A high-field cellular DNP-supported solid-state NMR approach to study proteins with sub-cellular specificity

Publication date

2023-09-05

Authors

Beriashvili, DavidISNI 0000000506322171
Yao, Ru
D'Amico, FrancescaISNI 0000000518035313
Krafčíková, Michaela DzurovISNI 0000000524014949
Gurinov, AndreiISNI 0000000493067967
Safeer, Adil A.ISNI 0000000507309489
Cai, Xinyi
Mulder, Monique P CISNI 0000000388562464
Liu, Yangping
Folkers, Gert E.ISNI 0000000390350786

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Advisors

Supervisors

Document Type

Article
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License

cc_by_nc

Abstract

Studying the structural aspects of proteins within sub-cellular compartments is of growing interest. Dynamic nuclear polarization supported solid-state NMR (DNP-ssNMR) is uniquely suited to provide such information, but critically lacks the desired sensitivity and resolution. Here we utilize SNAPol-1, a novel biradical, to conduct DNP-ssNMR at high-magnetic fields (800 MHz/527 GHz) inside HeLa cells and isolated cell nuclei electroporated with [ 13C, 15N] labeled ubiquitin. We report that SNAPol-1 passively diffuses and homogenously distributes within whole cells and cell nuclei providing ubiquitin spectra of high sensitivity and remarkably improved spectral resolution. For cell nuclei, physical enrichment facilitates a further 4-fold decrease in measurement time and provides an exclusive structural view of the nuclear ubiquitin pool. Taken together, these advancements enable atomic interrogation of protein conformational plasticity at atomic resolution and with sub-cellular specificity.

Keywords

General Chemistry

Citation

Beriashvili, D, Yao, R, D'Amico, F, Krafčíková, M, Gurinov, A, Safeer, A, Cai, X, Mulder, M P C, Liu, Y, Folkers, G E & Baldus, M 2023, 'A high-field cellular DNP-supported solid-state NMR approach to study proteins with sub-cellular specificity', Chemical Science, vol. 14, no. 36, pp. 9892-9899. https://doi.org/10.1039/d3sc02117c