Time domain DNP with the NOVEL sequence

Time domain DNP with the NOVEL sequence

Show other versions (1)

We present results of a pulsed dynamic nuclear polarization (DNP) study at 0.35 T (9.7 GHz/14.7 MHz for electron/1H Larmor frequency) using a lab frame-rotating frame cross polarization experiment that employs electron spin locking fields that match the 1H nuclear Larmor frequency, the so called NOV...

Full description

Bibliographic Details
Main Authors: Can, Thach V (Contributor), Walish, Joseph John (Contributor), Swager, Timothy M (Contributor), Griffin, Robert Guy (Contributor)
Other Authors: Massachusetts Institute of Technology. Department of Chemistry (Contributor), Francis Bitter Magnet Laboratory (Massachusetts Institute of Technology) (Contributor)
Format: Article
Language:English
Published: AIP Publishing, 2022-02-07T20:01:01Z.
Subjects:
Article
Online Access:Get fulltext
Description
Summary:We present results of a pulsed dynamic nuclear polarization (DNP) study at 0.35 T (9.7 GHz/14.7 MHz for electron/1H Larmor frequency) using a lab frame-rotating frame cross polarization experiment that employs electron spin locking fields that match the 1H nuclear Larmor frequency, the so called NOVEL (nuclear orientation via electron spin locking) condition. We apply the method to a series of DNP samples including a single crystal of diphenyl nitroxide (DPNO) doped benzophenone (BzP), 1,3-bisdiphenylene-2-phenylallyl (BDPA) doped polystyrene (PS), and sulfonated-BDPA (SA-BDPA) doped glycerol/water glassy matrices. The optimal Hartman-Hahn matching condition is achieved when the nutation frequency of the electron matches the Larmor frequency of the proton, ω[subscript 1S] = ω[subscript 0I], together with possible higher order matching conditions at lower efficiencies. The magnetization transfer from electron to protons occurs on the time scale of ∼100 ns, consistent with the electron-proton couplings on the order of 1-10 MHz in these samples. In a fully protonated single crystal DPNO/BzP, at 270 K, we obtained a maximum signal enhancement of ε = 165 and the corresponding gain in sensitivity of ε(T[subscript 1]/T[subscript B])[superscript 1/2] = 230 due to the reduction in the buildup time under DNP. In a sample of partially deuterated PS doped with BDPA, we obtained an enhancement of 323 which is a factor of ∼3.2 higher compared to the protonated version of the same sample and accounts for 49% of the theoretical limit. For the SA-BDPA doped glycerol/water glassy matrix at 80 K, the sample condition used in most applications of DNP in nuclear magnetic resonance, we also observed a significant enhancement. Our findings demonstrate that pulsed DNP via the NOVEL sequence is highly efficient and can potentially surpass continuous wave DNP mechanisms such as the solid effect and cross effect which scale unfavorably with increasing magnetic field. Furthermore, pulsed DNP is also a promising avenue for DNP at high temperature.
National Institute for Biomedical Imaging and Bioengineering (U.S.) (Grant No. EB-002804)
National Institute for Biomedical Imaging and Bioengineering (U.S.) (Grant No. EB-002026)
National Institute of General Medical Sciences (U.S.) (Grant No. GM095843)

Similar Items