Direct Aminolysis of Ethoxycarbonylmethyl 1,4-Dihydropyridine-3-carboxylates

The ethoxycarbonylmethyl esters of 1,4-dihydropyridines were directly converted into carbamoylmethyl esters in the presence of 1,5,7-triazabicyclo[4.4.0]dec-5-ene (TBD) in good to excellent yields under mild conditions. The use of TBD is crucial for the successful aminolysis of ethoxycarbonylmethyl ester of 1,4-dihydropyridines with secondary amines as without it the reaction does not proceed at all. The aminolysis reaction proceeded regioselectively, as the alkyl ester conjugated with the 1,4-dihydropyridine cycle was not involved in the reaction. Screening of other N-containing bases, such as triethylamine (TEA), pyridine, 4-(N,N-dimethylamino)pyridine (DMAP), 1,8-diazabicyclo[5.4.0]undec-7-ene (DBU), 1,5-diazabicyclo[4.3.0]non-5-ene (DBN), imidazole, tetramethyl guanidine (TMG) and 7-methyl-1,5,7-triazabicyclo[4.4.0]dec-5-ene (MTBD) as catalysts revealed no activity in the studied reaction.


Introduction
As a privileged structure 1,4-dihydropyridine (1,4-DHP) represents an important scaffold for the design and development of novel pharmaceuticals [1]. Bis(alkyl) 4-aryl-2,6-dimethyl-1,4dihydropyridine-3,5-dicarboxylates are well known as a class of calcium channel blockers [2,3]. Substituents at positions 3 and 5 of 4-aryl-2,6-dimethyl-1,4-dihydropyridine-3,5-dicarboxylates have crucial influence on biological activities and chemical properties such as hydrolysis, and transesterification [4]. Thus, alkyl esters at positions 3 and 5 of 1,4-DHP are exceptionally stable upon treatment with nucleophilic reagents due to electronic and steric reasons [5]. In the case of ethoxycarbonylmethyl 1,4-dihydropyridine-3-carboxylates, alkaline and enzyme-catalysed hydrolysis takes place only at the more remote from the 1,4-DHP cycle ester groups forming the corresponding carboxymethyl esters because of steric and electronic factors [6,7]. The antiviral activity of 1,4-DHP-3,5-bis(alkoxymethylcarboxylates) and a pronounced synergism with the anti-cancer drug 5-FU have been reported recently [8,9]. Studies of carbamoylmethyl 1,4-DHP-3-carboxylates are rather limited and fragmented. There is one reported synthesis of phenylcarbamoylmethyl ester of 1,4-DHP via a three component Hantzsch-type condensation [10,11]. However, this approach is avoided since the commercially unavailable carbamoylmethylacetoacetates would require synthesis from diketene. Another method involves hydrolysis of the ethoxycarbonylmethyl ester of 1,4-DHP followed by activation of the resulting acid and amidation reaction with an amine [12]. Previously our laboratory reported that the 3-ethoxycarbonylmethyl ester containing 1,4-DHP derivatives together with removal of a protecting group using methylamine readily formed methylcarbamoylmethyl esters which possess calcium level controlling activities [13]. Amidation of the appropriate acids through activated intermediates with secondary amines remains the only option leading to tertiary carbamoylmethyl esters.
During the last decade a noticeable improvement for direct aminolysis of acetates or benzoates has been achieved by using amine-based bases as catalysts: imidazole [14], TEA [15], 2-pyridone [16], TBD [17], DBU [18], and others. It is worth mentioning that primary amines have recently been reported for aminolysis of alkoxycarbonylmethyl ester of asiatic acid [19], substituted piperidines [20] and substituted alkoxymethyl oxycarbamates [21], however no catalytic methods to promote this slow reaction have been found up to now.
In the case of 1,4-DHPs the aminolysis is more preferential, versatile, and faster method since the starting materials are easily obtained via Hantzsch synthesis. From the synthetic point of view elaboration of synthetic procedures for convenient construction of the desired carbamoylmethyl esters of 4-aryl-2,6-dimethyl-1,4-dihydropyridine-3,5-dicarboxylates through direct aminolysis is the main objective of this work. In this paper, we report our studies on aminolysis of the ethoxycarbonylmethyl ester of 1,4-dihydropyridines 3a-d with primary and secondary alkyl and cyclic amines.
Molecules 2015, 20, page-page 2 possess calcium level controlling activities [13]. Amidation of the appropriate acids through activated intermediates with secondary amines remains the only option leading to tertiary carbamoylmethyl esters.
During the last decade a noticeable improvement for direct aminolysis of acetates or benzoates has been achieved by using amine-based bases as catalysts: imidazole [14], TEA [15], 2-pyridone [16], TBD [17], DBU [18], and others. It is worth mentioning that primary amines have recently been reported for aminolysis of alkoxycarbonylmethyl ester of asiatic acid [19], substituted piperidines [20] and substituted alkoxymethyl oxycarbamates [21], however no catalytic methods to promote this slow reaction have been found up to now.
In the case of 1,4-DHPs the aminolysis is more preferential, versatile, and faster method since the starting materials are easily obtained via Hantzsch synthesis. From the synthetic point of view elaboration of synthetic procedures for convenient construction of the desired carbamoylmethyl esters of 4-aryl-2,6-dimethyl-1,4-dihydropyridine-3,5-dicarboxylates through direct aminolysis is the main objective of this work. In this paper, we report our studies on aminolysis of the ethoxycarbonylmethyl ester of 1,4-dihydropyridines 3a-d with primary and secondary alkyl and cyclic amines.

Results and Discussion
The starting ethoxycarbonylmethyl esters of 1,4-dihydropyridines 3a-d (Scheme 1) were prepared via a two-component Hantzsch type cyclisation of the appropriate ethoxycarbonylmethyl 3-oxo-(1arylmethylidene)butyrate [13] 2a-c and 3-aminobut-2-enoic acid ester [22] 1a-c utilising by using diglyme as solvent and 1-butyl-4-methylpyridinium chloride (4-MBPy) as catalyst. The reactions were carried out at 60-80 °C for two hours giving ethoxycarbonylmethyl esters of 1,4-dihydropyridines 3a-d in 33%-75% yields in analogy with already reported methodologies [23]. Synthesis of 1,4-DHPs 3b-d was performed based on the fact that these motifs are common structural scaffolds in drug molecules. Recently a non-catalytic direct aminolysis of 3-ethoxycarbonylmethyl ester containing 1,4-DHP derivatives with methylamine leading to the corresponding methylcarbamoylmethyl esters in 48 h was described [13]. To explore the scope and limitation of this reaction a variety of primary and secondary alkylamines and cyclic amines were reacted with 1,4-DHPs 3a-d. Primary aminolysis screening of ethoxycarbonylmethyl ester of 1,4-dihydropyridine 3a with piperidine as a model substrate, utilising by using N-containing bases, such as TEA, Pyridine, DMAP, DBU, DBN, Imidazole, TMG, TBD and MTBD as catalysts was performed and the results are summarised in Scheme 2 and Table 1.
Screening reactions were carried out with 1 equiv. of 1,4-DHP 3a, 3 equiv. of piperidine and 20 mol % of the appropriate catalyst, at 30 °C for thirty minutes in DMF and the reaction rates were measured with LC-MS technique. The amount of DMF used for dissolution of 1.5 mmol of 1,4-DHP 3a was 1 mL. It was found that only the bicyclic guanidine base TBD catalysed aminolysis reaction proceeded efficiently (Table 1, entry 9). For the rest of the cases where other bases were used as catalysts (Table 1, entries 2-8 and 10) and in the absence of a catalyst (Table 1, entry 1) no aminolysis reaction proceeded, as only trace amounts of carboxymethyl derivative 5a were found. Scheme 1. Synthesis of ethoxycarbonylmethyl esters of 1,4-dihydropyridines 3a-d.
Recently a non-catalytic direct aminolysis of 3-ethoxycarbonylmethyl ester containing 1,4-DHP derivatives with methylamine leading to the corresponding methylcarbamoylmethyl esters in 48 h was described [13]. To explore the scope and limitation of this reaction a variety of primary and secondary alkylamines and cyclic amines were reacted with 1,4-DHPs 3a-d. Primary aminolysis screening of ethoxycarbonylmethyl ester of 1,4-dihydropyridine 3a with piperidine as a model substrate, utilising by using N-containing bases, such as TEA, Pyridine, DMAP, DBU, DBN, Imidazole, TMG, TBD and MTBD as catalysts was performed and the results are summarised in Scheme 2 and Table 1.
Screening reactions were carried out with 1 equiv. of 1,4-DHP 3a, 3 equiv. of piperidine and 20 mol % of the appropriate catalyst, at 30˝C for thirty minutes in DMF and the reaction rates were measured with LC-MS technique. The amount of DMF used for dissolution of 1.5 mmol of 1,4-DHP 3a was 1 mL. It was found that only the bicyclic guanidine base TBD catalysed aminolysis reaction proceeded efficiently ( Molecules 2015, 20, page-page 3 Scheme 2. Screening of various catalysts for aminolysis using 1,4-DHP 3a and piperidine as model substrates.     Such a lack of reactivity of other catalysts in the aminolysis reaction is perhaps due to their lower basicity compared to TBD [24,25], steric hindrance and low nucleophilicity. For guanidine-catalysed reactions an interplay between basicity and nucleophilicity of the catalyst was already considered as crucial [26]. As TBD possessed the highest catalytic activity to provide amide 4h, this base was selected for further experiments. TBD is an efficient guanidine-based bifunctional catalyst, which has found applications in promotion of various reactions including aminolysis of benzoates and methylphenyl acetates [17]. Screening of three TBD loadings (5, 10 and 20 mol %) for aminolysis reactions of the ethoxycarbonylmethyl ester of 1,4-dihydropyridine 3a with piperidine have been evaluated ( Table 2, entries 1-3). Using 5 mol % of TBD ( Table 2, entry 3) the conversion of 1,4-DHP 3a led mainly to the formation of carboxymethyl derivative 5a with minor formation of amide 4h. The catalytic activity of TBD was remarkable at 10 mol % loading, however after 4 h the reaction was still incomplete, with formation of carboxymethyl derivative 5a as by-product ( Table 2, entry 2). Increasing the catalyst loading from 10 to 20 mol % secured a complete transformation of ester 3a into amide 4h, with almost no formation of carboxymethyl derivative 5a ( Table 2, entry 1). Catalyst loading was selected as 20 mol % as it was used in the screening experiments. Further experiments have revealed that the aminolysis at 70˝C was much faster together with formation of carboxymethyl derivative 5a but decreasing the temperature to 4˝C slowed the reaction down ( Table 2, entries 4 and 5). Therefore, performing the reaction at 30˝C was found to be optimal and this temperature was used in further experiments.
Altering the reaction media from DMF ( Table 2, entry 1) to THF led to rather similar results (Table 2, entry 6). Selectivity of the reaction was changed considerably when acetonitrile, dichloromethane, dioxane or methanol were used as solvents. Aminolysis reaction, with the same TBD and piperidine loading performed in dichloromethane or dioxane led to extensive formation of carboxymethyl derivative 5a as by-product along with recovered starting material (Table 2, entries 7-9). Performing aminolysis in methanol led to a complete disappearance of the starting ester 3a with formation of a mixture of carboxymethyl derivative 5a and amide 4h (Table 2, entry 10).
Next, we explored the influence of TBD on the aminolysis reactions of 1,4-DHP 3a with primary amines (Table 3, entries 1-7). TBD catalysed aminolysis of 1,4-DHP 3a using 3 fold excess of 1-propylamine and DMF as the solvent (Table 3, entry 1) proceeded smoothly with 78% yield in 2 h at 30˝C. In the absence of a catalyst in 2 h aminolysis of 1,4-DHP 3a with 1-propylamine at the same reaction conditions practically does not occur as only 2% of amide 4a was detected (Table 3, entry 2).
The reaction of ester 3a was performed by using 2-propylamine as also the solvent, that is in the presence of 15 fold excess of nucleophile for 4 h at 30˝C in 76% yield (Table 3, entry 5), and by adding the amine only in a reduced amount (3 equiv.) to DMF the amide 4b was obtained in 79% yield (Table 3, entry 3). Without adding a catalyst reaction of 1,4-DHP 3a with 2-propylamine proceeded very slowly in DMF at 30˝C, as only 4% of conversion to amide 4b was observed in 4 h ( Table 3, entry 4), a longer reaction time did not improve this reaction significantly. The influence of TBD on aminolysis of ester 3a using a 3 fold excess of 1-butylamine (Table 3, entries 6, 7) in DMF was also studied. The usefulness of TBD as a catalyst has been proven also in this case, as almost quantitative conversion of ester 3a to amide 4c in the case of TBD catalysed reaction (Table 3, entry 6) was observed compared to only 3% of conversion to 4c in the case where no catalyst was used (  (Table 3, entry 5), and by adding the amine only in a reduced amount (3 equiv.) to DMF the amide 4b was obtained in 79% yield (Table 3, entry 3). Without adding a catalyst reaction of 1,4-DHP 3a with 2-propylamine proceeded very slowly in DMF at 30 °C, as only 4% of conversion to amide 4b was observed in 4 h ( Table 3, entry 4), a longer reaction time did not improve this reaction significantly. The influence of TBD on aminolysis of ester 3a using a 3 fold excess of 1-butylamine (Table 3, entries 6, 7) in DMF was also studied. The usefulness of TBD as a catalyst has been proven also in this case, as almost quantitative conversion of ester 3a to amide 4c in the case of TBD catalysed reaction (Table 3, entry 6) was observed compared to only 3% of conversion to 4c in the case where no catalyst was used (  Similarly to the reactions of 1,4-DHP 3a with primary amines in the presence of TBD, the secondary alkyl and cyclic amines also showed good activity toward 1,4-DHPs 3a-d under the present reaction conditions, thus in three or four hours 75%-97% yields of the target amides 4d-m were reached (Scheme 3, Table 3, entries 8, [11][12][13][14][15][16][17][18][20][21][22][23]. When TBD was applied to the reaction of ester 3a with diethylamine in DMF for 4 h at 30 °C, amide 4d was obtained in 75% yield ( Table 3, entry 8). No aminolysis reaction was observed when ester 3a was treated with the bulkier diisopropylamine or diphenylamine perhaps due to steric reasons (Table 3, entries 9, 10). However, ethoxycarbonylmethyl ester 3a was hydrolysed to carboxymethyl derivative 5a in 70% with diisopropylamine (Table 3, entry 9) as this base is considerably stronger than diphenylamine. In the case of diphenylamine no hydrolysis of ester 3a was observed (Table 3, entry 10). Reactions of 1,4-DHP 3a with unsymmetrical secondary amines-N-methylbutylamine or N-methyloctylamine (Table 3, entries 11 and 12) also proceeded smoothly with high yields in the presence of TBD in DMF for 4 h at 30 °C. Reactions of 3a-d with piperidine, morpholine, pyrrolidine and thiomorpholine were performed in DMF for three or four hours at 30 °C in the presence of TBD (Table 3, entries 13, 14, 16 and 18, 20-22). No aminolysis of ester 3a with the sterically bulky 1-naphthylamine was observed (Table 3, entry 19). Alternatively, reactions of esters 3a,d with piperidine and morpholine can be performed where nucleophiles were also used as solvents (Table 3, Table 3, entries 20-23) and 1,4-dihydropyridines 3c,d (Table 3, entries 21-23) having other ester moieties on the other side of 1,4-DHP ring that there is no significant influence of these substituents on the aminolysis reaction with cyclic amines.
Altering the reaction media had no significant influence on the yields of the reactions (Table 3, entries 3 vs. 5, 14 vs. 15, 16 vs. 17 and 22 vs. 23). It should be admitted that aminolysis reactions of 1,4-DHP 3a-d with secondary amines in the absence of TBD did not proceed at all.

Scheme 3. Aminolysis of ethoxycarbonylmethyl esters of 1,4-dihydropyridines 3a-d.
Similarly to the reactions of 1,4-DHP 3a with primary amines in the presence of TBD, the secondary alkyl and cyclic amines also showed good activity toward 1,4-DHPs 3a-d under the present reaction conditions, thus in three or four hours 75%-97% yields of the target amides 4d-m were reached (Scheme 3, Table 3, entries 8, 11-18, 20-23). When TBD was applied to the reaction of ester 3a with diethylamine in DMF for 4 h at 30˝C, amide 4d was obtained in 75% yield ( Table 3, entry 8). No aminolysis reaction was observed when ester 3a was treated with the bulkier diisopropylamine or diphenylamine perhaps due to steric reasons (Table 3, entries 9, 10). However, ethoxycarbonylmethyl ester 3a was hydrolysed to carboxymethyl derivative 5a in 70% with diisopropylamine (Table 3, entry 9) as this base is considerably stronger than diphenylamine. In the case of diphenylamine no hydrolysis of ester 3a was observed (Table 3, entry 10). Reactions of 1,4-DHP 3a with unsymmetrical secondary amines-N-methylbutylamine or N-methyloctylamine (Table 3, entries 11 and 12) also proceeded smoothly with high yields in the presence of TBD in DMF for 4 h at 30˝C. Reactions of 3a-d with piperidine, morpholine, pyrrolidine and thiomorpholine were performed in DMF for three or four hours at 30˝C in the presence of TBD (Table 3, entries 13, 14, 16 and 18, 20-22). No aminolysis of ester 3a with the sterically bulky 1-naphthylamine was observed (Table 3, entry 19). Alternatively, reactions of esters 3a,d with piperidine and morpholine can be performed where nucleophiles were also used as solvents (Table 3, entries 15, 17 and 23), however in this case a 15 fold excess of amine should be used. When aminolysis reactions were performed in DMF the amines were used in a 3-fold excess only.
It was also shown in the examples of aminolysis of 1,4-dihydropyridines 3b-d having substituted aromatic ring at position 4 (Table 3, entries 20-23) and 1,4-dihydropyridines 3c,d (Table 3, entries 21-23) having other ester moieties on the other side of 1,4-DHP ring that there is no significant influence of these substituents on the aminolysis reaction with cyclic amines.
Altering the reaction media had no significant influence on the yields of the reactions (Table 3,   Structures of all newly synthesised 1,4-DHPs were established and confirmed by 1 H-NMR, 13 C-NMR, MS, IR and elemental analysis data. The IR spectra of obtained compounds showed characteristic 1,4-DHPs absorption bands. Thus, N-H and C=O absorption bands were present at frequencies 3398-3200 cm´1 and 1750-1621 cm´1, respectively. The presence of C=O absorbance at 1740 cm´1 of the more remote carbonyl group from the 1,4-DHP cycle of esters 3a-d and acid 5a was observed, while for amides 4a-m this absorbance was shifted to lower frequencies (~1700 cm´1) and merged with C=O signals of the conjugated β-aminovinylcarbonyl system of 1,4-DHP. Molecular weights of compounds measured by LC-MS technique were in good agreement with the calculated values for all the compounds. The 1 H-NMR spectra obtained in both solvents CDCl 3 and DMSO-d 6 of all newly synthesised 1,4-DHP esters 3a-d, amides 4a-m and carboxymethyl derivative 5a have shown that the methylene group protons (COOCH 2 CO) at the position 3 (or 5) have appeared as AB-systems at δ interval between 4.10 and 4.86 with a coupling constant over 14 Hz. Chemical shifts and coupling constant values were dependent on the substituents of 1,4-DHP derivatives 3a-d, 4a-m, 5a and the solvents. It should be underlined that some of the signals in NMR spectra of carbamoylmethyl ester of 1,4-dihydropyridines 4e and 4f having unsymmetrical tertiary carbamoyl group were split due to nitrogen inversion of amide and slow N-C(O) bond rotation. Thus, the proton signals in 1 H-NMR spectra of AB-systems of methylene group and N-CH 3 group were split into two components with ratio-0.45:0.55. The carbon signals in 13 C-NMR spectra were also duplicated for some alkyl carbons of both carbonyl group carbons at the carbamoylmethyl ester of 1,4-DHPs 4e and 4f. Similar observations were found for N-acyl oxaziridine systems confirming the existence of two independent stereodynamic processes: nitrogen inversion and rotation about the N-C(O) bond, both processes were determined to be slow on the NMR timescale [27]. The interpretation of the conformational information for the Me-N-C(O)-CH 2 fragment of the carbamoylmethyl ester 4f was based on 1 H-1 H NOESY spectra. The observed cross peak between N-CH 3 (δ: 2.84) from the major conformer and methylene group (COOCH 2 CO) signals showed that these groups were close in space. Thus, the signal of N-CH 3 (δ: 2.84) belongs to the cis-isomer (55%). The observed cross peak between N-CH 2 -(δ: 3.12) from the minor conformer and methylene group (COOCH 2 CO) signals showed that these groups were close in space. Thus, the signal of N-CH 2 -(δ: 3.12) belongs to the trans-isomer (45%).
A potential mechanism for the aminolysis of methyl benzoate and methyl phenylacetate in the presence of TBD has been proposed [17], which includes TBD reaction with ester followed by proton transfer from the protonated nitrogen of TBD with further formation of the corresponding TBD amide and alcohol from the ester moiety. Finally, regeneration of free TBD resulted in the formation of amides. Theoretical studies of aminolysis of methyl acetate catalysed by TBD performed by Jin et al. have indicated a stepwise mechanism involving tetrahedral intermediates through hydrogen bonding of TBD [28].

General Information
All reagents were purchased from Acros Organics (Geel, Belgium), Sigma-Aldrich (St. Louis, MO, USA), Alfa Aesar (Lancashire, UK), or Merck KGaA (Darmstadt, Germany) and used without further purification. TLC was performed on silica gel 60 F 254 aluminium sheets 20ˆ20 cm (Merck KGaA, Darmstadt, Germany). 1 H-NMR (400 MHz) and 13 C-NMR (100.56 MHz) spectra were recorded with a Varian Mercury BB spectrometer (Agilent, Santa Clara, CA, USA). The coupling constants are expressed in Hertz (Hz). The chemical shifts of the hydrogen and carbon atoms are presented in parts per million (ppm) and referred to the residual signals of the non-deuterated CDCl 3 (δ: 7.26) or partially deuterated DMSO-d 6 (δ: 2.50) solvent for 1 H-NMR spectra and CDCl 3 (δ: 77.0) or DMSO-d 6 (δ: 39.5) solvent for 13 C-NMR, respectively. Multiplicities are abbreviated as s = singlet; d = doublet; t = triplet; m = multiplet; br = broad; dd = double doublet; dt = double triplet; td = triple doublet; tt = triple triplet; ddd = double double doublet. Mass spectral data were determined on an Acquity UPLC system (Waters, Milford, MA, USA) connected to a Waters SQ Detector-2 operating in the ESI positive or negative ion mode on a Waters Acquity UPLC BEH C18 column (1.7 µm, 2.1ˆ50 mm, using a gradient elution with acetonitrile (0.01% trifluoroacetic acid) in water (0.01% trifluoroacetic acid) at a flow rate of 0.5 mL/min. LC-MS data were recorded with a Waters MassLynx 4.1 chromatography data system. The conversions of the reactions were analysed by HPLC on Waters Alliance 2695 system and Waters 2485 UV/Vis detector equipped with Alltima ODS-2 column (5 µm, 4.6ˆ150 mm, Grace, Columbia, MD, USA) using a gradient elution with methanol/water (v/v), at a flow rate of 1 mL/min. Peak areas were determined electronically with Waters Empower 2 chromatography data system. Melting points (m.p.) of the synthesised compounds were determined on an OptiMelt (SRS Stanford Research Systems, Sunnyvale, CA, USA). Infrared spectra were recorded with a Prestige-21 FTIR spectrometer (Shimadzu, Kyoto, Japan). Elemental analyses were determined on an Elemental Combustion System ECS 4010 (Costech Instruments, Pioltello, Italy).

Conclusions
The synthesis of carbamoylmethyl esters of dihydropyridines in direct aminolysis reaction of the appropriate ethoxycarbonylmethyl esters with primary and secondary alkylamines and cyclic amines under mild conditions in good to excellent yields in the presence of TBD was achieved. The usefulness of TBD as an efficient catalyst has been shown in the example of aminolysis reaction with secondary cyclic amines where from a number of N-containing bases tested, such as TEA, pyridine, DMAP, DBU, imidazole, TMG and MTBD, only TBD was found capable to catalyse this reaction. It should be admitted that aminolysis reactions of 1,4-DHP 3a-d with secondary amines in the absence of TBD did not proceed at all and with primary ones aminolysis occurred with very low reaction rates. Aminolysis reactions of ethoxycarbonylmethyl ester of 1,4-dihydropyridines with 1-propyl-, 2-propyl-or 1-butylamine as well as secondary alkylamines and cyclic amines proceeded with good to excellent yields in all cases. It was also found that there is no significant influence of substituents at position 4 and the other ester moiety of 1,4-dihydropyridine on the aminolysis reaction with cyclic amines. The absence of aminolysis for ethoxycarbonylmethyl esters with sterically crowded secondary amines, such as diisopropylamine and diphenylamine or 1-naphtylamine was caused by steric hindrance of the bulky structure of the amines. Aminolysis reactions in all cases occurred regioselectively, as other alkyl esters of the 1,4-DHP molecule were not involved in the reaction. In the example of 2-propylamine, piperidine and morpholine it was shown that reactions can be performed both by using the reacting amine as solvent and nucleophile, however in this case a 15 fold excess of the amine should be used. In our view, it is more practical to perform aminolysis reactions in DMF as the amine in this case can be used in a reduced amount. The elaborated methodology of direct catalytic amide formation will certainly find its applications in the synthetic pathways for constructing of various heterocyclic compounds for further pharmacological studies.