4.5 Article

Solvent-Free Dynamic Nuclear Polarization of Amorphous and Crystalline ortho-Terphenyl

Journal

JOURNAL OF PHYSICAL CHEMISTRY B
Volume 117, Issue 10, Pages 3040-3046

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/jp311237d

Keywords

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Funding

  1. National Institute of Health of DNP projects at the Francis Bitter Magnet Laboratory [EB002804, EB002026, GM095843]
  2. Natural Sciences and Engineering Research Council of Canada
  3. Deutsche Forschungsgemeinschaft [CO802/1-1]

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Dynamic nuclear polarization (DNP) of amorphous and crystalline ortho-terphenyl (OTP) in the absence of glass forming agents is presented in order to gauge the feasibility of applying DNP to pharmaceutical solid-state nuclear magnetic resonance experiments and to study the effect of intermolecular structure, or lack thereof, on the DNP enhancement By way of H-1-C-13 cross polarization, we obtained a DNP enhancement (epsilon) of 58 for 95% deuterated OTP in the amorphous state using the biradical bis-TEMPO terephthalate (bTtereph) and epsilon of 36 in the crystalline state. Measurements of the H-1 T-1 and electron paramagnetic resonance experiments showed the crystallization process led to phase separation of the polarization agent, creating an inhomogeneous distribution of radicals within the sample. Consequently, the effective radical concentration was decreased in the bulk OTP phase, and long-range H-1-H-1 spin diffusion was the main polarization propagation mechanism. Preliminary DNP experiments with the glass forming anti-inflammation drug, indomethacin, showed promising results, and further studies are underway to prepare DNP samples using pharmaceutical techniques.

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