Molecular Recognition of Imidazole Derivatives by Co(III)-Porphyrins in Phosphate Buffer (pH = 7.4) and Cetylpyridinium Chloride Containing Solutions

By means of spectrophotometric titration and NMR spectroscopy, the selective binding ability of the Co(III)-5,15-bis-(3-hydroxyphenyl)-10,20-bis-(4-sulfophenyl)porphyrin (Co(III)P1) and Co(III)-5,15-bis-(2-hydroxyphenyl)-10,20-bis-(4-sulfophenyl)porphyrin (Co(III)P2) towards imidazole derivatives of various nature (imidazole (L1), metronidazole (L2), and histamine (L3)) in phosphate buffer (pH 7.4) has been studied. It was found that in the case of L2, L3 the binding of the “first” ligand molecule by porphyrinates Co(III)P1 and Co(III)P2 occurs with the formation of complexes with two binding sites (donor–acceptor bond at the center and hydrogen bond at the periphery of the macrocycle), while the “second” ligand molecule is added to the metalloporphyrin only due to the formation of the donor–acceptor bond at the macrocycle coordination center. The formation of stable complexes with two binding sites has been confirmed by density functional theory method (DFT) quantum chemical calculations and two-dimensional NMR experiments. It was shown that among the studied porphyrinates, Co(III)P2 is more selective towards to L1-L3 ligands, and localization of cobalt porphyrinates in cetylpyridinium chloride (CPC) micelles does not prevent the studied imidazole derivatives reversible binding. The obtained materials can be used to develop effective receptors for recognition, delivery, and prolonged release of drug compounds to the sites of their functioning. Considering that cetylpyridinium chloride is a widely used cationic biocide as a disinfectant, the designed materials may also prove to be effective antimicrobial agents.


Introduction
Molecular recognition processes, in which one molecule ("host" or receptor) recognizes and binds another molecule ("guest" or substrate) to form a system due to intermolecular interactions find broad application in the design of multifunctional devices for new molecular technologies. Examples are the separation of mixtures of closely related compounds and enantiomers, gas or toxic substances storing, stabilization of highly reactive compounds, the prolonged release of drugs in the conditions close to the physiological and control of reaction routes by including such particles into molecular reactors or channels [1][2][3][4][5].
the recognition ability of two hydrophilic Co(III)-porphyrins with hydroxyl groups in the phenyl rings of the macrocycle towards to imidazole derivatives-unsubstituted imidazole (L1), metronidazole (L2), and histamine (L3) due to possibility of formation additional hydrogen bonds between the functional groups of the receptor (porphyrin molecule) and substrate (imidazole derivative). Structures of the Co(III)-porphyrins bis-axial complexes with the ligands L are depicted in Figure 1.
The complexation processes in phosphate buffer (pH = 7.4) imitating blood plasma has been studied. We previously found that the more effective method of influence and control of binding and elimination processes of hydrophilic Co(III)-porphyrins with various organic bases in aqueous media is micellization, namely the localization to the outer layer (it may be intercalated among the CPC chains, most likely with the pyridinium group extending into the polar headgroup region of the micelle) surfactant micelle [21], which gives them new properties. In this regard, the investigation of the recognition ability of the studied Co(III)-porphyrins hydroxy derivatives were carried out both in phosphate buffer (pH = 7.4) and in solutions containing cetylpyridinium chloride (CPC). The complexation processes in phosphate buffer (pH = 7.4) imitating blood plasma has been studied. We previously found that the more effective method of influence and control of binding and elimination processes of hydrophilic Co(III)-porphyrins with various organic bases in aqueous media is micellization, namely the localization to the outer layer (it may be intercalated among the CPC chains, most likely with the pyridinium group extending into the polar headgroup region of the micelle) surfactant micelle [21], which gives them new properties. In this regard, the investigation of the recognition ability of the studied Co(III)-porphyrins hydroxy derivatives were carried out both in phosphate buffer (pH = 7.4) and in solutions containing cetylpyridinium chloride (CPC).

Formation of the Co(III)P bis-Axial Complexes with Imidazole Derivatives
Co(III)-complexes of water-soluble tetraarylporphyrins [Co(III)P] are characterized by bis-axial coordination of both nitrogen and oxygen-containing small organic molecules, in which there is one additional ligand coordinated on each sides of the macrocycle plane [18,19]. Earlier, we studied the processes of Co(III)-tetra(carboxyphenyl)porphyrin (Co(III)TPPC) and Co(III)-tetra(sulfophenyl)porphyrin (Co(III)TPPS) complexation with various drugs based on nitrogen-containing heterocycles [20,21].
Co(III)P1 and Co(III)P2 form bis-aqua complexes in aqueous media at pH 7.4 similar to Co(III)TPPC and Co(III)TPPS. The replacement process of aqua-groups with organic bases goes sequentially in two stages: Co(III)P-(H 2 O) 2 + L ↔ Co(III)P-(L)(H 2 O) (1a) Co(III)P-(L)(H 2 O) + L ↔ Co(III)P-(L) 2 (1b) Each stage of the process is accompanied by its own characteristic spectral changes in the UV-Vis spectra of the reaction system. In particular, the replacement of the "first" water molecule with the imidazole molecule is characterized by a slight decrease in the intensity of the Soret band in the UV-Vis spectrum and its red shift by 3.5 nm. The replacement of the second water molecule was accompanied by less noticeable spectral changes ( Figure 2b). The calculated constants of water molecules replacement for the imidazole compounds (K 1 and K 2 ) are listed in Table 1 and Figure 3. The bis-axial complexes formation is confirmed by the 1 H NMR and mass spectrometry data. The spectral changes observed with the replacement of water molecules by imidazole-containing drugs are similar to those shown in Figure 2.
The mono-axial complexes Co (III)P-(L) (H 2 O) are formed at a 1:1 concentration ratio of the reagents. A small excess of imidazoles is required to replace the "second" water molecule. It was found that the imidazole derivatives L2, and L3 form more stable monoaxial complexes with the Co (III)P(1-2), in comparison with the unsubstituted imidazole L1. This is probably due to the formation of additional binding centers between the porphyrinate and the ligand-hydrogen bonds, namely between the porphyrin hydroxyl group and the carbonyl oxygen atom of the ligand L3 or between the porphyrin hydroxyl group and the oxygen atom of the nitro group of the ligand L2.

Formation of the Co(III)P bis-Axial Complexes with Imidazole Derivatives
Co(III)-complexes of water-soluble tetraarylporphyrins [Co(III)P] are characte by bis-axial coordination of both nitrogen and oxygen-containing small organic cules, in which there is one additional ligand coordinated on each sides of the macro plane [18,19]. Earlier, we studied the processes of Co(III)-tetra(carboxyphenyl)porp (Co(III)TPPC) and Co(III)-tetra(sulfophenyl)porphyrin (Co(III)TPPS) complexation various drugs based on nitrogen-containing heterocycles [20,21].
Co(III)P1 and Co(III)P2 form bis-aqua complexes in aqueous media at pH 7.4 si to Co(III)TPPC and Co(III)TPPS. The replacement process of aqua-groups with or bases goes sequentially in two stages: Each stage of the process is accompanied by its own characteristic spectral ch in the UV-Vis spectra of the reaction system. In particular, the replacement of the " water molecule with the imidazole molecule is characterized by a slight decrease intensity of the Soret band in the UV-Vis spectrum and its red shift by 3.5 nm. T placement of the second water molecule was accompanied by less noticeable sp changes ( Figure 2b). The calculated constants of water molecules replacement fo imidazole compounds (K 1 and K 2 ) are listed in Table 1 and Figure 3. The bis-axial plexes formation is confirmed by the 1 H NMR and mass spectrometry data. The sp changes observed with the replacement of water molecules by imidazole-conta drugs are similar to those shown in Figure 2.     The mono-axial complexes Co (III)P-(L) (H2O) are formed at a 1:1 concentrati of the reagents. A small excess of imidazoles is required to replace the "second molecule. It was found that the imidazole derivatives L2, and L3 form mor mono-axial complexes with the Co (III)P (1-2), in comparison with the unsubstitu idazole L1. This is probably due to the formation of additional binding centers b the porphyrinate and the ligand-hydrogen bonds, namely between the porphy droxyl group and the carbonyl oxygen atom of the ligand L3 or between the po hydroxyl group and the oxygen atom of the nitro group of the ligand L2.
In the reports [13][14][15][16][17], devoted to the formation of supramolecular porphyr plexes with several binding points, the contributions of axial coordination energy In the reports [13][14][15][16][17], devoted to the formation of supramolecular porphyrin complexes with several binding points, the contributions of axial coordination energy (∆G axial coord. ) and H-bonds (∆G HB ) to the total energy of the complex formation were estimated. A quantitative measure of increase in stability of the complex "porphyrinate-polyfunctional ligand" due to additional bond formation is K 1 /K 1,o , where K 1,o is a stability constant of an axial metalloporphyrin complex with one binding center, and K 1 is a stability constant of an axial metalloporphyrin complex containing additional binding center (or centers) ( Table 2). N p -nitrogen atom of Co(III)P. N j -nitrogen atom of imidazole ligand (L 2 and L 3 ).
As seen from the Table 1 The selectivity of mono-axial binding of histamine, metronidazole, and their precursor imidazole with Co(III)P1, Co(III)P2 is confirmed by both quantum-chemical calculations and NMR spectroscopy data. The optimization of structures by quantum-chemical calculations showed that a partial transfer of the electron pair of the Nj-atom to the empty orbitals of the Co-atom (LP N → LP × Co) is observed in the Co(III)P1, Co(III)P2 complexes with two axial ligands (L2 and L3). According to the natural bond orbital (NBO), the stabilization energy of the Co-Nj bond was 214.6-238.5 kJ/mol, and the corresponding charge transfer value was 0.215-0.259 e ( Table 2).
The calculation results showed that a decrease in the Co-Nj bond length led to an increase in the binding energy E st (Co-Nj) ( Table 2). At the same time, an inverse relationship is observed between the length of the Co-Nj bonds and the binding energy of porphyrin with the ligand E int ( Table 2). The reason for this dependence is an increase in the stability of the Co(III)P-L complex not only due to Co-L donor-acceptor interactions in these complexes, but also due to the formation of additional hydrogen bonds. However, the saddle-like structure of the macrocycle led to the formation of only one additional hydrogen bond between the hydroxyl group in the phenyl ring of the porphyrinate and the oxygen atom of the carboxyl group of L2 or nitro group of L3 ( Figure 4).
Thus, the strongest binding of the ligand to porphyrin (E int ) corresponded to the smaller value of the hydrogen bond length between them (r(OH . . . O = L)). Therefore, the strongest bonds are formed when porphyrinate Co(III)P2 binds the metronidazole (L2). The lengths of the formed hydrogen bond and the energies of the intermolecular interaction of the bis-axial complex are in good agreement with the values of the energies of hydrogen bonds determined from the formation constants of the Co(III)P-(L)(H 2 O) complexes ( Figure 5).
For the analysis of the chemical structure of Co(III)P(1-2) and its complexes with L1-L3, 1 H NMR spectra were obtained as shown in the Figure 4, which are the superposition (convolution) of spectra, relating to a certain range of self-diffusion coefficients, which these bonds are characterized [17,[27][28][29][30][31]. Such superposition is obtained by a projection of a pseudo-two-dimensional spectrum of the diffusive ordered DOSY spectroscopy on the set range of self-diffusion coefficients. The analysis of the obtained ranges ( Figure 5) showed a change in the values of chemical shifts and a shape of the signals of characteristic groups that are usually observed as a result of the formation of complexes with ligands. In particular, formation of hydrogen bonds between one OH group of the porphyrin Co(III)P1 and oxygen atom of carboxy-group of the ligand L3 or oxygen atom of nitro-group of the ligand L2 was evidenced by the up-field shift of signals of the porphyrin OH groups, which were involved in the hydrogen bonds formation (∆ = 1.14 ppm in case of the complexes Co(III)P1(L 3 )(H 2 O), and 2.60 ppm in case of the Co(III)P1(L 2 )(H 2 O)), compared to the OH group proton of the Co(III)P1. The protons of another OH group of the Co(III)P1, which are not involved in the formation of the considered hydrogen bonds in the complexes Co(III)P1(L 3 )(H 2 O), Co(III)P1(L 2 )(H 2 O) appear in the same region (6.26 ppm) as in the initial complex Co(III)P1. Up-field shift of the Co(III)P(1-2) complexes proton signals agreed well with the DOSY experiments. The experiments were used for the compounds identification according to their self-diffusion coefficients, which depend on the size and the form of a molecule in accordance with the Stokes-Einstein equation [32][33][34][35]. The complexes Co(III)P(1-2) are characterized by a higher relative value of the self-diffusion coefficient to the solvent (0.39), than the complexes with ligands (0.34 and 0.28), which confirms the changes of molecular mass as a result of the complex formation. In addition to this, Co(III)P2 and Co(III)P2-L2, and Co(III)P2-L3 complexes were completely characterized by means of two-dimensional correlation spectroscopy (1H-1H 2D of COSY), which also is applied for the determination of macromolecules chemical structure [17,[30][31][32][33][34][35].    For the analysis of the chemical structure of Со(III)P(1-2) and its complexes with L1-L3, 1 H NMR spectra were obtained as shown in the Figure 4, which are the superpo sition (convolution) of spectra, relating to a certain range of self-diffusion coefficients which these bonds are characterized [17,[27][28][29][30][31]. Such superposition is obtained by a projection of a pseudo-two-dimensional spectrum of the diffusive ordered DOSY spec troscopy on the set range of self-diffusion coefficients. The analysis of the obtained ranges ( Figure 5) showed a change in the values of chemical shifts and a shape of the signals of characteristic groups that are usually observed as a result of the formation o complexes with ligands. In particular, formation of hydrogen bonds between one OH group of the porphyrin Со(III)Р1 and oxygen atom of carboxy-group of the ligand L3 o oxygen atom of nitro-group of the ligand L2 was evidenced by the up-field shift of sig nals of the porphyrin OH groups, which were involved in the hydrogen bonds formation (∆ = 1.14 ppm in case of the complexes Со(III)Р1(L3)(H2O), and 2.60 ppm in case of the Со(III)Р1(L2)(H2O)), compared to the OH group proton of the Со(III)Р1. The protons o another OH group of the Со(III)Р1, which are not involved in the formation of the con sidered hydrogen bonds in the complexes Со(III)Р1(L3)(H2O), Со(III)Р1(L2)(H2O) appea in the same region (6.26 ppm) as in the initial complex Со(III)Р1. Up-field shift of th Co(III)P(1-2) complexes proton signals agreed well with the DOSY experiments. The ex Based on this spectroscopic technique, the signals in the one-dimensional nuclear magnetic resonance experiment were assigned to the characteristic groups of the studied compounds. As shown in Figure 6, we unambiguously assign the proton signals both Co(III)P and the corresponding ligands of Co(III)P2-L2 and Co(III)P2-L3 complexes. In addition, the nuclear Overhauser effect experiment in a rotating system of coordinates (1H-1H 2D ROESY) was carried out to confirm of the space orientation of L2 to oxygen atoms of Co(III)P2. Recently, this method has been successfully applied to define the spatial structure of macromolecules [36][37][38][39], and the small biologically active molecules [40]. This experiment unambiguously showed through space interactions of ligand protons with the Co(III)P protons located in close proximity to oxygen. The appearance of an additional cross-peak (a red circle) resulting due to the interaction of the COOH or NO 2 groups of the ligands with the OH group of the porphyrins ( Figure 6) confirms this fact. spatial structure of macromolecules [36][37][38][39], and the small biologically active molecules [40]. This experiment unambiguously showed through space interactions of ligand protons with the Co(III)P protons located in close proximity to oxygen. The appearance of an additional cross-peak (a red circle) resulting due to the interaction of the COOH or NO2 groups of the ligands with the OH group of the porphyrins ( Figure 6) confirms this fact.

Co(III)/Co(II) Red-Ox Processes in the Composition of the Со(III)P in the Presence of CPC
Axial complexes of the porphyrinates with imidazole derivatives [Co(III)P-(L)2] are very stable in aqueous media, and the central cation reduction Со(III)/Co(II) in the metalloporphyrin is the only method of this complexes decomposition (imidazole derivatives elimination). As shown earlier [21], such a reduction takes place in solutions containing surfactants with opposite charged porphyrin.
The study of the water-soluble porphyrin interactions with micelles of ionic surfactants revealed the presence of three different forms of porphyrins in solutions: the free porphyrins in the monomers form, the premicellar surfactant-porphyrin aggregates and the micellized monomer [21,[41][42][43][44][45]. The formation of premicellar porphyrin aggregates occurs at low surfactant concentrations, and is accompanied by a decrease in the intensity and broadening of absorption bands in the UV-Vis spectra. The formation of a micellar monomer is observed with an increase in the surfactant concentration, and is accompanied by an increase in the intensity of absorption bands in the UV-Vis spectra.
Upon spectrophotometric titration of Сo(III)P(1-2)-(L)2 porphyrin solutions with CPC ( Figure 7a, Equation (2a)) with small additions of surfactants, the decrease in the absorption intensity is observed, which corresponds to the formation of an

Co(III)/Co(II) Red-Ox Processes in the Composition of the Co(III)P in the Presence of CPC
Axial complexes of the porphyrinates with imidazole derivatives [Co(III)P-(L) 2 ] are very stable in aqueous media, and the central cation reduction Co(III)/Co(II) in the metalloporphyrin is the only method of this complexes decomposition (imidazole derivatives elimination). As shown earlier [21], such a reduction takes place in solutions containing surfactants with opposite charged porphyrin.
The study of the water-soluble porphyrin interactions with micelles of ionic surfactants revealed the presence of three different forms of porphyrins in solutions: the free porphyrins in the monomers form, the premicellar surfactant-porphyrin aggregates and the micellized monomer [21,[41][42][43][44][45]. The formation of premicellar porphyrin aggregates occurs at low surfactant concentrations, and is accompanied by a decrease in the intensity and broadening of absorption bands in the UV-Vis spectra. The formation of a micellar monomer is observed with an increase in the surfactant concentration, and is accompanied by an increase in the intensity of absorption bands in the UV-Vis spectra.
Upon spectrophotometric titration of Co(III)P(1-2)-(L) 2 porphyrin solutions with CPC ( Figure 7a, Equation (2a)) with small additions of surfactants, the decrease in the absorption intensity is observed, which corresponds to the formation of an [Co(III)P(1-2)-(L) 2 ] Agg associate. After passing through the minimum and further increase in the CPC concentration, the intensity of the absorption bands in the corresponding UV-Vis spectra began to increase (Figure 6b, Equation (2b)), which indicates the destruction of associates and the appearance of micellar monomeric porphyrins.
As can be seen from the data of Figure 8 and Table 3, the CPC concentrations, at which the largest premicellar aggregates and micellar monomeric porphyrins (CCM) are formed, practically did not depend on the position of the hydroxyl group in the phenyl rings of Co(III)P(1-2), but significantly depended on the nature of the axial ligands. The more bulky axial ligands were coordinated on the porphyrinate, the greater the number of CPC molecules required for the formation of a complete micellar shell.
To determine the localization place of Co(III)P (preferentially in the hydrophobic regions of the micelle interior or at the water-micellar interface), and to deduce the ori-  Table 4. The resonance signals of the surfactant protons occurred in the spectral region of 0.78-9.10 ppm. The chemical shifts of CPC headgroup protons (-CHortho-, meta-, and para-) and those of the hydrophobic alkyl chain protons (α-CH 2 -, β-CH 2 -,γ-CH 2 -, (-CH 2 -) 12 , and ω-CH 3 ) indicated that the Co(III)P interacts with all groups of CPC but with various strength. The protons of the highly hydrophobic section of the molecules remain in the core portion of micelle and are highly shielded, with the NMR signals appeared in the low frequency range (in the present case protons exhibited low frequency signals at 0.95, 1.38, 1.57, and 2.12 ppm, respectively) (Figure 9a). As can be seen from the data of Figure 8 and Table 3, the CPC concentrations, at which the largest premicellar aggregates and micellar monomeric porphyrins (CCM) are formed, practically did not depend on the position of the hydroxyl group in the phenyl rings of Co(III)P(1-2), but significantly depended on the nature of the axial ligands. The more bulky axial ligands were coordinated on the porphyrinate, the greater the number of CPC molecules required for the formation of a complete micellar shell.      The CPC molecules in the micelle are mobile and can freely rotate, bend, or fold inside the micelle and are characterized by a sharply peak. However, with the addition of Co(III)P, the CPC molecule mobility inside micelles is decreased, significant broadening and changes in chemical shift are observed. This increase in line width in the presence of 50 mM Co(III)P is consistent with a reduced exchange rate at a higher concentration of СоР [46][47][48].
The protons closest to the surfactant head group and ones on the cationic head group gave rise to higher frequency NMR signals, as they were less shielded than protons located in the end of the alkyl chain. The COSY experiment of the [Co(III)P1-(H2O)2] Mc system showed strong correlations between the CPC head groups protons and porphyrin phenyl rings, as evidenced by the high cross-peaks between them. Besides, there are comparatively intense cross peaks between porphyrinate protons and CPC chain protons. All these observations led us to conclude that the hydrophilic fragments of porphyrin are solubilized in the micelle head groups, and the tetrapyrrole macrocycle is located in the micelle "palisade" layer.
In the presence of surfactant micelles due to the inclusion of the porphyrin molecule The CPC molecules in the micelle are mobile and can freely rotate, bend, or fold inside the micelle and are characterized by a sharply peak. However, with the addition of Co(III)P, the CPC molecule mobility inside micelles is decreased, significant broadening and changes in chemical shift are observed. This increase in line width in the presence of 50 mM Co(III)P is consistent with a reduced exchange rate at a higher concentration of CoP [46][47][48].
The protons closest to the surfactant head group and ones on the cationic head group gave rise to higher frequency NMR signals, as they were less shielded than protons located in the end of the alkyl chain. The COSY experiment of the [Co(III)P1-(H 2 O) 2 ] Mc system showed strong correlations between the CPC head groups protons and porphyrin phenyl rings, as evidenced by the high cross-peaks between them. Besides, there are comparatively intense cross peaks between porphyrinate protons and CPC chain protons. All these observations led us to conclude that the hydrophilic fragments of porphyrin are solubilized in the micelle head groups, and the tetrapyrrole macrocycle is located in the micelle "palisade" layer.
In the presence of surfactant micelles due to the inclusion of the porphyrin molecule in its outer micellar shell and the screening of the metalloporphyrin coordination center by the surfactant hydrocarbon chains, the Co(III)porphyrin is reduced into Co(II)porphyrin, which is accompanied by the elimination of axial ligands.
It is known that cobalt cation in the porphyrin coordination center can have two oxidation states (2 + and 3 + ), and both states can quite easily transform into each other. So, when Co(II)-tetraarylporphyrins are dissolved in electron-donating or non-polar solvents in the presence of organic bases, the Co(II) cation almost instantaneously oxidizes into Co(III), coordinating on itself two additional electron-donating ligands or one ligand and one solvent molecule [49][50][51][52]. The catalyst for this process is molecular oxygen contained in the air. That is, in practice, the presence of an electron donor environment and air atmosphere is the condition for finding the cobalt cation in the 3 + state in the corresponding porphyrinate. As noted above, when Co(III)P-(L) 2 is localized into CPC micelle, the aquaor imidazole complex of the porphyrinate is incorporated into the hydrophobic part of the micelle. An inert environment is created around the coordination center of the porphyrin, completely eliminating the presence of water molecules, which apparently initiates the process of Co(III) reduction into Co(II): τ, T Table 5 and Figure 10.    Table 5 and Figure 10.  Our investigations have shown that the Co(III)/Со(II) reduction rate in the micellized porphyrinate depends on various factors such as the surfactant nature, buffer ionic strength, temperature, and axial ligand nature. Co-porphyrinates with aqua-ligands have the highest reduction rate. The reduction rate of Co(III)/Со(II) is decreased at the pres- Our investigations have shown that the Co(III)/Co(II) reduction rate in the micellized porphyrinate depends on various factors such as the surfactant nature, buffer ionic strength, temperature, and axial ligand nature. Co-porphyrinates with aqua-ligands have the highest reduction rate. The reduction rate of Co(III)/Co(II) is decreased at the presence of one unsubstituted imidazole ligand by 1.5 times. The two-sites binding of imidazole derivative depending on strength of additional hydrogen bond makes the Co(III)-porphyrins more stable to reduction from 2 to 4 times. Bis-axial complexes of [Co(III)P-(L) 2 ] Mc are reduced especially slow. The formation constants of mono-axial complexes of [Сo(III)P(1-2)(L)(Н2О)] Mc obtained according with the equilibrium 4a confirm that selective ability of imidazole derivative binding by Со-porphyrin in CPC micellar solutions was retained ( Figure 12). As the Co-porphyrin monomer, as micellized porphyrin binding ligands L2 and L3 via formation of donor-acceptor and hydrogen bonds.  -(methoxyphenyl)-10,20-bis-phenylporphyrins (1,2) were obtained according to [53] through acid catalyzed condensation reaction between meso-phenyldipyrrolylmethane and corresponding methoxy-benzaldehydes followed by oxidation of reaction mixture by o-chloranil. The formation constants of mono-axial complexes of [Co(III)P(1-2)(L)(H 2 O)] Mc obtained according with the equilibrium 4a confirm that selective ability of imidazole derivative binding by Co-porphyrin in CPC micellar solutions was retained ( Figure 12). As the Co-porphyrin monomer, as micellized porphyrin binding ligands L2 and L3 via formation of donor-acceptor and hydrogen bonds. The formation constants of mono-axial complexes of [Сo(III)P(1-2)(L)(Н2О)] Mc obtained according with the equilibrium 4a confirm that selective ability of imidazole derivative binding by Со-porphyrin in CPC micellar solutions was retained ( Figure 12). As the Co-porphyrin monomer, as micellized porphyrin binding ligands L2 and L3 via formation of donor-acceptor and hydrogen bonds.  -(methoxyphenyl)-10,20-bis-phenylporphyrins (1,2) were obtained according to [53] through acid catalyzed condensation reaction between meso-phenyldipyrrolylmethane and corresponding methoxy-benzaldehydes followed by  (1,2) were obtained according to [53] through acid catalyzed condensation reaction between meso-phenyldipyrrolylmethane and corresponding methoxy-benzaldehydes followed by oxidation of reaction mixture by o-chloranil. 5,15-bis-(3-methoxyphenyl)-10,20-bis-phenylporphyrin (1). To a solution of 0.2 g (0.96 mmol) meso-phenyldipyrrolylmethane in 50 mL of dichloromethane, were added 0.14 g (1.21 mmol) of 3-methoxybenzaldehyde in 25 mL dichloromethane and 1 mL of trichloroacetic acid. The solution was refluxed for 30 min and subjected oxidation by treatment with 0.1 g of o-chloranil. The reaction mixture was washed with water, evaporated to a minimum volume and chromatographed on aluminum oxide using dichloromethane as an eluent. Yield of the compound (1)  5,15-bis-(hydroxyphenyl)-10,20-bis-(sulfophenyl)porphyrins (5,6) were prepared as described in [55] from the intermediate products (3,4) respectively. 5,15-bis-(3-hydroxyphenyl)-10,20bis-(4-sulfophenyl)porphyrin (5). Of 5,15-bis-(3-hydroxyphenyl)-10,15-bis-phenylporphyrin 0.15 g (0.19 mmol) was dissolved by stirring in 30 mL of concentrated sulfuric acid at room temperature and heated at 70 • C for 30 min. The resulting solution was cooled poured onto ice, the precipitate was filtered and washed with water and used without further purification. Yield of the compound (5) was equal to 87%. 5,15-bis-(2-hydroxyphenyl)-10,15bis-(4-sulfophenyl)porphyrin (6) was obtained similarly to (5). Yield of the compound (6) was equal to 79%. The compounds 5 and 6 were used in subsequent transformations without additional purification.

Spectrophotometric Studies
Thermodynamic constants for the complexation of the Co(III)P with L were calculated according to the Equation (6) on the base of the spectrophotometric titration experiment results: where λ 1 is descending wavelength, λ 2 is ascending wavelength; [Co(III)P-Im] is the concentration of the porphyrinate with one axial ligand; and [L] is the ligand concentration. ∆A 0 is the maximal change of solution optical density at the given wavelength, and ∆Ai is the change of solution optical density at the given wavelength at the given concentration [57].
Kinetic parameters of the investigated reaction were obtained according to the known procedure [33]. Effective rate constants (k eff ) were determined by the change in the solution optical density on working wave lengths (λ = 414, 425 nm) after definite time intervals by the equation of formally first order (Equation (7)) when CPC were in excess.

Spectrophotometric Studies
Thermodynamic constants for the complexation of the Co(III)P with L were calculated according to the Equation (6) on the base of the spectrophotometric titration experiment results: where λ1 is descending wavelength, λ2 is ascending wavelength; [Co(III)P-Im] is the concentration of the porphyrinate with one axial ligand; and [L] is the ligand concentration. ΔАo is the maximal change of solution optical density at the given wavelength, and ΔАi is the change of solution optical density at the given wavelength at the given concentration [57]. Kinetic parameters of the investigated reaction were obtained according to the known procedure [33]. Effective rate constants (keff) were determined by the change in the solution optical density on working wave lengths (λ = 414, 425 nm) after definite time intervals by the equation of formally first order (Equation (7)) when CPC were in excess. keff=1/τ log(c0/cτ) where c0 and cτ are the complexes concentrations of at start of the process and at time τ.
Values keff and determination of average deviations were optimized with using of Microsoft Excel and ggh.exe (QB-45) by the Guggenheim method. Relative error was 3-5%.

NMR Studies
NMR experiments were performed on a Bruker Avance III 500 MHz NMR spec-

NMR Studies
NMR experiments were performed on a Bruker Avance III 500 MHz NMR spectrometer (Bruker Biospin, Karlsruhe, Baden-Württemberg, Germany) equipped with a 5-mm probe using standard Bruker TOPSPIN Software. Temperature control was performed using a Bruker variable temperature unit (BVT-2000) in combination with a Bruker cooling unit (BCU-05) to provide chilled air. Experiments were performed at 298 K without sample spinning. TMS signals were used as internal standards for counting chemical shifts. The two-dimension diffusion ordered spectroscopy (2D DOSY) spectra were recorded with PGSTE pulse sequence using a bipolar gradient pulses and the insertion of a supplementary delay (LED) [58]. The PGSTE sequence was used with a diffusion delay of 0.1 s, a total diffusion-encoding pulse width of 5 ms. For each of 32 gradient amplitudes, 32 transients of 16.384 complex data points were acquired. The two-dimensional correlation spectroscopy (2D COSY) spectra with a zero-quantum suppression element [59] were acquired with a 16.96 ppm spectral window in the direct dimension F1 with 2048 complex data points and a 16.96 ppm spectral window in the indirect dimension F2 with 128 complex points. The spectra were acquired with 64 scans and relaxation delay of 2 s. Two-dimensional rotating frame nuclear Overhauser effect spectroscopy (2D ROESY) [59] experiments were performed with pulsed filtered gradient techniques. The spectra were recorded in a phasesensitive mode using Echo/Antiecho-TPPI gradient selection with 2048 points in the F2 direction and 256 points in the F1 direction. Spin-lock delay values for 2D ROESY were 200 ms. The spectra were acquired with 64-72 scans and relaxation delay of 2 s.

Quantum-Chemical Calculations
Were performed using the Gaussian 09 software package [60]. The optimization of the geometrical parameters of the compounds under study and NBO-analysis were performed using the density functional theory method (DFT) with the introduction of dispersion interactions in the semiempirical Grimm DFT-D3 (BJ) model [61]. We used the CAM-B3LYP functional [62] with the basic set: Def2TZVPP [63,64] for the Co atom and 6-31G (d, p) [65,66] for the rest of the atoms. All structures did not have virtual frequencies in vibration spectra correspond to energy minimum.
The energy of intermolecular interaction of the studied complexes ∆E with taking into account the superposition error of BSSE was calculated according to the Equation (8) where E(AB,aUb,R),E(A,a,R), and E(B,b,R) are the energy of the complex and the initial molecules, respectively. Molecules A and B are separated by the distance R in the complex, a and b are the basic set of isolated molecules, and aUb is the basic set of the AB complex. The stabilization energy of the electronic pair acceptor orbitals at the bond formation (E st ) and the values of charge transfer (q CT ) were calculated by the following Equation (10) [69,70]: where F ij -the Fock matrix element between i and j NBO orbitals and ∆E-the difference in orbital energies.

Conclusions
Thus, it was found that disulfoderivatives of Co(III)-tetraarylporphyrines with hydroxyl groups in two aryl fragments of the macrocycle have the ability to recognize the various imidazole derivatives (including drugs) due to the formation of additional hydrogen bonds upon their axial coordination on the cobalt cation in aqueous media. The strongest additional hydrogen bonds were formed in the case of Co(III)-porphyrinate with a hydroxyl group in the ortho-position of the phenyl fragment and the nitro group of the pharmaceutical metronidazole molecule. Moreover, the selectivity of binding was recorded when only one imidazole derivative was attached in axial-position. It was found that the localization of the investigated sulfonated Co(III)-tetraarylporphyrin into spherical micelles of cetylpyridine chloride decreased their binding ability towards imidazoles, but the selectivity of their binding was retained.
Micellation of the Co(III)-porphyrins leads to a complete or partial reduction of the central cobalt cation into Co(II). The rate of the reduction process and the degree of its occurrence very strongly depended on the strength of the axial ligands binding: bis-aqua Co(III)-porphyrins were reduced more rapidly, and bis-imidazole complexes were reduced more slowly. The presence of additional hydrogen bonds during the formation of monoaxial complexes of Co(III)-porphyrins with imidazole derivatives increased their resistance to reduction by 2-4 times. The rate of reduction can also be controlled by increasing the temperature, varying the nature of substrate or medium. The obtained materials can be used to develop effective receptors for recognition, delivery, and prolonged release of drug compounds to the sites of their functioning. Considering that cetylpyridinium chloride is a widely used cationic biocide as a disinfectant, the materials we developed might prove to be effective antimicrobial agents. We are currently conducting research in this area.