Synthesis of novel alkynyl imidazopyridinyl selenides: copper-catalyzed tandem selenation of selenium with 2-arylimidazo[1,2-a]pyridines and terminal alkynes.

Alkynyl selenides have attracted considerable research interest recently, owing to their applications in the biological and pharmaceutical fields. The Cu-catalyzed tandem reaction for the synthesis of novel alkynyl imidazopyridinyl selenides is presented. A one-pot synthesis route afforded alkynyl imidazopyridinyl selenides in moderate to good yields. This was achieved by a two-step reaction between terminal alkynes and diimidazopyridinyl diselenides, generated from imidazo[1,2-a]pyridines and Se powder, using 10 mol % of CuI and 1,10-phenanthroline as the catalytic system under aerobic conditions. The C(sp2)-Se and C(sp)-Se bond-formation reaction can be performed in one-pot by using inexpensive and easy to handle Se powder as the Se source. The reaction proceeded with terminal alkynes having various substitutions, such as aryl, vinyl, and alkyl groups. The obtained alkynyl imidazopyridinyl selenide was found to undergo nucleophilic substitution reaction on Se atom using organolithium reagents and 1,3-dipolar azide-alkyne cycloaddition based on the alkyne moiety.

Introduction

Imidazo[1,2-a]pyridines are important heterocycles that serve as key functional groups in many biologically active substances and pharmaceuticals, such as zolpidem, alpidem, and GSK812397 [1-3]. Therefore, the development of multiple chemical modification methods, at the 3-position of the imidazo[1,2-a]pyridine skeleton, for the synthesis of 3-substituted-imidazo[1,2-a]pyridines with potential bioactivity, has been reported [4-7]. Similarly, organoselenium compounds have also received increased attention in recent years due to their promising applications as bioactive substances in drug discovery [8]. Among these compounds, alkynyl selenides have attracted interest in the last two decades owing to their applicability in biological and pharmaceutical fields [9-10]. For example, butyl (2-phenylethynyl)selenide (I, Figure 1) has an antinociceptive effect on the formalin test in mice [11], selanyl acetylenic retinoids II show an RAR agonist activity [12], and bis-alkynylselenides III exhibits a binding interaction between calf-thymus DNA and human serum albumin [13]. Moreover, imidazopyridine derivatives IV with selanyl groups, 3-aryl- or alkylselanylimidazo[1,2-a]pyridines, were reported to act as potential antioxidants and showed antiproliferative activity [14-15]. However, there is no reported example of the synthesis of alkynyl imidazopyridinyl selenides.

Figure 1

Biologically active selenides having alkynyl or imidazopyridinyl groups.

The Se–C bond-formation reaction using transition metals such as Pd, Ru, Ni, Fe, and Cu as catalysts is one of the most powerful synthetic tools for preparing organoselenium compounds [16-18]. Diselenides (RSeSeR) and selanyl halides (RSeX) have been widely used as Se sources in these reactions. However, they have poor commercial availability and require complicated synthetic routes. Therefore, an alternative approach using the commercially available and easy-to-handle Se powder has attracted significant attention [15,19-26]. This method involves a transition-metal-catalyzed one-pot, three-component reaction in which two functional groups are simultaneously introduced on the Se atom via double selenation. As examples, the following Cu-catalyzed one-pot reactions have been reported for the synthesis of unsymmetrical selenides with imidazopyridinyl groups substituted at position 3. Guo and Li et al. reported the reaction of Se powder with imidazopyridine and aryl iodides in the presence of KOH (2 equiv) as base using Cu(OAc)2 catalyst to form aryl imidazopyridinyl selenides [15]. Guo, Han and Ma et al. also performed the synthesis of aryl imidazopyridinyl selenides in the presence of Ag2CO3 (2 equiv) and Cs2CO3 (2 equiv) using the CuI/1,10-phenanthroline catalytic system by replacing the aryl group donor with arylboronic acids [23]. Zhou et al. reported the reaction of Se powder with imidazopyridine and aryl iodides or alkyl halides in the presence of Na2CO3 (2 equiv) using the NiBr2/2,2-bipyridine system to give aryl or alkyl imidazopyridinyl selenides [24]. In these reactions, aryl iodides, arylboronic acids, and alkyl halides are coupled with Se powder to form diaryl or dialkyl diselenides, followed by C–H selenation with imidazopyridines to form the corresponding compounds. We also reported the one-pot two-step reaction of Se powder with imidazopyridine and triarylbismuthines using the CuI/1,10-phenanthroline catalytic system without bases, which formed similar selenides [25]. In this reaction, unlike the former, bis(imidazo[1,2-a]pyridin-3-yl) diselenides are generated through C–H selenation at the 3-position of 2-arylimidazopyridines with Se powder, followed by the cross-coupling reaction between diselenides and triarylbismuthines. These one-pot reactions are limited to C(sp2)–Se–C(sp2) or C(sp2)–Se–C(sp3) bond-formation reactions. However, C(sp2)–Se–C(sp) bond formation reactions using the imidazopyridines and alkyne derivatives have not been reported to date. Based on previous reports and our ongoing investigation of the synthesis of unsymmetrical selenides with an imidazo[1,2-a]pyridine ring, this study focused on the Cu-catalyzed one-pot C(sp2)–Se and C(sp)–Se bond formation for the synthesis of novel alkynyl imidazopyridinyl selenides using Se powder, 2-arylimidazo[1,2-a]pyridines, and terminal alkynes.

Results and Discussion

Synthesis of alkynyl imidazopyridinyl selenides

A Cu-catalyzed cross-coupling reaction using benzene ring substituted diaryl diselenides with terminal alkynes in the presence of bases is effective for synthesizing aryl alkynyl selenides [27-31]. We previously reported a simple method for the synthesis of bis(2-arylimidazo[1,2-a]pyridin-3-yl) diselenides using a Cu-catalyzed C–H selenation at the 3-position of 2-arylimidazo[1,2-a]pyridines with Se powder [32]. Initially, the reaction of bis(2-phenylimidazo[1,2-a]pyridin-3-yl) diselenide (2a), generated from Se powder and 2-phenylimidazo[1,2-a]pyridine (1a), with phenylacetylene (3a) was used as a model reaction to determine a suitable base and an equivalent number of reagents (Table 1). The key intermediate 2a was prepared in situ from 1a (0.5 mmol) and Se powder (0.5 mmol) in the presence of 10 mol % of CuI and 1,10-phenanthroline at 130 °C in DMSO under aerobic conditions without bases using the method reported previously [25,32]. The reaction mixture was then treated with phenylacetylene (3a, 0.5 mmol) and various bases at room temperature. The formation of 4aa was confirmed by thin-layer chromatography. The use of various bases (2 equiv) such as K2CO3, Na2CO3, and triethylamine resulted in the formation of the expected alkynyl imidazopyridinyl selenide 4aa in moderate to good yields (Table 1, entries 1–8). Among them, Na2CO3 was identified as the optimal base in terms of yield of product 4aa and reaction time (entry 5 in Table 1). Notably, during the one-pot reaction, both selanyl groups from the diselenide transferred to the product 4aa. When no base was added or the amount of the base was reduced, the yield of 4aa decreased significantly (Table 1, entries 9 and 10). Moreover, increasing the amount of the alkyne 1a or Na2CO3 did not affect the progress of the reaction (Table 1, entries 5, 11, and 12). Consequently, the optimal result was obtained when diselenide 2a was treated with equal amounts of alkyne 1a and two equivalents of Na2CO3 under aerobic conditions at room temperature (Table 1, entry 5). The reaction was also attempted by mixing the three components (Se powder, 1a, and 3a) in the presence of Na2CO3 at 130 °C, but unfortunately it did not proceed and gave a complex mixture (Table 1, entry 13).

Table 1

One-pot reaction of Se powder with 1a and 3aa.

Entry	Alkyne 3a (equiv)	Base (equiv)	Time (h)	Yield of 4aa (%)b
1	1	K2CO3 (2)	3	60
2	1	K3PO4 (2)	3	34
3	1	KOH (2)	3	20
4	1	KOt-Bu (2)	24	30
5	1	Na2CO3 (2)	2	74
6	1	Cs2CO3 (2)	2	36
7	1	NaHCO3 (2)	4	42
8	1	Et3N (2)	3	73
9	1	Na2CO3 (1)	3	42
10	1	–	24	20
11	2	Na2CO3 (4)	2	73
12	1	Na2CO3 (3)	2	69
13c	1	Na2CO3 (2)	1	–

aConditions: 1a (0.5 mmol), Se (0.5 mmol), 3a (0.5 mmol), CuI (0.05 mmol), 1,10-phenanthroline (0.05 mmol), DMSO (3 mL); bisolated yield; csimultaneously added all reagents of 1a, Se, 3a, and Na2CO3 at 130 °C.

Single crystals suitable for X-ray analysis of 4aa were obtained by repeated recrystallization from dichloromethane/hexane as solvent. Figure 2a shows the crystal structure of 4aa, revealing that the ethynylselanyl group is located at the 3-position of the imidazo[1,2-a]pyridine core, and the bond angle of C1–Se–C2 was 100.45°. The imidazo[1,2-a]pyridine plane and the phenyl ring were observed to be slightly twisted, with a C2–C3–C4–C5 torsion angle of 10.28°. 2-Phenylimidazo[1,2-a]pyridine moieties of neighboring molecules were arranged into slipped-parallel π-stacks with head-to-tail or head-to-head orientations. The distances between parallel mean planes were 3.427 and 3.428 Å (Figure 2b).

Figure 2

(a) ORTEP drawing of 4aa and (b) its stacking structure.

To demonstrate the efficiency and to broaden the scope of the above-mentioned one-pot, two-step protocol, the reactions of 2-arylimidazopyridines 1 (1 mmol), Se powder (1 mmol), and terminal alkynes 3 (1 mmol) in the presence of Na2CO3 (2 mmol) were investigated under the optimized conditions. This method involved forming the diselenides, followed by the addition of terminal alkynes and Na2CO3 to the same reaction flask at room temperature. The reaction of imidazopyridine 1a and Se powder with various terminal alkynes 3b–e containing aryl groups yielded the corresponding arylalkynyl imidazopyridinyl selenides 4ab–ae, respectively, in 41–57% yields (Table 2, entries 1–4). The electronic nature of the substituents in the arylalkynes 3 did not affect the outcome of the reaction. For terminal alkynes 3f and 3g with a heteroaryl group such as thiophene (Table 2, entry 5) and the vinyl group (Table 2, entry 6), the coupling products 4af and 4ag were also isolated with yields of 61% and 71%, respectively. Conversely, 1-hexyne 4h with a butyl moiety as the alkyl group formed 4ah with a lower yield (see Table 2, entry 7) than those observed for other terminal alkynes.

Table 2

One-pot two-step synthesis of alkynyl imidazopyridinyl selenides 4a.

Entry	Product 4	Yieldb	Reaction timec
1	4ab	57%	2 h (2 h)
2	4ac	51%	2 h (3 h)
3	4ad	41%	2 h (2 h)
4	4ae	48%	2 h (2 h)
5	4af	61%	2 h (3 h)
6	4ag	71%	2 h (5 h)
7	4ah	31%	2 h (21 h)
8	4ba	69%	2 h (2 h)
9	4ca	58%	2 h (2 h)
10	4da	77%	2 h (2 h)
11	4ea	41%	3 h (3 h)
12	4fa	0%	24 h
13	4ga	68%	2 h (2 h)
14	4ha	61%	2 h (2 h)
15	4ia	69%	3 h (2 h)
16	4ja	66%	2 h (3 h)
17	4ka	72%	2 h (2 h)
18	4la	51%	3 h (2 h)
19	4ma	59%	2 h (2 h)

aConditions: 1 (1 mmol), 3 (1 mmol), Se (1 mmol), CuI (0.1 mmol), 1,10-phenanthroline (0.1 mmol), Na2CO3 (2 mmol), DMSO (3 mL); bisolated yields; cthe reaction time for the synthesis of diselenides 2 is provided, followed by the time for alkynyl imidazopyridinyl selenides 4 in parentheses.

Next, the reaction of 2-phenylimidazopyridines 1b–e with electron-donating or halogen groups at the 6-position of the imidazopyridine ring were tested and gave the desired products 4ba–ea in fair to good yields (Table 2, entries 8–11). Conversely, imidazopyridine 1f with an electron-withdrawing trifluoromethyl group did not yield the corresponding product 4fa, because the diselenide 2f could not be generated (Table 2, entry 12). The reaction not only proceeded for the 6-substituted 2-phenylimidazopyridines but also for 2-arylimidazopyridines 1g–m with a substituent on the phenyl group at the 2-position of the imidazopyridine ring, and the coupling products 4ga–ma were obtained in 51–72% yields (Table 2, entries 13–19).

We also performed control experiments to investigate the reaction pathway and mechanism. The reaction of the isolated diselenide 2a with phenylacetylene (3a) under the standard conditions afforded the desired product 4aa in 80% yield. On the other hand, under an argon atmosphere, the reaction yield decreased by approximately half. This reaction, without Na2CO3 as base, also afforded 4aa in 85% yield (Scheme 1, reaction 1). Although bis(imidazo[1,2-a]pyridin-3-yl)monoselenides 5 could form in situ [32], the reaction of 5 with acetylene 3a under the standard conditions did not proceed (Scheme 1, reaction 2).

Scheme 1

Control reactions.

The reaction mechanism for this coupling reaction is presently unclear. We propose that the reaction mechanism may be similar to that of the C(sp)–Se bond formation of terminal alkynes with diaryl diselenides reported by Stieler and Schneider [31]. Based on this report and the above control experiments, a plausible selenation reaction mechanism is shown in Figure 3. The first step of the reaction involves the generation of intermediate A by the oxidative addition of the Cu(I) catalyst to the diselenide 2. The terminal alkyne coordinates with intermediate A to form a π-complex B, and a ligand exchange reaction from B occurs to produce intermediate D, together with the elimination of selenol C. The selenol C is oxidized to diselenide 2. Finally, the intermediate D undergoes a reductive elimination to form the desired product 4, with the regeneration of Cu(I). As an alternative route, we also surmise that Cu–acetylide E attacks intermediate A to produce intermediate D. Although this reaction was performed under aerobic conditions, Glaser-type homocoupling of terminal alkynes did not occur, and no diynes were observed as byproducts. Moreover, the reaction of diselenides 2a with 3a without a base afforded the corresponding product 4aa in good yield (Scheme 1, reaction 1). Therefore, it was concluded that this reaction proceeds predominantly via the intermediate B route. The base appears to trap the protons generated during the first step involving the derivation of diselenide 2 from imidazopyridine 1 and Se powder.

Figure 3

Proposed mechanism.

Transformation from alkynyl imidazopyridinyl selenides

To investigate the chemical reactivity of the alkynyl imidazopyridinyl selenides, several reactions were performed (Scheme 2). Treatment of 4aa with two equivalents of phenyllithium in THF at −78 °C led to a nucleophilic substitution reaction with the elimination of the ethynyl group to form the desired phenylimidazopyridinyl selenide 6a in 49% yield. In the reaction with n-butyllithium, alkyl derivative 6b was isolated in the same way. The reaction of 4aa with the Ruppert–Prakash reagent (TMSCF3) in the presence of Cs2CO3 as base in MeCN at 0 °C gave product 7 with a trifluoromethyl group. Stefani et al. reported the 1,3-dipolar azide–alkyne cycloaddition (AAC) of organotellanyl alkynes with organic azides in the presence of a copper reagent to form 5-organotellanyl-1,2,3-triazoles [33]. Based on these findings, we examined the reaction of Cu-mediated AAC. The reaction of 4aa with benzyl azide in the presence of one equivalent of CuI and pentamethyldiethylenetriamine (PMDETA) in THF at 60 °C gave the desired 5-selanyl-1,2,3-triazole 8 in 72% yield. This reaction yielded a single product, and the regiochemistry of 5-selanyltriazole 8 was confirmed by single crystal X-ray analysis (see Supporting Information File 1). The reaction performed using 10 mol % of CuI and PMDETA as catalytic system afforded only a small amount of product 8 (12%).

Scheme 2

Transformation from 4aa.

Based on the results obtained in this study, the synthesis route still has some limitations such as the yields of alkynyl imidazopyridinyl selenides and the scope of substrates. Nevertheless, the scope of future research includes the application of this synthesis route using other heterocycles, and the investigation of the biological activity of the compounds obtained via this synthesis route.

Conclusion

In this study, the synthesis route for novel alkynyl imidazopyridinyl selenides using the Cu-catalyzed one-pot reaction of Se powder with imidazo[1,2-a]pyridines and terminal alkynes was developed. A variety of desired compounds was synthesized using a simple operation that can be performed under aerobic conditions. Moreover, the results showed that the obtained compounds underwent nucleophilic substitution reactions involving the elimination of the alkyne moiety on Se atoms to form aryl or alkyl imidazopyridinyl selenides and regioselective 1,3-dipolar azide–alkyne cycloaddition to form 5-selanyl-1,2,3-triazole. The investigation of the biological activity of the compounds obtained in this study and the application of this synthesis route using other heterocycles, instead of imidazopyridine, are currently underway in our laboratory.

Experimental

General procedure for the synthesis of alkynyl imidazopyridinyl selenides

A solution of 2-phenylimidazo[1,2-a]pyridine (1a, 1.0 mmol), selenium powder (79 mg, 1.0 mmol, 1 equiv), CuI (14 mg, 0.1 mmol, 10 mol %) and 1,10-phenanthoroline (18 mg, 0.1 mmol, 10 mol %) in DMSO (3 mL) was heated at 130 °C under air atmosphere. After the reaction was completed, the mixture was allowed to cool to room temperature. Then, the alkyne (3, 1.0 mmol, 1 equiv) and Na2CO3 (212 mg, 2.0 mmol, 2 equiv) were added and the mixture was stirred at room temperature. After the reaction was completed, the reaction mixture was diluted with CH2Cl2 (30 mL) and 5% aqueous ammonia (30 mL) at 0 °C. The phases were separated and the aqueous layer was extracted with CH2Cl2 (20 mL × 2). The combined organic layer was washed with 5% aqueous ammonia (30 mL × 3), dried over anhydrous magnesium sulfate, filtered, and concentrated under reduced pressure. The residue was purified by column chromatography using hexane/AcOEt as eluent to give the desired products 4aa–ma.

Characterization data of all new compounds, synthetic procedures for compounds 6–8, X-ray crystallography details, and copies of spectra.

X-ray crystal structure of 4aa.

X-ray crystal structure of 8.