHz

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NATURE PROTOCOLS
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NATURE PORTFOLIO
DOI: 10.1038/s41596-023-00921-9

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Nuclear magnetic resonance (NMR) spectroscopy is a powerful technique for characterizing biomolecules at atomic resolution. The availability of ultra-high-field NMR instrumentation has opened up new possibilities for studying more complex systems, such as flexible proteins and protein regions. While conducting experiments at such high field strengths comes with challenges, strategies and tricks can be employed to optimize the experiments.
Nuclear magnetic resonance (NMR) spectroscopy is a powerful technique for characterizing biomolecules such as proteins and nucleic acids at atomic resolution. Increased magnetic field strengths drive progress in biomolecular NMR applications, leading to improved performance, e.g., higher resolution. A new class of NMR spectrometers with a 28.2 T magnetic field (1.2 GHz H-1 frequency) has been commercially available since the end of 2019. The availability of ultra-high-field NMR instrumentation makes it possible to investigate more complex systems using NMR. This is especially true for highly flexible intrinsically disordered proteins (IDPs) and highly flexible regions (IDRs) of complex multidomain proteins. Indeed, the investigation of these proteins is frequently hampered by the crowding of NMR spectra. The advantages, however, are accompanied by challenges that the user must overcome when conducting experiments at such a high field (e.g., large spectral widths, radio frequency bandwidth, performance of decoupling schemes). This protocol presents strategies and tricks for optimising high-field NMR experiments for IDPs/IDRs based on the analysis of the relaxation properties of the investigated protein. The protocol, tested on three IDPs of different molecular weight and structural complexity, focuses on C-13-detected NMR at 1.2 GHz. A set of experiments, including some multiple receiver experiments, and tips to implement versions tailored for IDPs/IDRs are described. However, the general approach and most considerations can also be applied to experiments that acquire H-1 or N-15 nuclei and to experiments performed at lower field strengths.

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