Author
Listed:
- Jacob A. Smith
(University of Virginia Department of Chemistry)
- Katy B. Wilson
(University of Virginia Department of Chemistry)
- Reilly E. Sonstrom
(University of Virginia Department of Chemistry)
- Patrick J. Kelleher
(University of Virginia Department of Chemistry)
- Kevin D. Welch
(University of Virginia Department of Chemistry)
- Emmit K. Pert
(University of Virginia Department of Chemistry)
- Karl S. Westendorff
(University of Virginia Department of Chemistry)
- Diane A. Dickie
(University of Virginia Department of Chemistry)
- Xiaoping Wang
(Oak Ridge National Laboratory)
- Brooks H. Pate
(University of Virginia Department of Chemistry)
- W. Dean Harman
(University of Virginia Department of Chemistry)
Abstract
The hydrogen isotopes deuterium (D) and tritium (T) have become essential tools in chemistry, biology and medicine1. Beyond their widespread use in spectroscopy, mass spectrometry and mechanistic and pharmacokinetic studies, there has been considerable interest in incorporating deuterium into drug molecules1. Deutetrabenazine, a deuterated drug that is promising for the treatment of Huntington’s disease2, was recently approved by the United States’ Food and Drug Administration. The deuterium kinetic isotope effect, which compares the rate of a chemical reaction for a compound with that for its deuterated counterpart, can be substantial1,3,4. The strategic replacement of hydrogen with deuterium can affect both the rate of metabolism and the distribution of metabolites for a compound5, improving the efficacy and safety of a drug. The pharmacokinetics of a deuterated compound depends on the location(s) of deuterium. Although methods are available for deuterium incorporation at both early and late stages of the synthesis of a drug6,7, these processes are often unselective and the stereoisotopic purity can be difficult to measure7,8. Here we describe the preparation of stereoselectively deuterated building blocks for pharmaceutical research. As a proof of concept, we demonstrate a four-step conversion of benzene to cyclohexene with varying degrees of deuterium incorporation, via binding to a tungsten complex. Using different combinations of deuterated and proteated acid and hydride reagents, the deuterated positions on the cyclohexene ring can be controlled precisely. In total, 52 unique stereoisotopomers of cyclohexene are available, in the form of ten different isotopologues. This concept can be extended to prepare discrete stereoisotopomers of functionalized cyclohexenes. Such systematic methods for the preparation of pharmacologically active compounds as discrete stereoisotopomers could improve the pharmacological and toxicological properties of drugs and provide mechanistic information related to their distribution and metabolism in the body.
Suggested Citation
Jacob A. Smith & Katy B. Wilson & Reilly E. Sonstrom & Patrick J. Kelleher & Kevin D. Welch & Emmit K. Pert & Karl S. Westendorff & Diane A. Dickie & Xiaoping Wang & Brooks H. Pate & W. Dean Harman, 2020.
"Preparation of cyclohexene isotopologues and stereoisotopomers from benzene,"
Nature, Nature, vol. 581(7808), pages 288-293, May.
Handle:
RePEc:nat:nature:v:581:y:2020:i:7808:d:10.1038_s41586-020-2268-y
DOI: 10.1038/s41586-020-2268-y
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Citations
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Cited by:
- Nian Li & Jinhang Li & Mingzhe Qin & Jiajun Li & Jie Han & Chengjian Zhu & Weipeng Li & Jin Xie, 2022.
"Highly selective single and multiple deuteration of unactivated C(sp3)-H bonds,"
Nature Communications, Nature, vol. 13(1), pages 1-8, December.
- Justin T. Weatherford-Pratt & Jacob A. Smith & Jeremy M. Bloch & Megan N. Ericson & Jeffery T. Myers & Karl S. Westendorff & Diane A. Dickie & W. Dean Harman, 2023.
"The double protonation of dihapto-coordinated benzene complexes enables dearomatization using aromatic nucleophiles,"
Nature Communications, Nature, vol. 14(1), pages 1-8, December.
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