Synthesis of Optically Active Bicyclic Derivatives of Nitroimidazoles

: Nitroimidazoles are characterized by a wide range of biological activity and many of them are used as therapeutics. Moreover, some bicyclic nitroimidazooxazoles show considerable potency against Mycobacterium tuberculosis. Some authors noticed that in the case of chiral derivatives of nitroimidazodihydrooxazoles, the ( R ) form shows a greater tuberculostatic activity than the ( S ) enantiomer. This work describes the procurement of new 12 enantiomeric bicyclic derivatives of nitroimidazole.

Compounds 2021, 1 146 as chiral catalysts. It is also possible that the obtained substances will have interesting biological properties.

Materials and Methods
The melting points of the resulting series of compounds were measured in open capillaries with a Kofler apparatus and are reported without correction for the measurement conditions. Proton ( 1 H NMR) and carbon ( 13 C NMR) magnetic resonance spectra were performed in DMSO-d 6 . A Varian Gemini 300VT spectrometer (Varian, Palo Alto, Santa Clara County, CA, USA) with tetramethylsilane (TMS) as an internal standard was used to record the spectra. The chemical shift values (δ) are expressed with an accuracy of ±0.01 ppm. Coupling constants are expressed in Hz. Mass spectrometry was recorded on an ADM 402 apparatus. Thin layer chromatography (TLC) was performed on aluminum plates covered with Kieselgel 60 DC-Alufol silica gel from MERCK (Darmstadt, Germany). This is a bottom-up technique using the development phase which was 9:1 (CH 2 Cl 2 :CH 3 OH) by volume mixture. The position of the spots of the synthesized products on the chromatograms was determined by observing the plates under UV light with a wavelength λ = 254 nm. Preparative column chromatography (CC) was performed by gravity using a 30 cm long, 1.5 to 2.0 cm internal diameter chromatography column packed with 70-230 Mesh silica gel from the MERCK company. Specific rotation was measured with a Perkin Elmer 243 B polarimeter (Perkin Elmer, Waltham, MA, USA) at 20 • C.

Results
In the last few decades, there has been a significant development of asymmetric synthesis methods. This is due to the confirmation that two enantiomers of a compound can exhibit various types of pharmacological activity. Sasaki et al. proved that in the case of chiral derivatives of nitroimidazodihydrooxazoles, the (R) form shows a greater tuberculostatic activity than the (S) enantiomer [18]. These researchers developed a method for the synthesis of a number of optically active 6-nitroimidazo[2,1-b]-2,3-dihydrooxazoles substituted in the 2-position ( Figure 1). The aim of this work was to obtain enantiomeric bicyclic derivatives of nitroimidazole. It is known from the chemical literature [17] that two-ring optically active compounds, which are derivatives of imidazole, can be used during asymmetric synthesis as chiral catalysts. It is also possible that the obtained substances will have interesting biological properties.

Materials and Methods
The melting points of the resulting series of compounds were measured in open capillaries with a Kofler apparatus and are reported without correction for the measurement conditions. Proton ( 1 H NMR) and carbon ( 13 C NMR) magnetic resonance spectra were performed in DMSO-d6. A Varian Gemini 300VT spectrometer (Varian, Palo Alto, Santa Clara County, CA, USA) with tetramethylsilane (TMS) as an internal standard was used to record the spectra. The chemical shift values (δ) are expressed with an accuracy of ±0.01 ppm. Coupling constants are expressed in Hz. Mass spectrometry was recorded on an ADM 402 apparatus. Thin layer chromatography (TLC) was performed on aluminum plates covered with Kieselgel 60 DC-Alufol silica gel from MERCK (Darmstadt, Germany). This is a bottom-up technique using the development phase which was 9:1 (CH2Cl2:CH3OH) by volume mixture. The position of the spots of the synthesized products on the chromatograms was determined by observing the plates under UV light with a wavelength λ = 254 nm. Preparative column chromatography (CC) was performed by gravity using a 30 cm long, 1.5 to 2.0 cm internal diameter chromatography column packed with 70-230 Mesh silica gel from the MERCK company. Specific rotation was measured with a Perkin Elmer 243 B polarimeter (Perkin Elmer, Waltham, MA, USA) at 20 °C.

Results
In the last few decades, there has been a significant development of asymmetric synthesis methods. This is due to the confirmation that two enantiomers of a compound can exhibit various types of pharmacological activity. Sasaki et al. proved that in the case of chiral derivatives of nitroimidazodihydrooxazoles, the (R) form shows a greater tuberculostatic activity than the (S) enantiomer [18]. These researchers developed a method for the synthesis of a number of optically active 6-nitroimidazo [  Enantiomerically pure epoxides are also used in the synthesis of chiral derivatives of nitroimidazotetrahydrooxazine systems, built of a 5-membered imidazole ring fused with a 6-membered cyclic oxazine system ( Figure 1) [19].
It was decided to prepare an optically active 3-hydroxy-8-nitroimidazo[5,1-b]-1,4,5,6tetrahydropyrimidine core in which a six-membered ring is connected to N-1 and C-5 atoms of nitroimidazole moiety. The preparation of two enantiomerically pure nitroimidazodihydrooxazoles was carried out according to the method known from the literature [20] describing the synthesis of racemic analogous compounds. For our purposes, (R)-(+)- Enantiomerically pure epoxides are also used in the synthesis of chiral derivatives of nitroimidazotetrahydrooxazine systems, built of a 5-membered imidazole ring fused with a 6-membered cyclic oxazine system ( Figure 1) [19].
It was decided to prepare an optically active 3-hydroxy-8-nitroimidazo[5,1-b]-1,4,5,6tetrahydropyrimidine core in which a six-membered ring is connected to N-1 and C-5 atoms of nitroimidazole moiety. The preparation of two enantiomerically pure nitroimidazodihydrooxazoles was carried out according to the method known from the literature [20] describing the synthesis of racemic analogous compounds. For our purposes, (R)-(+)-and (S)-(−)-epichlorohydrin was used for this reaction. In our previous works [21,22], on the basis of X-ray analysis results, it has been shown that the respective (S)-(−)-derivative was obtained when (S)-(+)-epichlorohydrin was used in the synthesis process and that the respective (R)-(+)-derivative was achieved when (R)-(−)-epichlorohydrin was applicated as a substrate.
In an alkaline environment, there is a reaction of intramolecular cyclization to form a bicyclic nitroimidazole derivative (Scheme 1). and (S)-(−)-epichlorohydrin was used for this reaction. In our previous works [21,22], on the basis of X-ray analysis results, it has been shown that the respective (S)-(−)-derivative was obtained when (S)-(+)-epichlorohydrin was used in the synthesis process and that the respective (R)-(+)-derivative was achieved when (R)-(−)-epichlorohydrin was applicated as a substrate.
The substrates in a molar ratio of 1:3:0.75 (4,5-dinitroimidazole: epichlorohydrin, K2CO3, respectively) were heated for 25 min in ethanol solution. On the other hand, derivatives with a methyl group in a molar ratio of 1:2:0.5 (2-methyl-4,5-dinitroimidazole, epichlorohydrin, K2CO3, respectively) were heated for 15 min in a propanol solution. After the reaction, about 60 mL of water was added to the mixture each time. The solutions were extracted with methylene chloride due to there being little or no precipitate. The organic extracts were dried with anhydrous magnesium sulfate. After evaporation of the solvent, a yellow solid residue was obtained.
Then, the focus was on obtaining new enantiomeric nitroimidazotetrahydropyrimidine bicyclic systems with the use of an aromatic amine, i.e., aniline, according to the method known from the literature [23] describing the synthesis of analogous racemic compounds. These reactions were carried out on the (R)-and (S)-methyl derivative of the nitroimidazodihydrooxazole and the (R)-and (S)-derivative devoid of the 2-methyl group (Scheme 1). The appropriate nitroimidazodihydrooxazole, aniline and K2CO3 were mixed in ethanol and heated under reflux conditions for 45 min. The possible mechanism is described in [23].
In the next stage of the research, an attempt was made to synthesize analogous enantiomeric bicyclic systems with the use of an aliphatic amine, i. e., butylamine (Scheme 1). These reactions were carried out on the (R)-and (S)-methyl derivative of nitroimidazodihydrooxazole and the (R)-and (S)-derivative devoid of the 2-methyl group. The appropriate nitroimidazodihydrooxazole and butylamine along with the K2CO3 were mixed in ethanol and heated under reflux conditions for 45 min. All synthesized compounds were subjected to spectral analysis, which confirmed their identity and structure. Detailed experimental data are presented in Appendix A section.
The m/z values for the molecular ions of these compounds are in agreement with the calculated molecular weights. In the 1 H NMR spectrum, the hydrogen atoms bound to the C-2 carbon of the imidazole ring appeared as singlets at approximately 7.6 ppm (7,8) and 7.3 ppm (9,10). The benzene ring protons in the aniline system provided the multiplet signals which were observed in the range of 7.0-7.4 ppm. The peak was located at about The substrates in a molar ratio of 1:3:0.75 (4,5-dinitroimidazole: epichlorohydrin, K 2 CO 3 , respectively) were heated for 25 min in ethanol solution. On the other hand, derivatives with a methyl group in a molar ratio of 1:2:0.5 (2-methyl-4,5-dinitroimidazole, epichlorohydrin, K 2 CO 3 , respectively) were heated for 15 min in a propanol solution. After the reaction, about 60 mL of water was added to the mixture each time. The solutions were extracted with methylene chloride due to there being little or no precipitate. The organic extracts were dried with anhydrous magnesium sulfate. After evaporation of the solvent, a yellow solid residue was obtained.
Then, the focus was on obtaining new enantiomeric nitroimidazotetrahydropyrimidine bicyclic systems with the use of an aromatic amine, i.e., aniline, according to the method known from the literature [23] describing the synthesis of analogous racemic compounds. These reactions were carried out on the (R)-and (S)-methyl derivative of the nitroimidazodihydrooxazole and the (R)-and (S)-derivative devoid of the 2-methyl group (Scheme 1). The appropriate nitroimidazodihydrooxazole, aniline and K 2 CO 3 were mixed in ethanol and heated under reflux conditions for 45 min. The possible mechanism is described in [23].
In the next stage of the research, an attempt was made to synthesize analogous enantiomeric bicyclic systems with the use of an aliphatic amine, i. e., butylamine (Scheme 1). These reactions were carried out on the (R)-and (S)-methyl derivative of nitroimidazodihydrooxazole and the (R)-and (S)-derivative devoid of the 2-methyl group. The appropriate nitroimidazodihydrooxazole and butylamine along with the K 2 CO 3 were mixed in ethanol and heated under reflux conditions for 45 min. All synthesized compounds were subjected to spectral analysis, which confirmed their identity and structure. Detailed experimental data are presented in Appendix A Section.
The m/z values for the molecular ions of these compounds are in agreement with the calculated molecular weights. In the 1 H NMR spectrum, the hydrogen atoms bound to the C-2 carbon of the imidazole ring appeared as singlets at approximately 7.6 ppm (7,8) and 7.3 ppm (9,10). The benzene ring protons in the aniline system provided the multiplet signals which were observed in the range of 7.0-7.4 ppm. The peak was located at about 5.4 ppm (7,8,9,10) or 5.2 ppm (11,12,13,14) and was assigned to the -OH group. The proton from the carbon atom bound to the hydroxyl group was visible in the form of a multiplet in the area of 4.7-4.8 ppm (7,8,9,10), and in the case of compounds substituted with an aliphatic amine (11,12,13,14), these signals were shifted towards the higher magnetic field strength and were in the range of 4.4-4.5 ppm. The remaining protons from the tetrahydropyrimidine ring were observed in the ranges of 4.3-4.4 ppm and 3.9-4.1 ppm. The spectra of compounds with a methyl group in the C-2 position of the imidazole ring showed the presence of a singlet at 2.13 ppm (13,14) or at 2.26 ppm (9,10) derived from three H atoms of the methyl group. The remaining multiplets, occurring in the range of 0.8-4.0 ppm in the spectra of the compounds (11,12,13,14), were derived from hydrogen atoms of aliphatic chains, constituting the rest of the butylamine.
In the 13 C NMR spectra, signals from the carbon atoms of the imidazole ring were usually found at about 146 (C-4), 134 (C-2) and 126 (C-5) ppm. The other peaks observed in the range of 122-140 ppm were assigned to the carbon atoms of the aromatic aniline ring (7,8,9,10). The carbon that was bonded to the secondary hydroxyl group gave a signal at about 60 ppm, while the adjacent C atoms were seen as peaks at about 55 and 44 ppm (7,8,9,10). In the spectra of compounds with an aliphatic substituent (11,12,13,14), the values characterizing this group were at 69 and 44 ppm, respectively.

Calculation of Potential Biological Activities of the Obtained Compounds Using the PASS Method and Calculation of the Partition Coefficient
The PASS program (Prediction of Activity Spectra for Substance) is widely used to assess the biological activity of substances [24]. It was developed at the Institute of Biomedical Chemistry of the Russian Academy of Sciences in the 1970s. Since then, it has been repeatedly improved and systematically updated. Access to the program is possible through the following website: www.pharmaexpert.ru/PASSOnline/ (accessed on 15 July 2021). The program predicts the occurrence of a pharmacological effect with estimated probability based on the structure of the compound in question. Using this program, we can also predict the mechanism of action, effects on fetal development (teratogenicity and embryotoxicity) and carcinogenicity. Dependencies of this kind are described on the basis of MNA (Multilevel Neighborhoods of Atoms) descriptors. The PASS program determines the potential occurrence of a specific activity (Pa) or its absence (Pi) for a testing compound based on the probability of its presence in the set of active and inactive substances of the SAR (Structure-Activity Relationship). This program consists of such elements as: characterization of the structure of a chemical compound, a database of known biologically active molecules and a mathematical model that is used to estimate the probability of a specific activity for the analyzed substance.
This database is updated based on information contained in various types of scientific publications. The values of Pa and Pi are in the range of 0-1 or 0-100%. A Pa result > 70% applies to compounds likely to show specific biological activity in vitro.
The Partition coefficient (P) is the ratio of the concentrations of substances in two different, immiscible solvents at equilibrium [25]. Most often, one of the solvents is water, the other is a hydrophobic substance, e.g., octan-1-ol. The non-ionized form of the substance is used for measurement by selecting the appropriate pH. The website www.vcclab.org/lab/alogps/start.html (accessed on 12 July 2021).was used to calculate the mean value of the partition coefficient. The partition coefficient is used to determine the lipophilicity of a substance. Values in the range of logP > 1 are considered average or good. All synthesized nitroimidazole derivatives were analyzed by the PASS C&T method and the value of the partition coefficient was calculated for them. Table 1 shows the results of the PASS analysis as well as the mean logP value.
When testing the obtained compounds, the PASS program predicts the anti-alcohol activity of compounds 7,8 with a probability higher than 70%. It must be noted, however, that most of the obtained compounds tested by the PASS method may show an effect increasing the sensitivity to radiation-the estimated radiosensitizing activity is 50-60%. It must also be noted that the program did not show significant differences in predicting biological activities for the enantiomers of a given compound. The partition coefficient values of the obtained compounds are within logP > 1. Table 1. The results of PASS analysis for obtained products (7)(8)(9)(10)(11)(12)(13)(14).

Conflicts of Interest:
The authors declare no conflict of interest.
Isolation of 3: Due to the absence of precipitate, the solution was extracted repeatedly with methylene chloride. The combined organic extracts were dried with anhydrous MgSO 4 . Evaporation of the solvent left a yellow solid residue. The separated product was recrystallized from water with the addition of charcoal. As a result, 0.509 g (25% yield) of a cream solid was obtained with mp = 151-152 • C, R f = 0.58.
Isolation of 4: A crystalline solid weighing 0.762 g was obtained. Liquids were extracted twice with methylene chloride, then dried with MgSO 4 . After evaporation of the solvent, a yellow-beige precipitate was crystallized from water with the addition of activated charcoal. As a result, 0.17 g of pure product (4) was obtained. Both precipitates had the same mp =153-154 • C, R f = 0.58, and a total weight of 0.932 g (45% yield). 1.7 g (10 mmol) of 2-methyl-4,5-dinitroimidazole (2), 1.6 mL (20 mmol) of (R)-or (S)-epichlorohydrin and 5 mL of propanol were mixed in a round bottom flask, then 0.7 g (5 mmol) of anhydrous K 2 CO 3 was added. The mixture was heated under reflux for 15 min, then poured into about 60 mL of water and allowed to stand for several hours.
Isolation of 5: A small amount of precipitate was isolated, and the solution was extracted three times with methylene chloride. The combined organic extracts were dried with anhydrous MgSO 4 . Evaporation of the solvent gave a yellow oily residue which was purified by silica gel column chromatography using: CH 2 Cl 2 :CH 3 OH (9:1) as eluent. The harvested product was crystallized from water with the addition of charcoal. A colorless precipitate of 0.19 g (8.8% yield) was obtained; mp = 114-116 • C, R f = 0.42. Isolation of 6: A small amount of precipitate was isolated, and the residue was extracted three times with methylene chloride. The combined organic extracts were dried with anhydrous MgSO 4 . After evaporation of the solvent, a yellow oily residue was obtained which was purified by column chromatography. The eluent was CH 2 Cl 2 :CH 3 OH (98:2). As a result, 0.16 g (7.4% yield) of colorless product (6) with mp = 115-117 • C, R f = 0.42 was obtained.