Pyranophane Transannular Diels−Alder Approach to (+)-Chatancin:  A Biomimetic Asymmetric Total Synthesis

Soucy, Pierre; L’Heureux, Alexandre; Toró, and András; Deslongchamps, Pierre

doi:10.1021/jo035193y

Cited by 38 publications

(16 citation statements)

References 20 publications

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“…The compact structure of 1 , containing seven stereocenters (six of which are contiguous), has proven to be a formidable synthetic challenge that is further exacerbated by its extreme acid sensitivity; it rapidly dehydrates to anhydrochatancin ( 3 ) under even mildly acidic conditions. Gossinger and co‐workers reported the first synthesis of (±)‐ 1 in 33 chemical steps from thymoquinone (0.7 % overall yield),7 and in 2003, after significant chemical experimentation,8 the group of Deslongchamps reported a fundamentally disparate synthetic strategy to (+)‐ 1 (23 steps from cis ‐2‐butene‐1,4‐diol) 9. Guided by the biosynthetic hypothesis shown (Figure 1 a), chatancin was postulated to be of cembrane biosynthetic origins and its complex polycyclic skeleton the result of a transannular Diels–Alder cycloaddition (TADA) of pyranophane precursor 4 .…”

Section: Methodsmentioning

confidence: 99%

Short, Enantioselective Total Synthesis of Chatancin

Zhao

Maimone

2014

Angewandte Chemie

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An enantioselective total synthesis of the polycyclic diterpene (+)‐chatancin, a potent PAF antagonist, is reported. Proceeding in seven steps from dihydrofarnesal, this synthetic route was designed to circumvent macrocyclization‐based strategies to complex, cyclized cembranoids. The described synthesis requires only six chromatographic purifications, is high yielding, and avoids protecting‐group manipulations. An X‐ray crystal structure of this fragile marine natural product was obtained.

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Section: Methodsmentioning

confidence: 99%

Short, Enantioselective Total Synthesis of Chatancin

Zhao

Maimone

2014

Angewandte Chemie

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“…These cembranoids feature two cis ‐decalin motifs possessing six or seven stereogenic centers, and are folded into an unprecedented polycyclic arrangement through a transannularly bridged hemiketal between a tertiary alcohol at C10 and a ketone at either C3 or C14. The highly congested architectures as well as the intriguing biological properties of the sarcophytin family members have stimulated several elegant total syntheses of their core structures and target molecules from the groups of Gössinger,, Deslongchamps,,– Maimone and Carreira …”

Section: Figurementioning

confidence: 99%

“…Although a biosynthetic origin of 5 based on an intramolecular Michael/aldol process was proposed, we were more intrigued by its distinctive carbon functional pattern similar to that of the sarcophytin family members. We hypothesized that a C5(10→11) Wagner–Meerwein rearrangement on the B/C rings of the sarcophytin/chatancin skeleton, which was postulated to be constructed through an transannular Diels–Alder cycloaddition of cembrane,,, might be involved in an alternative biosynthetic pathway to 5 . Therefore, a systematic investigation on the collective synthesis of these cembranoids is highly desirable to shed light on the biosynthetic relationship between their polycyclic skeletons.…”

Section: Figurementioning

confidence: 99%

Total Syntheses of (+)‐Sarcophytin, (+)‐Chatancin, (−)‐3‐Oxochatancin, and (−)‐Pavidolide B: A Divergent Approach

Xuan

Rao

et al. 2019

Angew Chem Int Ed

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A concise and divergent approach for the total syntheses of four cembrane diterpenoids, namely (+)‐sarcophytin, (+)‐chatancin, (−)‐3‐oxochatancin, and (−)‐pavidolide B, has been developed, and it also led to the structural revision of (−)‐isosarcophytin. The key steps of the strategy feature a double Mukaiyama Michael addition/elimination, a Helquist annulation, two substrate‐controlled facial‐selective hydrations, and a pinacol rearrangement. The described syntheses not only achieved these natural products in an efficient manner, but also provided insight into the biosynthetic relationship between the two different skeletons.

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“…To remedy this situation, we decided to inhibit such isomerizations by incorporating the triene into a macrolide ring, such as 24, and switch from IMDA to TADA [8] cyclization (Scheme 7). To achieve smooth macrocyclization, an (E)-enoate had to replace the former (Z)-enoate, and the former endo transition state had to be converted into the exo transition state.…”

Section: Synthesis Of Side Chainmentioning

confidence: 99%