Synthesis and Diversification of Chiral Spirooxindoles via Organocatalytic Cascade Reactions †
División de Ciencias Naturales y Exactas, Universidad de Guanajuato, Noria Alta, Guanajuato 36050, Gto., Mexico
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Authors to whom correspondence should be addressed.
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Presented at the 27th International Electronic Conference on Synthetic Organic Chemistry (ECSOC-27), 15–30 November 2023; Available online: https://ecsoc-27.sciforum.net/ .
Chem. Proc. 2023, 14(1), 37; https://doi.org/10.3390/ecsoc-27-16100
Published: 15 November 2023
(This article belongs to the Proceedings of 27th International Electronic Conference on Synthetic Organic Chemistry)
Abstract
:The synthesis of chiral spirooxindoles through different amino catalytic activation modes is described herein. Several alkenylisatins were obtained from the Knoevenagel reaction of isatin and activated methylene derivatives containing electron withdrawing groups such as ethyl cyanoacetate. A spirooxindole derivative was obtained from the oxa-Michael-Michael reaction between one of the synthesized alkenylisatins and 2-hydroxycinnamaldehyde. Currently, new methodologies that allow access to spirooxindole scaffolds are being explored, mainly though Diels-Alder reactions between 2-methylenindolin-2-ones and aldehydes via the trienamine activation mode. The following cascade reactions will be explored in the future to obtain the proposed polycyclic spirooxindole derivatives.
1. Introduction
The search for bioactive compounds relies on the ability of synthetic chemists to efficiently prepare molecule libraries with structural, stereochemical and skeletal diversity. Evans coined the term “privileged scaffolds” in the 1980s [1]. These synthetic frameworks can be identified by either their high affinity towards several receptors or by the fact that multiple molecules containing said framework are bioactive. At first, privileged scaffolds were only found within the structure of important natural products; nowadays there are a couple different ways of getting to and determining the activity of new privileged scaffolds [2].
In general, there are two types of methodologies for the obtention of biologically important compounds, TOS, and DOS. Originally, TOS (Target-Oriented Synthesis) was the only methodology used in the search for bioactive compounds though retrosynthetic analysis. Later, DOS (Diversity-Oriented Synthesis) replaced it in many instances; mainly due to its higher ability to create diversity and, therefore, have a higher probability of finding a molecule with promising biological activity. Recently, a new strategy for developing molecule libraries was described; ApDOS (Aminocatalytic privileged Diversity-Oriented Synthesis) which involves a diversification pathway through the aminocatalytic mode instead of the skeletal building blocks [3].
Spirooxindoles are oxindole derivatives that contain a ring fused in a spiro manner at the C-3 atom. Spirooxindoles are a particularly important class of organic moieties due to their significant biological activities, such as anti-tumor, antiviral and antibacterial activities Figure 1 [4]. The synthesis of these heterocycles is a challenge that has especially interested chemists since the last decade.
The synthesis of chiral spirooxindoles through different amino catalytic activation modes is described herein. Once obtained, the spirooxindoles would be submitted to a cascade sequence of reactions (nucleophilic addition/elimination/Pictet–Spengler) to yield polycyclic derivatives such as 3 (Scheme 1).
2. Methods
Proton (1H) NMR spectra were recorded on aBruker UltraShield Plus 500 MHz, Avance III HD (equipment sourced from Bruker Biospin AG; Industriestrasse 26; CH-8117 Fällanden, Switzerland). Flash column chromatography was performed on silica gel using hexane/ethyl acetate as the mobile phase. 3-Methylenindolin-2-ones 7a and 7b were synthesized using the reported conditions [5,6].
3. Results and Discussion
Starting from triptamine and ethyl cyanoacetate, amide 4 was formed with an 80% yield. Then, isatin and 4 were allowed to react under the Knoevenagel condensation conditions reported [5]. However, the desired product (2) was not obtained under these conditions, probably because the nitrogen in isatin may be exerting unwanted side reactions and preventing the formation of 2. Therefore, isatin was protected to N-benzyl-isatin in 85% yield. This new isatin derivative reacted, hoping for Knoevenagel condensation under modified conditions from Tiwari’s report [6]. 3-Methylenindolin-2-one derivative 6 was obtained with a 12% yield (Scheme 2).
Similarly, Knoevenagel condensation between isatin and ethyl cyanoacetate was performed under two different conditions to yield the two isomers Z (7a) and E (7b). Both isomers were used in different aminocatalytic processes to yield spirooxindoles.
The Diels–Alder reaction between dienophile 7a, aldehyde 8 and Jørgensen–Hayashi catalyst was performed. A product was isolated, but its characterization has not been possible as of now (Scheme 3A).
The aminocatalytic oxa-Michael-Michael reaction between 7b and o-hydroxy cinnamaldehyde 9 yielded 16% of the spirooxindole derivative 11 (Scheme 3B).
4. Conclusions
Spirooxindoles are an important class of privileged structures. The search for new synthetic pathways for their constriction has been on the rise within the synthetic organic chemists’ community since the last decade. A new spirooxindole derivative was obtained through aminocatalytic activation. The synthesis and diversification of spirooxindole derivatives through Diels–Alder and oxa-Michael-Michael reactions is underway.
Author Contributions
Conceptualization, D.C.C. and C.V.G.; methodology, J.N.V.; validation, D.C.C. and C.V.G.; formal analysis, J.N.V.; investigation, J.N.V.; resources, D.C.C. and C.V.G.; data curation, J.N.V.; writing—original draft preparation, J.N.V.; writing—review and editing, D.C.C. and C.V.G.; supervision, D.C.C. and C.V.G.; project administration, D.C.C. and C.V.G.; funding acquisition, D.C.C. and C.V.G. All authors have read and agreed to the published version of the manuscript.
Funding
This research was funded by DAIP-UG grants number 54/2023 and 55/2023.
Institutional Review Board Statement
Not applicable.
Informed Consent Statement
Not applicable.
Data Availability Statement
The data presented in this study are available in the article.
Acknowledgments
We would like to thank CONAHCyT for grant number 824881.
Conflicts of Interest
The authors declare no conflict of interest.
References
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Figure 1.
Examples of spirooxindoles.
Scheme 1.
Project outline.
Scheme 2.
3-Methylenindolin-2-one synthesis.
Scheme 3.
3-Methylenindolin-2-one synthesis and spirooxindole formation. (A) Knoevenagel condensation between isatin and ethyl cyanoacetate yielded 7a, and subsequent organocatalytic Diels-Alder reaction to yield spirooxindole 10. (B) Knoevenagel condensation between isatin and ethyl cyanoacetate yielded 7b, and organocatalytic oxa-Michael-Michael reaction for the obtention of spirooxindole 11.
Scheme 3.
3-Methylenindolin-2-one synthesis and spirooxindole formation. (A) Knoevenagel condensation between isatin and ethyl cyanoacetate yielded 7a, and subsequent organocatalytic Diels-Alder reaction to yield spirooxindole 10. (B) Knoevenagel condensation between isatin and ethyl cyanoacetate yielded 7b, and organocatalytic oxa-Michael-Michael reaction for the obtention of spirooxindole 11.
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MDPI and ACS Style
Navarro Vega, J.; Cruz Cruz, D.; Villegas Gómez, C. Synthesis and Diversification of Chiral Spirooxindoles via Organocatalytic Cascade Reactions. Chem. Proc. 2023, 14, 37. https://doi.org/10.3390/ecsoc-27-16100
AMA Style
Navarro Vega J, Cruz Cruz D, Villegas Gómez C. Synthesis and Diversification of Chiral Spirooxindoles via Organocatalytic Cascade Reactions. Chemistry Proceedings. 2023; 14(1):37. https://doi.org/10.3390/ecsoc-27-16100
Chicago/Turabian StyleNavarro Vega, Jessica, David Cruz Cruz, and Clarisa Villegas Gómez. 2023. "Synthesis and Diversification of Chiral Spirooxindoles via Organocatalytic Cascade Reactions" Chemistry Proceedings 14, no. 1: 37. https://doi.org/10.3390/ecsoc-27-16100
