Synthesis of Bridged Five-Membered Ring Systems by Type II [3 + 2] Annulation of Allenylsilane-ene PDF

Summary

This article details a novel approach to synthesize bridged five-membered ring systems. The method involves a type II [3 + 2] annulation reaction of allenylsilane-ene. The synthesis of natural products, including (+)- and (-)-strepsesquitriol and pierisjaponol D, is also outlined in the work.

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Synthesis of Bridged Five-Membered Ring Systems by Type II [3 + 2]
Annulation of Allenylsilane-ene
Ling-Zi Li, Yu-Rou Huang, Zi-Xun Xu, Hong-Sen He, Hong-Wei Ran, Ke-Yu Zhu, Jing-Chun Han,*
and Chuang-Chuang Li*
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ABSTRACT: The first type II intramolecular [3 + 2] annulation of allenylsilane-ene has been achieved, enabling diastereoselective
and efficient construction of synthetically challenging bridged five-membered ring systems such as bicyclo[3.2.1]. This mild and
direct process shows a broad substrate scope and is highly stereospecific. Particularly, this work represents the first stereoselective
method for the direct synthesis of bicyclo[3.2.1] ring systems from acyclic precursors. Additionally, the first asymmetric total
syntheses of (+)- and (−)-strepsesquitriol, and the efficient formation of the synthetically challenging tetracyclic core of
pierisjaponol D are achieved by this type II [3 + 2] annulation reaction.

B ridged ring systems (Figure 1) are strained and widely
found in natural products with important biological
activities.1 For example, taxol contains a bridged six-membered
membered ring systems directly (Scheme 1). Specifically,
compound 1 with an allenylsilane linked to an enone moiety
was designated as a practical cascade cyclization precursor. We
ring system.2 Interestingly, camphor, longifolene, ent-kaurene, proposed that an intramolecular conjugate addition of the
and ajmaline have bridged five-membered ring systems allenylsilane to the enone could occur when 1 was treated with
(highlighted in red, Figure 1A). Type II intramolecular a Lewis acid (LA), giving intermediate A, in which the sp2
cycloaddition is an efficient strategy for the synthesis of carboncation is stabilized by β-silicon effect. Intermediate A
bridged ring systems.3 Shea type II intramolecular Diels−Alder could go through a [1, 2]-silyl shift to generate intermediate B.
cycloadditions (with a dienophile connected at the 2-position The enolate of B could undergo intramolecular SN2-type
of the diene) are effective for producing bridged six-membered
nucleophilic attack to afford the desired compound 2 with a
ring systems4 (Figure 1B). However, no bridged five-
bridged five-membered ring. However, the formation of the
membered ring systems have yet been accessed by Shea’s
approach or other type II intramolecular cycloadditions strained bridged five-membered ring would be energetically
(including Wender-[4 + 4],5a Davies-[4 + 3],5b Li-[5 + 2],5c unfavorable. There have been no reports of the [3 + 2]
and Xu-[4 + 4]5d), because it requires the formation of an annulation of allenylsilane-enes to construct bridged rings.8
unfavorable strained bridgehead double bond (Bredt’s rule).6 Conversely, intermediate A or B could undergo competitive
Furthermore, there are few reactions available for the single- desilylation to give the undesired byproduct C. These factors
step synthesis of bridged five-membered ring systems (such as make the desired type II intramolecular [3 + 2] annulation of 1
bicyclo[3.2.1]) from acyclic precursors.7 Therefore, it is still challenging. Furthermore, it was unclear if the chirality of the
important to develop new and efficient strategies to make these allenylsilane in 1 would transfer to the final product 2.
attractive bridged five-membered ring systems. We began our investigation by preparing the linear substrate
Danheiser et al.8 described a notable intermolecular [3 + 2] 1a (Scheme 2), which was easily accessed in three steps from a
annulation of allenylsilanes. However, this reaction provided commercially available compound (see the Supporting
only a single five-membered ring or a fused five-membered ring Information (SI) for details). After optimization, treatment
system (Figure 1C). Surprisingly, only one example of of 1a with TiCl4 (1.5 equiv.) in DCM at − 78 °C produced the
intramolecular [3 + 2] annulation of allenylsilane-enes has desired product 2a as a single diastereomer in 79% isolated
been reported since 1981.9 Additionally, no reported intra- yield. The structure of 2a was confirmed by X-ray crystallo-
molecular [3 + 2] annulations of allene-enes gave bridged five- graphic analysis of its derivative 2a′ (see SI for details).
membered ring systems.10 In our continuing efforts toward the Interestingly, this reaction constructed a bridged
total synthesis of natural products with bridged ring systems,11
we herein present the first type II intramolecular [3 + 2]
annulation of allenylsilane-ene, which enables the first Received: July 10, 2024
asymmetric total synthesis of strepsesquitriol and the efficient Revised: August 18, 2024
construction of the synthetically challenging tetracyclic core of Accepted: August 27, 2024
pierisjaponol D (Figure 1D).
Initially, we anticipated that the type II intramolecular [3 +
2] annulation of allenylsilane-enes would deliver bridged five-

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Figure 1. A. Selected natural products with bridged ring systems. B. Type II intramolecular Diels−Alder cycloaddition. C. Intermolecular [3 + 2]
annulation of allenylsilaness. D. Type II intramolecular [3 + 2] annulation of allenylsilane-ene and asymmetric total synthesis of strepsesquitriol.

Scheme 1. Proposed Type II Intramolecular [3 + 2] the following investigation. We then turned our attention to
Annulation of Allenylsilane-ene to Access Bridged Five- the substituted group of allenylsilane. The reactions proceeded
Membered Ring Systems successfully with alkyl-substituted allenylsilanes, giving a series
of functionalized bicyclo[3.2.1]octanes 2d−2g in good yields
(even of 2g with a bulky tertiary butyl substituent). Pleasingly,
the all-carbon quaternary stereocenter was constructed from α-
alkyl- or α-aryl-substituted enones, giving products 2h−2k in
77%−85% yield. Of note was compound 2l with two adjacent
quaternary carbons, which formed with an excellent yield of
87%. Additionally, a tetrasubstituted allenylsilane substrate
gave compound 2m, which possessed an all-carbon quaternary
stereocenter, in 62% yield. These results are important because
the construction of an all-carbon quaternary stereocenter is
very challenging.12 Interestingly, when substrate 1n with α, β-
substituted enone was treated with Me2AlCl (2.5 equiv.)
instead of TiCl4, it formed the more functionalized product 2n
with three stereocenters diastereoselectively.
The synthesis of products with an external carbonyl group
on the bridged ring system was then investigated using this
method (Scheme 2B). The reactions proceeded well with
alkyl-substituted ketones, giving a series of functionalized
products 2o−2u in moderate or good yields. The substrates
with cyclic aliphatic- or aryl-substituted ketones were all
tolerated and the desired products 2v−2ee were obtained in
moderate yields. The reactions of substrates with conjugated or
unconjugated alkenyl-substituted groups proceeded well,
giving desired products 2ff−2hh. Substrate 1ii (see its
bicyclo[3.2.1]octane ring system, two new C-C bonds, one structure in Scheme 3A) with a ketal group reacted in the
new C-Si bond, and two stereogenic centers in a single step. presence of TiCl4 (3.0 equiv.) in DCM, giving dicarbonyl
Consequently, the generality of this approach was explored product 2ii in 72% yield. The structures of 2m, 2n, 2aa, and 2ii
using different substrates to construct functionalized bridged were established by X-ray crystallographic analyses of their
five-membered ring systems, as shown in Scheme 2A. We corresponding derivatives (see SI for details), confirming the
found that allenylsilanes with different silyl groups provided generality of this approach.
products 2a−2c in good yields. Considering stability and steric Next, we sought to determine whether the chirality of the
factors, TES was selected as the silyl group of allenylsilane in allenylsilane could be transferred to the final product (Scheme
B https://doi.org/10.1021/jacs.4c09384
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Scheme 2. Substrate Scopea,b Scheme 3. Stereospecific Type II [3 + 2] Annulation of
Chiral Allenylsilane-enes and Synthesis of the Tetracyclic
Core of Pierisjaponol D

a
Conditions: 1 (0.1−0.6 mmol), TiCl4 (1.5 equiv.), DCM (0.05 M), annulation of optically active (−)-1ii (96% ee) and (+)-1ii
0.5 h. bIsolated yield. cMe2AlCl (2.5 equiv.) was used.
(97% ee) also proceeded smoothly to give (−)-2ii (97% ee)
and (+)-2ii (94% ee, 15 g scale), respectively. These results
3A). Pleasingly, optically active (−)-1j (97% ee, see SI for show that this type II intramolecular [3 + 2] annulation
details) underwent a stereospecific type II [3 + 2] annulation, reaction is highly stereospecific and that the chirality of the
giving (−)-2j as a single diastereomer in 77% yield and 98% ee. substrate transfers to the product. In our previous work, we did
The structure of (−)-2j was confirmed by X-ray crystallog- DFT calculation to explain the chirality transfer process and
raphy of its derivative. Furthermore, the desired [3 + 2] the results are consistent.9a In this work, the experiment results
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show that the electrophile is always anti with respect to carbon- Scheme 4. Asymmetric Total Synthesis of (+)- and
silicon bond as our previous work did, which determines the (−)-Strepsesquitriol
chirality of the product. This result is due to steric and
electronic nature of the allenylsilane (see SI for details).13
Pleasingly, the cascade DMP-oxidation/[3 + 2] annulation
reaction of compound 3 (dr = 1:1) proceeded smoothly to
afford (±)-2ii in 83% overall yield without using a Lewis acid
(Scheme 3B). This outcome is likely due to the presence of
dicarbonyl groups in intermediate 3a, which renders the
double bond of the conjugate acceptor extremely electronically
deficient. Additionally, optically active (+)-3 (97% ee) also
underwent a stereospecific cascade oxidation/[3 + 2]
annulation to give (+)-2ii (97% ee, see SI for details).
With compound (±)-2ii in hand (Scheme 3C), we
investigated the practical utility of our strategy by synthesizing
the tetracyclic core of pierisjaponol D.14 Treatment of (±)-2ii
with allenic boronate 4 and ZnEt2 followed by TBS protection
provided 5 as a single diastereomer.15 Diastereoselective 1,2-
addition of (4-(trimethylsilyl)but-3-yn-2-yl)lithium reagent to
5 in the presence of LaCl3·2LiCl gave 6 in 94% yield.16 The
stereochemical selectivity is controlled by the steric hindrance
of the substrates in the above reactions (see SI for details).
Then, compound 6 underwent the desired intramolecular
Pauson−Khand reaction with catalytic [RhCl(CO)2]2 under
CO atomsphere to deliver 7 in 73% yield.17 Dimethylation of 7
using NaH and MeI provided 8 in 94% yield. The structure of
8 was confirmed by X-ray crystallographic analysis. Pleasingly,
compound 8 contains the synthetically challenging [5−7−6−
5] tetracyclic structure of pierisjaponol D, including the
desired functional groups (highlighted in red). Accordingly,
this work provides a concise approach toward the total
synthesis of pierisjaponol D.
We then conducted the asymmetric total synthesis of
(+)-strepsesquitriol (Scheme 4), which shows inhibitory
activity against lipopolysaccharide-induced TNFα produc-
tion.18 Structurally, (+)-strepsesquitriol is a rearranged
went through ozonolysis with O3 and C-O bond cleavage with
zizaane-type sesquiterpenoid19 and has a trihydroxytricyclo-
SmI2 to provide (+)-12 in 64% yield over two steps. Treatment
[6.2.1.01,5]undecane core including a bridged bicyclo[3.2.1]-
of (+)-12 with NaH/MeI followed by diastereoselective 1,2-
octane ring system. Additionally, (+)-strepsesquitriol contains
four contiguous quaternary carbons, including two all-carbon addition of MeLi to the ketone group afforded (+)-13 in 55%
quaternary centers at C1 and C9 and two oxygenated overall yield. Finally, hydrogenative removal of the two benzyl
quaternary stereocenters at C5 and C10. Thus, (+)-strep- groups of (+)-13 provided (+)-strepsesquitriol in 95% yield,
sesquitriol poses a considerable synthetic challenge and its completing the asymmetric total synthesis. Interestingly, we
total synthesis has not yet been reported. also achieved the first asymmetric total synthesis of
The synthesis of (+)-strepsesquitriol commenced with (−)-strepsesquitriol using (−)-2ii (97% ee) as the starting
(+)-2ii. In the presence of LaCl3·2LiCl, sequential chemo- material by following a similar sequence to that shown in
and diastereoselective 1,2-additions of vinylmagnesium bro- Scheme 4. The syntheses of both (+)- and (−)-strepsesquitriol
mide and isopropenylmagnesium bromide to the aldehyde and will enable study of their structure−activity relationship.
ketone groups of (+)-2ii, respectively, gave (+)-9 in 63% yield. In summary, the first type II intramolecular [3 + 2]
Treatment of (+)-9 with Grubbs II catalyst, followed by TES annulation of allenylsilane-ene was achieved. This reaction
protection of the secondary hydroxyl group and diastereose- enables diastereoselective and efficient construction of
lective hydrogenation of the trisubstituted alkene with Pd/C synthetically challenging and multifunctionalized bridged five-
and H2 provided (+)-10 in 73% overall yield. It is worth membered ring systems, such as bicyclo[3.2.1]. This mild and
mentioning that the TES protection on C2-OH was removed direct transformation displays a broad substrate scope and is
under the acidic conditions of Pd/C/H2 reaction. The absolute highly stereospecific. Notably, this work represents the first
structure of (+)-10 was confirmed by X-ray crystallography. stereoselective approach for the direct synthesis of bicy-
Notably, direct hydrogenation of the trisubstituted alkene with clo[3.2.1] ring systems from acyclic precursors. Furthermore,
an unprotected secondary alcohol provided a mixture of the first asymmetric total synthesis of (+)- and (−)-strep-
diastereomers with a 1.8:1 ratio. Removal of the silyl group of sesquitriol and the efficient construction of the synthetically
(+)-10 with TFA and Bn protection of the two hydroxyl challenging tetracyclic core of pierisjaponol D were achieved
groups gave (+)-11 in 68% overall yield. Compound (+)-11 by this type II [3 + 2] annulation reaction. This approach
underwent SeO2-mediated allylic oxidative rearrangement to could be extended to the total synthesis of ent-kauranes and
provide a product with an exocyclic double bond. This product diterpenoid alkaloids with bicyclo[3.2.1] ring systems.20
D https://doi.org/10.1021/jacs.4c09384
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*
ASSOCIATED CONTENT
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ACKNOWLEDGMENTS
This paper is in memory of Professor Li-Xin Dai. This work
The Supporting Information is available free of charge at was supported by the National Natural Science Foundation of
https://pubs.acs.org/doi/10.1021/jacs.4c09384. China (22225102 and 22371114), National Key R&D
Detailed experimental procedure, 1H NMR and 13
C Program of China (No. 2022YFE0205500), the Guangdong
NMR spectra, X-ray data information (PDF) Basic and Applied Basic Research Foundation
(2022A1515011198), Shenzhen Bay Laboratory
Accession Codes (SZBL2021080601005 and Shenzhen Bay Scholars), and the
CCDC 2352592−2352596, 2352598, 2352644, 2352646, and Shenzhen Science and Technology Program
2364729−2364730 contain the supplementary crystallographic (JCYJ20220818100603008, JCYJ20210324104408023, and
data for this paper. These data can be obtained free of charge JCYJ20210324105202006).
via www.ccdc.cam.ac.uk/data_request/cif, or by emailing
[email protected], or by contacting The Cam-
bridge Crystallographic Data Centre, 12 Union Road,
Cambridge CB2 1EZ, UK; fax: +44 1223 336033.
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