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Chemical Synthesis of (+)-Ryanodine and (+)-20-Deoxyspiganthine

Version 7 2017-04-28, 12:21
Version 6 2017-04-27, 14:24
Version 5 2017-04-26, 05:15
Version 4 2017-04-19, 19:04
Version 3 2017-03-09, 17:50
Version 2 2017-03-09, 17:20
Version 1 2017-03-09, 14:20
Posted on 2017-04-28 - 12:21
(+)-Ryanodine is a natural product modulator of ryanodine receptors, important intracellular calcium ion channels that play a critical role in signal transduction leading to muscle movement and synaptic transmission. Chemical derivatization of (+)-ryanodine has demonstrated that certain peripheral structural modifications can alter its pharmacology, and that the pyrrole-2-carboxylate ester is critical for high affinity binding to ryanodine receptors. However, the structural variation of available ryanodine analogues has been limited by the challenge of site-specific functionalization of semisynthetic intermediates, such as (+)-ryanodol. Here we report a synthetic strategy that provides access to (+)-ryanodine and the related natural product (+)-20-deoxyspiganthine in 18 and 19 steps, respectively. A key feature of this strategy is the reductive cyclization of an epoxide intermediate that possesses the critical pyrrole-2-carboxylate ester. This approach allows for the direct introduction of this ester in the final stage of the synthesis and provides a framework for the synthesis of previously inaccessible synthetic ryanoids.

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