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Proceeding Paper

Catalytic Cycloaddition of Diazo Compounds Based on Pharmacologically Significant and Natural Compounds to C60-Fullerene  †

by
Liliya L. Khuzina
,
Airat R. Tuktarov
* and
Usein M. Dzhemilev
Institute of Petrochemistry and Catalysis, Ufa Federal Research Center of the Russian Academy of Sciences, 450075 Ufa, Russia
*
Author to whom correspondence should be addressed.
Presented at the 26th International Electronic Conference on Synthetic Organic Chemistry, 15–30 November 2022; Available online: https://sciforum.net/event/ecsoc-26.
Chem. Proc. 2022, 12(1), 38; https://doi.org/10.3390/ecsoc-26-13534
Published: 14 November 2022
(This article belongs to the Proceedings of The 26th International Electronic Conference on Synthetic Organic Chemistry)
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Abstract

:
The data obtained by the authors in the field of carbon cluster chemistry, namely, the catalytic cycloaddition of diazo compounds of modern pharmacologically significant and natural compounds to C60-fullerene under the action of complex Pd–catalysts, are summarized. Cycloaddition reactions of diazoacetates, diazoamides, and diazoketones with C60-fullerene, catalyzed by Pd(acac)2–PPh3–Et3Al, with the selective formation of methano– and pyrazolinofullerenes, are new and promising classes of biologically active derivatives of C60-fullerenes.

1. Introduction

The discovery of fullerenes, a new allotropic form of carbon, is recognized as one of the amazing and most important discoveries in the science of the XX century. The interest in fullerenes and its derivatives is due to the possibility of their wide application in various fields of technology and science. At the same time, fullerene derivatives are of particular practical value for medicine. Thus, according to the literature data, functionally substituted fullerenes have high antioxidant, antitumor, and antiviral properties, and are also of interest as X-ray reducing agents [1,2,3,4,5,6,7,8,9,10,11,12]. At the time of the beginning of our research, one of the popular directions in the synthesis of organic derivatives of C60-fullerene was the Bingel–Hirsch reaction [13,14] based on the cycloaddition of in situ generated α–halocarbanions to C60-fullerene with the formation of corresponding methanofullerenes. As well as an alternative method for obtaining functionally substituted fullerenes, C60 was considered to be the cycloaddition of diaz compounds followed by thermolysis or photolysis of the resulting fullerenopyrazolines [15,16,17]. However, there was practically no information in the literature concerning the selective cycloaddition of diazo compounds of complex structure synthesized on the basis of pharmacologically significant compounds, including natural ones, to C60-fullerene in the presence of metal complex catalysts.

2. Results and Discussion

To date, we have accumulated considerable experience in the catalytic method of selective citation of C60-fullerene under the action of Pd catalysts [18,19,20,21,22]. As a result of the research, effective preparative methods for the synthesis of functionally substituted fullerenes containing known natural and biologically active compounds as a substitute have been proposed.
Diazoacetates containing cholesterol in the ester group [23], α–tocopherol, Trolox methyl esters, 20.29–dehydrobetulic, and ursolic acids [24], which have antioxidant, antitumor, and antiviral properties, were used as the initial pharmacological objects of the study. It has been shown that the above diazo compounds interact with C60-fullerene (molar ratio 5:1) in the presence of 20 mol.% of the three–component catalyst Pd(acac)2–PPh3–Et3Al, taken in a ratio of 1:4:4 at 80 °C, for 1 h in 1,2–dichlorobenzene, the corresponding methanofullerenes 1–5 are selectively formed with a yield of 60–75% (Scheme 1).
Previously, we found that a change in the ratio of the components of the Pd(acac)2–PPh3–Et3Al catalytic system, taken in a ratio of 1:4:4 to 1:2:4 in the reactions of cyclopreduction of diazoacetates to fullerene C60, leads to the predominant formation of 5,6-open cycloadducts [18,19,20,21,22]. However, in our experiments under these conditions, the interaction of diaz-derived α-tocopherol and methyl ester 20,29–dehydrobetulin with C60-fullerene, instead of the expected homofullerenes, obtained the corresponding methanofullerenes 2,3 and pyrazolinofullerenes 6 and 7 with a total yield of 58 and 65%. When the reaction temperature drops to 60 °C, pyrazollinofullerenes 6 and 7 are predominantly formed with yields of 35 and 41%, respectively (Scheme 2).
In the development of our research, and also taking into account the lack of information in the literature on the catalytic cycloaddition of diazoamides to fullerenes, we studied the possibility of catalytic cycloaddition to C60-fullerene of diazoamides synthesized on the basis of glycine and cyclohexylamine, aniline, or adamantane–containing amines [25]. As a result of the reactions, we isolated individual pyrazolinofullerenes 9–13. In the absence of a catalyst, this reaction proceeds with the formation of a mixture of methane and stereoisomerichomofullerenes [26] (Scheme 3).
It is known from the literature that pyrazolinofullerenes thermally transformed into the corresponding methanofullerenes [27,28]. By boiling the synthesized [2+3]–cycloadducts 9–13 in 1,2–dichlorobenzene for 100 h, the formation of the corresponding methanofullerenes not was found.
It is known [28] that the presence of a substituent in the α–position to the diazo group of the initial diazocompound leads to the destabilization of the pyrazolinofullerene and the formation of the corresponding [2+1]–cycloadducts. To this end, we have been involved in the reaction catalytic cycloaddition of diazoamides, synthesized from α–alanine, α–leucine, or α–methionine and cyclohexylamine. It was found that these diazoamides react with C60-fullerene in the developed conditions (40 °C, 1 h) in the presence of 20 mol.% of a three–component catalyst Pd(acac)2–PPh3–Et3Al (1:2:4) to form exclusively methanofullerenes 14–16 with a yield of 40–50% (Scheme 4).
In the development of ongoing research aimed at developing effective methods for covalent binding of C60-fullerene with modern pharmacologically significant compounds, we studied the catalytic cycloaddition to the latter of diazoketones synthesized on the basis of biologically active carboxylic acids. Trolox, a synthetic analogue of α–tocopherol, and tocopherylacetic acid, were chosen as model pharmacons. As a result of the interaction of C60-fullerene with diazoketones 17 and 19, individual methanofullerenes 18 and 20 were obtained in ~40% yield and 37%, respectively (Scheme 5).
In order to obtain previously undescribed optically active methanofullerenes [29], we implemented a catalytic cycloaddition of C60-fullerene with optically active diazoketones synthesized from L– and D– α–amino acids: alanine, leucine, methionine, tyrosine, and lysine, in which the amino group is protected with the butyloxycarbonyl (Boc) group (Scheme 6).
It was established that under the developed conditions (80 °C, 1 h, chlorobenzene) C60 interacts with diazoketones of the indicated amino acids (molar ratio 1:5) under the action of 20 mol.%Pd(acac)2–2PPh3–4Et3Al, selectively forming the corresponding methanoful-lerenes 2130 with yields of 30–77%. Unfortunately, all attempts to measure the optical angles of rotation of the polarization plane of synthesized methanofullerenes with protected amino groups were unsuccessful. Therefore, for a more reliable proof of the stereochemistry of optically active methanofullerenes, we turned to the circular dichroism (CD) method [30,31]. As expected, in the CD spectra for the synthesized enantiomers 21–30, a mirror image of the cotton effects (EC) was obtained (Figure 1).
Using the derivatizing shift reagent (tris [3–(heptafluorobutyryl)–L–camphorato]europium (III)), using the example of compound 21, we established a high enantiomeric purity (more than 98%).
Deprotection of functional groups in methanofullerenes 21–30 with CF3CO2H leads to the formation of cycloadducts 31–40 in the form of a solid powder, hardly soluble in traditional solvents for fullerenes and its derivatives (toluene, chlorobenzene, 1,2–dichlorobenzene, chloroform, carbon disulfide). In the case of compounds 31–40, we failed to record the CD spectra of their solutions in pyridine, but the saponification of the amino group associated with the chiral center made it possible to measure the optical rotation angles of the polarization plane of these methanofullerenes.
The development and implementation of new highly effective drugs is one of the priority areas of modern medicine and pharmacology. In connection with the foregoing, within the framework of this work, antioxidant activity was studied for adducts 2 and 19, as well as antitumor and anti-inflammatory activity for derivatives 3, 7, and 20.

3. Conclusions

Thus, based on the results obtained, it can be concluded that the hybrid molecules synthesized by us based on C60-fullerene and pharmacologically significant compounds are of exceptional interest for the development of a new generation of targeted drugs.

Author Contributions

Conceptualization, U.M.D., A.R.T. and L.L.K.; methodology, validation, and execution of chemistry experiments, L.L.K.; manuscript preparation, A.R.T., U.M.D. and L.L.K. All authors have read and agreed to the published version of the manuscript.

Funding

This work was supported by the Ministry of Science and Higher Education within the State Assignments of the Institute of Petrochemistry and Catalysis of RAS (FMRS–2022–0075).

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

Not applicable.

Data Availability Statement

Not applicable.

Acknowledgments

The structural studies of the synthesized compounds were performed with the use of the Collective Usage Centre “Agidel” at the Institute of Petrochemistry and Catalysis of RAS.

Conflicts of Interest

The authors declare no conflict of interest.

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Chemproc 12 00038 sch001 550
Scheme 1. Catalytic cycloaddition of diazoacetates to C60-fullerene.
Scheme 1. Catalytic cycloaddition of diazoacetates to C60-fullerene.
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Scheme 2. Synthesis of [2+3]-cycloadducts of C60-fullerene.
Scheme 2. Synthesis of [2+3]-cycloadducts of C60-fullerene.
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Scheme 3. Cycloaddition of diazoamides to C60-fullerene.
Scheme 3. Cycloaddition of diazoamides to C60-fullerene.
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Scheme 4. Cycloaddition of α–substituted diazoamides to C60-fullerene under the action of the [Pd] complex.
Scheme 4. Cycloaddition of α–substituted diazoamides to C60-fullerene under the action of the [Pd] complex.
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Scheme 5. Catalytic cycloaddition of diazoketones to C60-fullerene.
Scheme 5. Catalytic cycloaddition of diazoketones to C60-fullerene.
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Scheme 6. Catalytic cycloaddition of optically active diazoketones to C60-fullerene.
Scheme 6. Catalytic cycloaddition of optically active diazoketones to C60-fullerene.
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Figure 1. CD spectra of methanofullerenes 21–30 in chloroform with = 1.0 g/L.
Figure 1. CD spectra of methanofullerenes 21–30 in chloroform with = 1.0 g/L.
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MDPI and ACS Style

Khuzina, L.L.; Tuktarov, A.R.; Dzhemilev, U.M. Catalytic Cycloaddition of Diazo Compounds Based on Pharmacologically Significant and Natural Compounds to C60-Fullerene . Chem. Proc. 2022, 12, 38. https://doi.org/10.3390/ecsoc-26-13534

AMA Style

Khuzina LL, Tuktarov AR, Dzhemilev UM. Catalytic Cycloaddition of Diazo Compounds Based on Pharmacologically Significant and Natural Compounds to C60-Fullerene . Chemistry Proceedings. 2022; 12(1):38. https://doi.org/10.3390/ecsoc-26-13534

Chicago/Turabian Style

Khuzina, Liliya L., Airat R. Tuktarov, and Usein M. Dzhemilev. 2022. "Catalytic Cycloaddition of Diazo Compounds Based on Pharmacologically Significant and Natural Compounds to C60-Fullerene " Chemistry Proceedings 12, no. 1: 38. https://doi.org/10.3390/ecsoc-26-13534

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