Synthesis of Tunable Fluorescent Imidazole-Fused Heterocycle Dimers

A short, concise, and one-pot synthesis of imidazo-fused heterocycle dimers with tunable fluorescent properties has been developed. By the first time use of glyoxal dimethyl acetal in the Groebke–Blackburn–Bienaymé (GBB) three-component reaction (3CR), the innovation features a new series of fluorescence-tunable imidazo-fused heterocycle dimers exhibiting a broad substrate scope with good yields. Luminescence studies demonstrate that these GBB-dimers possess color-tunable properties, and their emission colors can be successively changed from blue to green and yellow by easy substituent control.

T here are many natural and synthetic symmetrical small molecule dimers with potential biological activities, such as anticancer, 1 antimalarial, 2 antibacterial, 3 and opioid antagonist activities. 4,5 One reason to synthetically aim for symmetrical compounds are homodimeric symmetrical receptors, such as that for PD-L1. 6 The imidazo[1,2-a]heterocyclic scaffold 7 accessible by the Groebke−Blackburn− Bienaymé(GBB) multicomponent reaction (MCR) is wellknown in many FDA-approved drugs, such as miroprofen, 8 zolpidem, 9 and DS-1. 10 The first imidazo[1,2-a]pyridine dimer was reported in 2015 by Manna et al. and was produced by the annulation of nitrosopyridine with alkynes ( Figure 1). 11 In 2016, Kudo disclosed the synthesis of noxious organism control agents exploiting the condensation of 2-aminopyridine and imidazo-bromomethyl ketone. 12 The GBB MCR reaction is an efficient way to get the important imidazo [1,2a]heterocycle scaffold with various aldehydes. 13 Based on our ongoing interest in MCR chemistry, we described the fast construction of a series of symmetric imidazo[1,2-a]heterocycle dimers by one-pot GBB reaction. Importantly, it is the first time that glyoxal dimethyl acetal, which acts as an orthogonal bifunctional monoprotected building block to achieve a new series of fluorescent imidazo[1,2-a]heterocycle dimers, was used in the GBB-3CR.
We first selected 1a and 2a as model substrates and employed various molar ratios, solvents, and catalysts, and glyoxal dimethyl acetal (60% in H 2 O) for condition optimization (Table 1). First, we screened the ratio of 1a, glyoxal dimethyl acetal, and 2a (entries 1−4). We used scandium triflate (Sc(OTf) 3 ) as catalyst and methanol as solvent because they are the most often used conditions for GBB-3CR. The reaction with ratio 1a/glyoxal dimethyl acetal/ 2a at 1:1:1 yielded product in 24% yield, and those with ratios 2:1:2, 2.2:1:2.2, and 1.3:1:1.3 gave 74%, 64%, and 34%, respectively. With the best ratio 2:1:2, we tried to find best solvent for this reaction. The product 3au was generated in 45% yield when we used trifluoroethanol (TFE) as solvent (entry 5). Water is also a widely used solvent in GBB-3CR; however, it only gave very low yield of 11% (entry 6). The reaction with acetonitrile as solvent gave 3au in 36% yield, while only 21% and 17% yield were achieved with solvent free reaction and PEG40, respectively (entries 7−9). Subsequently, we surveyed the effects of using different catalysts. When 4methylbenzenesulfonic acid (PTSA) was employed, 64% yield of product was obtained (entry 5). Inorganic acids such as perchloric acid and acetic acid gave product in 43% and 48% yield, respectively, whereas ammonium chloride could generate 3au in 51% yield. Zirconium tetrachloride (ZrCl 4 ) as Lewis acid could afford the desired product 3a in 63% yield. Using glyoxal (40 wt % in H 2 O) as the dialdehyde source gave a lower 40% yield. In addition, we also heated this reaction at 80°C for 12 h, resulting in 54% yield. Having identified the optimal reaction conditions ( Table 1, entry 2), we evaluated the substrate scope of the newly developed synthetic protocol (Scheme 1). When tert-butyl isocyanide reacted with substituted 2-aminopyridine with different electron-withdrawing groups, desired products were finally obtained in relatively good yields (3aa−3ad). Gratifyingly, cyclohexyl isocyanide was able to afford desired product 3ae in 81% yield. The use of various substituents on the 2aminopyridine regardless of their electronic characteristics, such as chloro (3af), bromo (3ag, 3ah), iodo (3aj), trifluoromethyl (3ak), methyl (3al), and methyl formate (3am), afforded the corresponding products in 35−66% yields.
To verify the synthetic practicality of this simple workup reaction, we carried out a gram-scale experiment in which the model reaction was performed on a 5 mmol scale; compound 3bc was isolated in 54% yield (1.69 g) by prolonging the reaction time to 2 h (Scheme 2a). Further application was demonstrated by the hydrolysis of compound 3am (Scheme 2b). The hydrolysis of 3am proceeded smoothly, giving the corresponding 3,3′-bis(cyclohexylamino)-[2,2′-biimidazo[1,2a]pyridine]-6,6′-dicarboxylic acid 3bo with 90% yield. 14 In addition to synthesis of symmetric GBB dimers, we also explored unsymmetric synthesis, incorporating two different imidazo heterocycles. As shown in Scheme 3, 5-chloropyridin-2-amine and 4-bromopyridin-2-amine were employed at the same time to afford unsymmetric compound 3bp in 26% yield, while the two homodimers 3bb and 3bd were generated in 40% and 8% yield, respectively. Likewise, another example produced unsymmetric 3bq in 28% yield and symmetric 3br and 3bs in 36% and 8% yield. We obtained the crystal structure of 3bp ( Figure S1).
Then, we investigated the luminescence properties of these GBB dimers. First, we determined a suitable wavelength for the photoluminescence assay by UV/vis spectroscopy. The UV/vis absorption spectrum of 3ae recorded in different solvents showed that THF is the best solvent to give a strong absorption band centered at 390 nm with another maxima (280 nm) in the ultraviolet region ( Figure S2A). Next, we recorded the UV/vis absorption spectra of 3bj, 3bm, 3aa, 3al, 3ai, 3ag, and 3ak in THF and obtained their maximum absorption wavelengths ( Figure S1B). Due to the weak fluorescence intensities achieved from the λ max in the ultraviolet region of these dimers, we chose another λ max in the visible region and tested the luminescence activity of 3ae with an excitation at 390 nm in different solvents, and THF turned out to be the best solvent, showing the highest luminescence intensity (Figure 2A). Then, we carried out luminescence photophysical studies on further GBB-dimer compounds. With excitation wavelengths at 365 or 370 nm, 3bj and 3bm, both containing aromatic amine moieties, emitted a blue luminescence at 455 nm in THF at 25°C. When arylamino substituents were changed to alkylamino substituents like tert-butylamino or cyclohexylamino groups, the emission wavelengths of 3aa and 3ae were red-shifted to 460 nm (light blue) or 500 nm (green). Interestingly, when an electron-donating methyl group was introduced on the pyridine ring, compound 3al could achieved a slight blue shift to 490 nm compared to that of 3ae (green). The electronwithdrawing nitrogen atom (3ai, 520 nm), 5-Br (3ag, 530 nm), or 5-CF 3 (3ak, 545 nm) employed with the pyridine resulted in the emission band being red-shifted to the yellow color range. Notably, 3ag showed a significantly weak fluorescence intensity, suggesting that 5-Br could be used to reduce luminescence activity. The relative fluorescence quantum yields (Φ) of compounds in Figure 2 are also summarized in Table S3 (see Supporting Information).
In summary, we have reported a multicomponent reaction of isocyanide, amidine, and glyoxal dimethyl acetal leading to various tunable fluorescence imidazole-fused heterocycle dimers. This method features high synthetic efficiency, mild conditions, operational simplicity, and broad substrate scope. A plausible mechanism has also been proposed in the Supporting Information. Furthermore, these compounds possess color fine-tunable luminescence properties, and we can achieve a sequentially change in the emission colors of these GBB-