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Understanding the Thalidomide Chirality in Biological Processes by the Self-disproportionation of Enantiomer
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- SHIBATA Norio
- Department of Nanopharmaceutical Sciences, Nagoya Institute of Technology
Bibliographic Information
- Other Title
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- サリドマイドの催奇形性と自己不均一化現象
Description
<p>Twenty years after the thalidomide disaster in the late 1950s, Blaschke et al. reported that only the (S)-enantiomer of thalidomide is teratogenic. However, other work has shown that the enantiomers of thalidomide interconvert in vivo, which begs the question: why is teratogen activity not observed in animal experiments that use (R)-thalidomide given the ready in vivo racemization (“thalidomide paradox”)? Herein, we disclose a hypothesis to explain this “thalidomide paradox” through the in-vivo self-disproportionation of enantiomers. Upon stirring a 20% ee solution of thalidomide in a given solvent, significant enantiomeric enrichment of up to 98% ee was observed reproducibly in the solution. We hypothesize that a fraction of thalidomide enantiomers epimerizes in vivo, followed by precipitation of racemic thalidomide in (R/S)-heterodimeric form. Thus, racemic thalidomide is most likely removed from biological processes upon racemic precipitation in (R/S)-heterodimeric form. On the other hand, enantiomerically pure thalidomide remains in solution, affording the observed biological experimental results: the (S)-enantiomer is teratogenic, while the (R)-enantiomer is not. </p>
Journal
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- Annual Meeting of the Japanese Society of Toxicology
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Annual Meeting of the Japanese Society of Toxicology 49.1 (0), S14-3-, 2022
The Japanese Society of Toxicology
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Details 詳細情報について
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- CRID
- 1390574666166663680
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- Text Lang
- ja
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- Data Source
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- JaLC
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- Abstract License Flag
- Disallowed