Gheorghita Zbancioc1, Ionel I Mangalagiu1,2, Costel Moldoveanu1. 1. Chemistry Department, Alexandru Ioan Cuza University of Iasi, 11 Carol 1st Bvd., 700506 Iasi, Romania. 2. Institute of Interdisciplinary Research-CERNESIM Centre, Alexandru Ioan Cuza University of Iasi, 11 Carol I, 700506 Iasi, Romania.
Abstract
Azaheterocycles rings with five and six members are important tools for the obtaining of fluorescent materials and fluorescent sensors. The relevant advances in the synthesis of azaheterocyclic derivatives and their optical properties investigation, particularly in the last ten years, was our main objective on this review. The review is organized according to the size of the azaheterocycle ring, 5-, 6-membered and fused ring azaheterocycles, as well as our recent contribution on this research field. In each case, the reaction pathways with reaction condition and obtained yield, and evaluation of the optical properties of the obtained products were briefly presented.
Azaheterocycles rings with five and six members are important tools for the obtaining of fluorescent materials and fluorescent sensors. The relevant advances in the synthesis of azaheterocyclic derivatives and their optical properties investigation, particularly in the last ten years, was our main objective on this review. The review is organized according to the size of the azaheterocycle ring, 5-, 6-membered and fused ring azaheterocycles, as well as our recent contribution on this research field. In each case, the reaction pathways with reaction condition and obtained yield, and evaluation of the optical properties of the obtained products were briefly presented.
Entities:
Keywords:
five and six membered ring azaheterocycles; fluorescence; optical properties; synthesis
The synthesis of fluorescent azaheterocycles continues to arouse strong interest due to their great potential for application as sensors and biosensors, luminophores on in the construction of Organic Light-Emitting Diode (OLED) devices, laser and other semiconductor devices [1,2,3,4], as well as to their potential biological properties as antimicrobial [5], antifungal [6], anticancer [7,8], antituberculosis [9,10] antioxidant [11] and anti-HIV [12] agents.The advantages of the azaheterocyclic fluorophores, such as small size, enriched photostability, a wide and tunable spectral range, and, frequently, high brightness, are the reason why these fluorophores are preferred and used in various medical application. Probe structure can be modified to adjust excitation and emission wavelengths, target-binding affinity, chemical reactivity, and subcellular localization [13,14,15,16].In this review, we try to present an overview of the newest research in the synthesis of fluorescent azaheterocyclic derivatives, from the literature reported during the last ten years. The methodology adopted for literature search and selection was to access the Reaxys database for “fluorescence”, “azaheterocycles” and “fluorescent azaheterocycles” keywords. The obtained results, as well as the references cited, were selected to be included in the present review if they present the synthesis of fluorescent azaheterocycles, and the fluorescent properties of these compounds were evaluated.The present review was organized taking into account the size of the azaheterocycle, the nature of the cycle (monocycle and fused polycycles), as well as our contribution in this research field.
2. Synthesis and Fluorescent Properties of Five- and Six-Membered Ring Azaheterocycles
2.1. Five Membered Ring Azaheterocycles
Five membered ring azaheterocycles, such as pyrroles, diazoles, triazoles, tetrazoles and their fused derivatives, are privileged scaffolds posing a wide range of biological activities and diverse applications in organic electronics [17,18,19,20,21,22,23,24,25]. Due to these properties, many researchers were focused on the obtaining of new compounds with such skeleton.Martínez-Lara et al. [26] developed a new obtaining methodology of two different angular indolocarbazole moieties by using two sequential gold- and molybdenum-catalysis to obtain new indolo [2,3-c]carbazoles as potential luminophores with application in OLED devices.A selection of 1,1-bis(indol-3-yl)-3-alkyn-2-ols 3, was readily prepared through the alkylation of the indole derivatives 1 with methyl or phenyl glyoxal, followed by a standard Sonogashira-type reaction with 2-nitroaryl iodides. Next, these compounds underwent a cyclization reaction, promoted by NaAuCl4, affording the corresponding carbazoles 4 (see Scheme 1).
Scheme 1
Synthetic procedure used for the obtaining of indolylcarbazole derivatives 4.
Without further purification, the crude carbazoles were directly subjected to Mo-catalyzed Cadogan reaction delivering the desired indolocarbazoles 5. All indolocarbazoles were obtained in high yields. The authors [26] used microwave irradiation for the synthesis of the indolocarbazole derivatives 4 and 5, and obtained final products in much shorter time and with better yields (see Scheme 2).
Scheme 2
Synthesis of indolo[2,3-c]carbazole derivatives.
To obtain a perspective on the effect that the C-7 substituent of the indolocarbazole skeleton (methyl in 5aa, and phenyl in 5ba) the photoluminescent properties of two selected compounds, 5aa and 5ba in DMSO were investigated Table 1.
Table 1
Fluorescent properties of the selected 5aa and 5ba in DMSO.
Compound
λabs(nm)
εmax(L·mol−1·cm−1)
λem(nm)
Φfl(%)
τ(ns)
kf(107·s−1)
Knr(107·s−1)
5aa
338
20,700 ± 300
407
72 ± 4
7.4 ± 0.1
9.54 ± 0.10
3.89 ± 0.04
351
23,700 ± 300
377
6900 ± 200
397
8200 ± 200
5ba
342
16,700 ± 200
424
69 ± 2
6.4 ± 0.1
10.77 ± 0.05
4.84 ± 0.02
354
20,000 ± 200
384
6500 ± 100
402
7500 ± 100
Maximum absorption wavelength (λabs), molar absorptivity at the absorption maximum wavelength (εmax), maximum emission wavelength (λem), fluorescence quantum yield (Φfl), average lifetime (τ), and fluorescence (kf) amd non-radiative (knr) rate constants.
The phenyl-substituted 5ba indolo[2,3-c]carbazole shows a wider absorption wavelength range than methylsubstituted 5aa indolo[2,3-c]carbazole and both show fluorescence quantum yields around 70% in DMSO, double as the Φfl of some similar compounds from the literature. These compounds are potentially useful for optoelectronic applications due to their high extinction coefficient and fluorescence quantum yields.By combining 2H-imiazole 1-oxides 7a–l with pentafluorophenyl lithium 8 made in situ from pentafluorobenzene 6 and n-BuLi, Moseev et al. [27] were able to create novel pentafluoroaryl-modified derivatives of 2H-imidazole type 10a–l and 11a–l, as is presented in Scheme 3. Pentafluorophenyllithium 8 first attacks the imidazole-N-oxide 7a–l, resulting in the unstable σH-adduct 9 that can be converted into the product either by “addition-elimination” (Path A), leading to the formation of compounds 10a–l, or by “addition–oxidation” (Path B), leading to the creation of compounds 11a–l containing N-oxide group.
Scheme 3
Synthesis of pentafluoroaryl-modified derivatives.
As possible applications, the authors claim that the push-pull fluorophore systems containing both electron-donating (EDG) and electron-withdrawing (EWG) groups in the vicinal position could be used as push–pull fluorophore systems. The obtained molecule types 10 and 11 have undergone a photophysical study to determine the potential practical uses in the construction of photoactive materials. The authors results are shown in Table 2.
Table 2
The photophysical properties for the obtained molecules 10 and 11.
Compound
λabs (nm) a
λem (nm) b
Φfl (%) c
Compound
λabs (nm) a
λem (nm) b
Φfl (%) c
10a
259
316
<0.1
11a
281
316
<0.1
10b
266
316
<0.1
11b
278
317
<0.1
10c
263
317
<0.1
11c
279
316
<0.1
10d
272
316
<0.1
11d
282
316
<0.1
10e
272
317
<0.1
11e
283
316
<0.1
10f
261, 302
333, 420 (br)
<0.1
11f
297
322
<0.1
10g
304
333, 420 (br)
<0.1
11g
297
321
<0.1
10h
272
316
0.6
11h
272
317
<0.1
10i
305
331, 475 (br)
0.1
11i
298
320
<0.1
10j
305
335, 464 (br)
0.2
11j
297
325
<0.1
10k
277
317, 352 (br)
<0.1
11k
288
317
<0.1
10l
256
316
1.9
11l
277
317
<0.1
a Absorption maxima in MeOH. b Emission maxima in MeOH. c Absolute fluorescence quantum yields in MeOH, br-broad peak.
The authors concluded that the presence of EWG in the para-position of the phenyl group improved the fluorescence quantum yield of the produced fluorophores by measuring the quantum yield of polyfluorinated-2Himidazole derivatives 10 and 11.The phenomenon of intramolecular charge transfer (ICT) in polar protonic solvents (MeOH and EtOH) has been shown for several compounds, and connections between “structure-photophysical characteristics” have been found. The characteristics of the investigated photophysical properties allow them to adjust the structures of the photoactive molecules, which opens the possibility of using the synthesized push-pull systems in the development of difficult fluorometric molecular sensors.Pu et al. [28] synthesized antipyrine-containing diarylethenes derivatives 14 in their attempt to obtain novel multi-controllable photochromic and fluorescent derivatives (see Scheme 4).
Scheme 4
Synthesis of antipyrine-containing diarylethenes derivatives 14.
It was determined that 14o had an absolute fluorescence quantum yield of 1.4%. UV light (297 nm) irradiation caused the photocyclization reaction, which resulted in the synthesis of 14c with a quantum yield of 0.8%. As a result, the emission strength of 14o abruptly reduced, and the fluorescence changed from bright orange to darkness. Conversely, by exposing 14o with appropriate visible light, the fluorescence may be recovered.At 580 nm, the isomer 14o showed high brightly orange fluorescence. The emission strength of 14o reduced to 18% with the addition of 5.0 equiv of tetrabutylammonium hydroxide, and the color changed noticeably from bright orange to blackness as a result of the creation of deprotonated 14o’. The fluorescence could return to its initial form upon neutralization with 2.0 equiv of HCl. Similar to this, the stimulation of TBAH/HCl in acetonitrile could reversibly alter the fluorescence of 14c. When irradiated to UV/vis light, the fluorescence alterations between 14o’ and 14c’ was irreversible. The fluorescence of 14o’ stayed unaltered when irradiated to UV light, however when exposed to visible light (λ > 500 nm), the fluorescence of 14c’ might return to that of 14o’, as may be observed in Scheme 5. The results obtained by the authors shown that the base could suppress the photochromism of diarylethene with an antipyrine unit’s and acid could restore it.
Scheme 5
Structure changes of 14 induced by TBAH/HCl and UV/vis.
In order to examine the fluorescence variations of 14o, 5.0 equiv of several metal ions, including Al3+, Zn2+, Ni2+, K+, Cd2+, Ca2+, Cu2+, Ba2+, Pb2+, Cr3+, Co2+, Sr2+, Mg2+, Mn2+, Hg2+ and Fe3+, were added. The authors pointed out that the addition of Al3+ was the only metal ion that significantly affected the fluorescence of 14o; other metal ions had a negligible effect. As a result of this study, the diarylethene with an antipyrine unit type 14o demonstrated special base-gated photochromic properties and could be used as a highly selective naked-eye chemosensor for Al3+ detection.
2.2. Six Membered Ring Azaheterocycles
Electron-deficient six membered ring azaheterocycles, such as azines and diazines, are strongly desired and studied due to their potential biological activities and also to their potential applications in organic electronics [29,30,31,32,33].Motivated by the small size and high quantum yield (Φ = 60%) of the unsubstituted pyridin-2-amine, being a potential scaffold for a fluorescent probe, Li et al. [34], in their research for new multisubstituted aminopyridines, used the Rh-catalyzed coupling of vinyl azide with isonitrile to form a vinyl carbodiimide intermediate, which followed a tandem cyclization with an alkyne to the desired amine.The reactions were carried “one-pot”, using vinyl azide 15 and isonitrile 16, Rh-catalyst, proper ligand and 1,4-dioxane as solvent, under N2 atmosphere and at room temperature in the first stage, then after the vinyl azide spot disappeared on TLC, NH4Cl, NaHCO3, and alkyne were added, and the mixture was heated to 120 °C for 8 h (see Scheme 6).
Scheme 6
One-pot synthesis of multi-substituted aminopyridines 17–26.
For quantitative fluorescent detection, the solution of aminopyridine was then diluted to 10 μM. The measured parameters are presented in Table 3.
Table 3
Fluorescent properties of aminopyridines.
Compound
Yield[%]
λabs[nm]
λex[nm]
λem[nm]
Φfl[%]
71
270
390
480
34
18
24
270
390
480
31
19
65
270
390
480
44
20
52
270
390
485
31
21
60
270
390
485
27
22
52
270
390
485
32
23
53
270
390
485
22
24
17
258
345
455
2
25
67
270
390
480
35
26
57
270
390
480
30
λabs-absorption maxima in ethanol (longest wavelength transition), λex-excitation wavelenght, λem-maxima of the corrected emission spectra in ethanol, Φfl-the fluorescence quantum yield, external standard: 9,10-diphenylanthracene (Φ = 95%, in cyclohexane).
Compound 17 was derivatized in order to observe the variation of the photoluminescent properties, as is presented in Scheme 7.
Scheme 7
Derivatization of multisubstituted aminopyridine 17.
Thus, when the tertiary butyl group was cleaved using CF3COOH the obtained compound 27 showed no fluorescence. When the ester groups were hydrolyzed to carboxylic acid, the obtained compound 28 still had a good fluorescence (Φ = 31%). When compound 35 was reduced with LiAlH4 a high fluorescent (Φ = 81%) alcohol 29 was obtained in excellent yield, but the λem was reduced to 400 nm.The same authors [34], in order to apply the newly synthesized compound as fluorescent probe, used the click reaction to bind the fluorescent aminopyridine scaffold to biomolecules conjugated with alkynyl group (see Scheme 8). Firstly, they synthesized a Boc-NH protected compound 30 accordingly to the above-described method from corresponding starting materials, then the azido substituted derivative 31 was obtained via a Sandmeyer reaction. Finally, the azide 31 react easily with phenylacetylene or propynol (by using catalytic amounts of Cu(II)) to obtain the desired triazole products 32 or 33.
Scheme 8
Binding the fluorescent aminopyridine scaffold to biomolecules conjugated with alkynyl group.
The authors successfully applied this “click-and-probing” experiment to bovine serum albumin (BSA) conjugated with a terminal alkyne, demonstrating the biochemical application of this probe and of the fluorescent multisubstituted aminopyridines for detection and analysis.Piloto et al. [35] studied the use of acridine azaheterocycle as a photochemically removable protecting group for the carboxylic group of amino acids involved in neurotransmision. In this respect, a series of amino acids 34 (glycine, alanine, glutamic acid, β-alanine and γ-aminobutyric acid) protected on amino group with tert-butoxycarbonyl, was treated with 9-bromomethylacridine 35, the corresponding heterocyclic ester 36 being obtained (see Scheme 9). The coupling reaction requires potassium fluoride as base and N,N-dimethylformamide as solvent, and take place at room temperature.
Scheme 9
The reaction of tert-butoxycarbonyl amino protected amino acids with 9-bromomethylacridine 35.
UV/Vis absorption and emission spectra for the ester conjugates 36a–e were measured on degassed 10−5 M solutions in two solvent systems: absolute ethanol, and a methanol–HEPES buffer (80:20), the measured parameters are presented in Table 4.
Table 4
Yields, UV/VIS and fluorescence data for esters 36a–e in absolute ethanol and a methanol-HEPES buffer (80:20) solution.
Compound
Yield[%]
EtOH
MeOH-HEPES (80:20)
λabs[nm]
log ε
λem[nm]
Φfl[%]
Δλ[nm]
λabs[nm]
log ε
λem[nm]
Φfl[%]
Δλ[nm]
36a
Boc-Gly-OAcm
69
360
3.90
435
9
75
362
3.48
423
12
61
36b
Boc-Ala-OAcm
93
361
3.93
411
11
50
360
3.69
412
15
52
36c
Boc-Glu-OAcm
19
361
4.04
433
8
72
362
3.57
433
11
71
36d
Boc-β-Ala-OAcm
72
361
3.91
412
11
51
361
3.79
417
14
56
36e
Boc-GABA-OAcm
49
361
3.97
424
4
63
360
3.94
424
11
64
λabs-the maximum wavelength of absorption spectra, log ε-logarithm of the molar absorption coefficient λem-the maximum wavelength of photoluminescence spectra, Φfl-photoluminescence quantum yield, calculated using 9,10-diphenylanthracene as a standard (Φfl = 0.95 in ethanol), Δλ-Stokes’ shifts (Δλ = λem − λabs).
Due to the heterocyclic chromophore, the absorption maximum of compounds showed no influence of amino acid residue. Ester derivatives 36a–e displayed emission maxima between 411–435 nm in both solvents, with moderate Stokes’ shifts (50–75 nm). These esters exhibited higher fluorescence quantum yields in a methanol–HEPES buffer solvent system.The deprotection of the carboxylic group from the corresponding fluorescent derivatives in methanol-HEPES buffer (80:20) solutions was achieved by irradiation. The best results on photorelease of these amino acids from were obtained on irradiation at 350 nm. This ability of acridinyl methyl ester make them a suitable option for the photochemical release of functional molecules bearing a carboxylic acid group in organic synthesis and in cellular applications.In order to obtain new luminogens for sensing strong acids Tang et al. [36] used Suzsuki cross-coupling reaction. The luminogens consist of one pyridine, 1,3-diazine, 1,4-diazine, 1,2-diazine and phthalazine moieties as the central cores and two AIE-active tetraphenylethene units in the lateral sides. Aggregation induced emission (AIE) effect exhibiting high emission in concentrated solution or even in the solid state, hold great promise for a luminogen in practical applications.PY-TPE 39b, PYM-TPE 39c, PYA-TPE 39d, PYD-TPE 39e and PTZ-TPE 39f were easily synthesized by 4-(1,2,2-triphenylvinyl) phenyl boronic acid 37 reaction with 2,5-dibromopyridine 38b, 2,5-dibromopyrimidine 38c, 2,5-dibromopyrazine 38d, 3,6-dibromopyridazine 38e, 1,4-dibromophthalazine 38f under Suzuki cross-coupling in high yields (see Scheme 10). For comparison, an analogue molecule BZ-TPE 38a fused with phenyl unit was also prepared.
Scheme 10
Suzuki cross-coupling reaction of 4-(1,2,2-triphenylvinyl) phenyl boronic acid 37 with 2,5-dibromopyridine 38b, 2,5-dibromopyrimidine 38c, 2,5-dibromopyrazine 38d, 3,6-dibromopyridazine 38e, 1,4-dibromophthalazine 38f.
The photophysical properties of the luminogens were studied by UV-vis and fluorescence spectroscopies in CH3CN, and are presented in Table 5. These luminogens show a colorless character in common organic solvents, making them good candidates for colorimetric or fluorometric detection with less self-absorption disturbance. All compounds show very weak fluorescence emission in CH3CN, caused by non-radiative fashion arising from the rotation of tetraphenylethene units.
Table 5
Photophysical data for the as-prepared luminogens.
Compound
UV-Vis Absorption
Fluorescence
λabs[nm]
log ε
λem[nm]
Φfl[%]
τ[ns]
kf 107[s−1]
knf 107[s−1]
39a BZ-TPE
332
4.43
480
53.7
3.5
15.3
13.2
39b PY-TPE
340
4.57
481
42.6
3.3
12.1
16.3
39c PYM-TPE
346
4.42
482
31.2
3.0
10.4
22.9
39d PYA-TPE
363
4.51
484
14.6
2.0
7.3
42.7
39e PYD-TPE
343
4.24
450
0.6
1.3
0.46
76.2
39f PTZ-TPE
323
4.45
480
1.6
1.7
0.94
57.8
λabs-the maximum wavelength of absorption spectra recorded in CH3CN (10−5 M), log ε-logarithm of the molar absorption coefficient λem-the maximum wavelength of photoluminescence spectra measured in CH3CN-water (1:9), Φfl-photoluminescence quantum yield, τ-fluorescence lifetime, kf-radiation rate constant (kf = Φfl/τ), knf-non-radiative rate constant (knf = kf (1 − Φfl)/Φfl).
The emission spectra (in CH3CN–water) were recorded in order to determine the AIE effect in aggregate states of the as-prepared luminogens. Benzyl-, pyridine-, pyrimidine- and pyrazine-tetraphenylethenes (39a–d) exhibited high fluorescence quantum yields in aggregate states due to a typical AIE effect. 1,2-Diazine-tetraphenylethenes (pyridazine-39e and phthalazine-39f) have strong yellow fluorescence emission under protonation enabling AIE performance. The synergetic effect of AIE and the protonation on the 1, 2-diazine segments allows them to detect strong acids with very low pKa values.The similarities of the 4-hydroxy-1,3-thiazole unit, a chromophore and fluorophore, with naturally occurring luciferin, determine Menzel et al. [37] to obtain new of arylamine-modified thiazoles as donor-acceptor dyes. The donor part of the dyes was based on the 4-methoxy-1,3-thiazole core substituted with an arylamine (phenyl-, p-anisole-, p-tolyl-, or phenothiazine-) in the 5-position as donor, and a pyridine, pyrimidine, or pyrazine moiety in the 2-position as acceptor.The synthesis of the 4-hydroxy-1,3-thiazoles 42a–c involved a Hantzsch thiazole cyclizations between the corresponding azaheterocyclic thioamides 40a–c and ethyl 2-bromo-2-(4-nitrophenyl)acetate 41a. Similarly, starting from ethyl 2-bromo-2-(4-bromophenyl)acetate 41b and pyridine-2-carbothioamide 40a, compound 42d was prepared, then methylated via Williamson ether synthesis, with methyl iodide in DMSO. The reduction of the nitro group in 43a–c with freshly prepared Raney nickel and hydrazine in EtOH fallowed (see Scheme 11).
Scheme 11
Synthesis of new arylamine-modified thiazoles donor-acceptor dyes.
The reaction condition for the double N-arylation Buchwald–Hartwig cross-coupling reaction were: bis(dibenzylideneacetone)palladium(0) [Pd(dba)2] as the precatalyst, KOtBu as the base, and toluene as solvent. By using the P(tBu)3 reagent, the desired products were obtained in moderate to good yields (76–90%). The obtaining of both disubstituted A1 and B1, and the monosubstituted products A1m (69%) and B1m (88%), demonstrates the two-step nature of the reaction (see Scheme 12).
Scheme 12
N-arylation Buchwald–Hartwig cross-coupling reaction of arylamines 44a–c.
The Buchwald–Hartwig reaction starting with 43d, a thiazole substituted aryl halide, was not successful under the conditions of the double N-arylation of the amines 44a–c, the biarylphosphane 2-(dicyclohexylphosphanyl)-2′,6′-dimethoxy-1,1′-biphenyl (SPHOS) was required as ligand (see Scheme 13).
Scheme 13
N-arylation Buchwald–Hartwig cross-coupling reaction of thiazole substituted aryl halide 43d.
The arylamine donors has a strong influence on the emission quantum yields recorded in CH3CN solution at room temp, the phenyl-based triarylamines having good quantum yields (40–47%), while the p-anisole-based triarylamines show values below 1% for quantum yields, and consequently no fluorescence for the p-N,N′-dimethylaniline derivative. The obtained photoluminescence quantum yields (see Table 6) are correlated with the measured emission lifetimes (τ).
Table 6
Spectroscopic properties, in CH3CN at room temperature, of the synthesized dyes.
Dye
λabs[nm]
log ε
λabs[nm]
log ε
λem[nm]
Φfl[%]
τ[ns]
A1
301
4.33
405
4.44
547
47
3.83
A2
299
4.35
417
4.43
605
<1
0.26
A3
307
4.43
433
4.36
n.d.
n.d.
n.d.
B1
303
4.40
425
4.47
593
40
2.99
B2
302
4.40
439
4.46
611
<1
0.13
C1
302
4.32
426
4.36
601
8
1.26
C2
301
4.38
433
4.46
630
<1
<0.1 *
D1
292
4.11
380
4.24
478
90
3.12
D2
257
4.72
377
4.42 **
484 sh,
507
2
0.11
D3
240
4.77
373
4.40
455 sh,
470
<1
0.13
λabs-the maximum wavelength of absorption, log ε-logarithm of the molar absorption coefficient λem -the maximum wavelength of photoluminescence, Φfl-photoluminescence quantum yield, τ-fluorescence lifetime, n.d-not detected, *-below demand interval, **-measured in THF, sh.-shoulder.
Only the emission due to the carbazole moiety, as a main band, can be observed for compound D1 in the polar CH3CN, while for D2 and D3 the emissions are modest.The authors [37] carried out measurements of the absorptions (and emissions) in different solvents for compounds A2 and D1 in order to investigate them in more detail (see Table 7). The increasing of the solvent polarity induces a weak hypsochromic shift on the absorption maxima, but a bathochromic shift on the emission maxima. This behavior is due to a conformational transformation from a planar locally excited (LE) state to an intramolecular charge-transfer (ICT) or, consequently, to a twisted intramolecular charge-transfer (TICT) state.
Table 7
Spectroscopic behavior of dyes A2 and D1 in different solvents.
Solvent
A2
D1
λabs[nm]
log ε
λem[nm]
Φfl[%]
Stokes Shift[cm−1]
τ[ns]
λabs[nm]
log ε
λem[nm]
Φfl[%]
Stokes Shift[cm−1]
τ[ns]
Heptane
427
4.585
483, 512
63
3900
2.6
387
4.466
456, 464
97
4300
2.4
Dioxane
425
4.441
530
59
4700
3.8
385
4.399
472
100
4800
2.7
CHCl3
428
4.422
561
40
5500
4.0
387
4.235
475
95
4800
2.9
THF
425
4.485
552
43
5400
3.8
384
4.474
473
100
4900
2.8
MeOH
421
4.456
581
<1
6500
0.1
382
*
489
81
5700
3.3
CH3CN
417
4.434
603
1
7400
0.1
380
4.244
475
90
5300
3.1
λabs—the maximum wavelength of absorption, log ε—logarithm of the molar absorption coefficient λem—the maximum wavelength of photoluminescence, Φfl—photoluminescence quantum yield, τ—fluorescence lifetime, *—extinction coefficient could not be measured, due to the poor solubility.
Menzel et al. [37] tested also the ability of these dyes to act as ligands and synthesized seven new ruthenium complexes and measured their emission spectra. The synthesis of the heteroleptic RuII complexes involve the activation of the cis-(dmbpy)2RuCl2 precursor with AgPF6 prior to the complexation in acetone with the appropriate ligand (1 equiv.) for 24 h under reflux conditions (see Scheme 14).
Scheme 14
The synthesis of the heteroleptic RuII complexes.
Each complex shows an enhanced absorption in the visible part of the UV/Vis spectrum, due to additional ligand-centered (LC) π–π* transitions and metal-to-ligand charge-transfer (MLCT) transitions originating from 4-methoxy-1,3-thiazole ligands.
2.3. Fused Azaheterocycles
Fused azaheterocycles combine an electron-excessive pyrrole and an electron deficient azine ring which involve an uneven π-electron distribution. This uneven π-electron distribution induces interesting optical properties on the compound with such fused azaheterocycles and make them very attractive materials in optoelectronics [38,39]. Moreover, the variety of potential applications in the fields of medicinal of these compounds explains the increased interest of researchers in their study [40,41,42].Rajbongshi et al. [38] obtained new chromeno[2,3-b]indoles 47a–c as part of the series of chromenoindole derivatives by reacting 1-(α-amino-α-arylalkyl)-2-naphthol 45 with indole 46 at 100 °C in the presence of catalytic p-toluenesulfonic acid, I2 and tert-butyl hydroperoxide (TBHP), as is presented in Scheme 15.
Scheme 15
Synthesis of chromeno[2,3-b]indoles 47a–c.
In various solvents, the fluorescence spectra of the produced chromeno[2,3-b]indoles 47a–c alter and show a significant Stokes shift, ranging from 250 nm in acetonitrile to 186 nm in ethyl acetate. The chromeno[2,3-b]indoles’ fluorescence quantum yield was evaluated at 280 nm using tryptophan in water as a reference and at 313 nm using naphthalene. Table 8 displays the fluorescence quantum yields of obtained compounds.
Table 8
Fluorescence quantum yield (Φfl) of the chromeno [2,3-b]indole derivatives 47a–c in acetonitrile and ethyl acetate at 280 nm (tryptophan in water as reference) and at 313 nm (naphthalene in ethanol as reference).
Compound
Fluorescence Quantum Yield
Acetonitrile
Ethyl Acetate
280 nm
313 nm
280 nm
313 nm
47a
3.7
3.5
3.9
3.7
47b
3.6
3.7
4.3
3.5
47c
3.9
3.6
3.7
3.4
The investigated chromeno[2,3-b]indoles 47a–c produce fluorescence at a significantly lower energy compared to their absorption, and their fluorescence spectra exhibit a solvatochromic shift, which suggests intramolecular charge transfer in the excited state. The three chromeno[2,3-b]indoles’ with strong Stokes-shifted fluorescence suggests that they may be used as luminescent solar concentrators or scintillators.Li et al. [39] obtained a fused five-membered azaheterocycle with an aggregation-induced emission (AIE) characteristic using an unanticipated regioselective photoreaction.The starting compound o-TPBQ 48 were easily prepared through a facile one-step synthetic route via a modified Sonogashira coupling reaction according to the previously reported literature [43,44].The authors proposed all of the potential products, including the common six-membered ones, 50 C6-TPBQ′ and 51 C6-TPBQ″, as well as the five-membered ring product 49 (C5-TPBQ), although the likelihood of this is very low. They also considered the specific location of the N atom in o-TPBQ and the reported literature on the photoreaction. Surprisingly, the typical six-membered cyclized product (C6-TPBQ’ or C6-TPBQ”) was not obtained; instead, only the five-membered cyclized product 49, C5-TPBQ, was obtained (see Scheme 16). NMR and high-resolution mass spectroscopies were used to confirm the structure of C5-TPBQ.
Scheme 16
Regioselective photoreaction of o-TPBQ 48.
In DMSO/water solutions with various water fractions, the photoluminescence spectra of C5-TPBQ were recorded. This compound has a low fluorescence quantum yield in DMSO solution (1.1%), and when water is gradually added to the solution, an increased photoluminescence signal is obtained. The AIE characteristic was demonstrated by the 110-fold increase in emission intensity in DMSO/water mixes with 99% water compared with DMSO solution.This research provides a method for quickly and easily creating fused five-membered azaheterocyclic compounds with unique fluorescence properties. These compounds have a wide range of uses in the biological and optoelectronic domains.Having in view the synthesis of new 1H-pyrazolo[3,4-b]quinoxaline (PQX) derivatives with specific photophysical properties as potential materials for optoelectronics, Wojtasik et al. [45] tried to improve the Cadogan synthesis of these compounds. The authors used triphenylphosphine as reducing agent, in dimethylacetamide (DMAc) at 240 °C, under microwave irradiation and obtained PQX derivatives in much shorter time and with better yields of the final product (see Scheme 17).
Scheme 17
Cadogan synthesis of 1H-pyrazolo[3,4-b]quinoxaline derivatives 53a–g.
The substrates 52a–g were obtained by the coupling of the appropriate 2-iodonitrobenzene derivatives 54 with 1,3-disubstituted 5-aminopyrrazole 55 in the presence of palladium catalyst and BINAP (2,2′-bis(diphenylphosphino)-1,1′-binaphtyl), as is presented in Scheme 18. By this reaction, authors obtained the best yields, despite the long reaction time.
Scheme 18
The coupling of 2-iodonitrobenzene derivatives 54 with 1,3-disubstituted 5-aminopyrrazole 55.
The recorded emission spectra of compounds 53e–g reveal an emission maximum between 436 nm and 483 nm, according to the nature of the substituents from the 6th position and the used solvent. These results are presented in the Table 9.
Table 9
The photophysical constants of the compounds 23e–g in different solvents.
Compound
Solvent
c[mol dm3]
λabs[nm]
ε(λabs)[M−1 cm−1]
λem[nm]
Φfl[%]
53e
MCHX
2.94 × 10−5
396
5315
436
1.0
THF
4.68 × 10−5
399
3816
459
1.5
ACN
4.89 × 10−5
398
3865
461
2.1
53f
MCHX
3.68 × 10−5
402
5324
442
0.7
THF
3.83 × 10−5
404
5175
467
3.4
ACN
4.02 × 10−5
406
4852
479
67.2
53g
MCHX
3.17 × 10−5
399
4051
443
1.0
THF
3.43 × 10−5
397
4055
480
6.8
ACN
3.44 × 10−5
397
4156
483
11.6
λabs—spectral position of the first absorption maxima, ε(λabs)—magnitude of the molar absorptivity of λabs, λem—the spectral position of the fluorescence maxima, Φfl—the fluorescence quantum yield, MCHX-methylcyclohexane, THF—tetrahydrofuran, CAN—acetonitrile.
The introduction of the electron donor substituent (methyl group-53e) in the 6th position of 1,3-dimethyl-1H-pyrazolo[3,4-b]quinoxaline 53d did not changed the emission properties comparing with the unsubstituted 53d system, while the electron-accepting substituents (chlorine-53f and trifluoromethyl group-53g) shifted the fluorescence band twoards longer wavelenghts by 8 nm to 21 nm, respectively, and induced an increase of the quantum yield of the fluorescence.In order to develop a new family of thermally activated delayed fluorescence (TADF) emitters, utilizing the donor-acceptor scaffold, Goya et al. [46] focused on the use of the electron-deficient azaaromatic scaffold in place of the usual dibenzo[a,j]phenazine (DBPHZ) unit. Organic compounds that can display TDAF are very intense studied as emitters for efficient OLEDs, since they can achieve theoretically 100% internal quantum efficiency (IQE) by harvesting electrically generated triplet excitation and convert into the emissive singlet excitations through reverse intersystem crossing (rISC).Pyrido[2,3-b]pyrazine (PYPZ) moiety was selected as the electron-acceptor (A) unit, due to the both pyridine and pyrazine π-deficient heterocycles. When this electron deficient core is connected with an appropriate electron-donor (D), intramolecular charge-transfer (ICT) in the excited state will occur and CT states should become the first singlet excited state (S1). As donor part was selected dihydrophenazasiline (DHPHAzSi) since DHPHAzSi compounds are moderate electron donor.The 7-bromo-2,3-diphenylpyrido[2,3-b]pyrazine 59 and 10-bromo-acenaphtho[1,2-b]pyrido[2,3-e]pyrazine 61 donors were bonded to the corresponding DHPHAzSi acceptors through the Pd-catalyzed Buchwald-Hartwig amination in good yields (see Scheme 19).
Scheme 19
Buchwald-Hartwig amination of 7-bromo-2,3-diphenylpyrido[2,3-b]pyrazine 59 and 10-bromo-acenaphtho[1,2-b]pyrido[2,3-e]pyrazine 61 donors with DHPHAzSi acceptors.
The starting compounds 59 and 61 were prepared according to the literature procedures [47,48], through the condensation between 2,3-diamino-5-bromopyridine with benzyl and phenanthrene-9,10-dione, respectively.The photophysical properties of compounds 56–58, were investigated in a non-polar polymer matrix Zeonex®, and in small molecule hosts, 4,4′-bis(N-carbazolyl)-1,1′-biphenyl (CBP) and tris(4-(9H-carbazoyl-9-yl)phenyl)amine (TCTA) and are presented in Table 10.
Table 10
The photophysical properties of the compounds 56–58.
Compound
Host
λem[nm]
Φfl[%]
τPF[ns]
τDF[μs]
DF/PF
EA[eV]
S1[eV]
T1[eV]
ΔEST[eV]
56
Zeonex®
527
25
13.24 ± 1.18
9.45 ± 0.98
6.08
0.024
2.46
2.27
0.19
CBP
555
34
25.28 ± 1.06
1.06 ± 0.11
1.57
0.031
2.24
2.12
0.12
TCTA
555
26
32.29 ± 0.57
2.10 ± 0.44
1.20
0.026
2.25
2.07
0.19
57
Zeonex®
521
8
8.68 ± 0.09
0.7 ± 0.06
5.16
0.062
2.37
2.26
0.11
CPB
553
29
17.67 ± 0.18
2.7 ± 0.24
1.99
0.033
2.28
2.05
0.22
TCTA
551
14
26.81 ± 0.83
3.92 ± 0.32
1.14
0.037
2.26
2.05
0.21
58
Zeonex®
507
6
7.27 ± 0.32
9.90 ± 0.76
3.15
0.061
2.44
2.34
0.10
CPB
535
20
11.84 ± 0.42
10.9 ± 0.66
0.78
0.036
2.33
2.07
0.27
TCTA
529
10
32.45 ± 1.23
5.26 ± 0.71
1.17
0.034
2.34
2.09
0.25
λem—the maximum wavelength of photoluminescence spectra, Φfl—photoluminescence quantum yield in degassed, τPF—prompt fluorescence lifetime, τDF—delayed fluorescence lifetime, DF/PF—the ratio of delayed fluorescence to prompt fluorescence, EA—activation energy of the triplet to singlet transfer, error ± 0.01 eV, S1—singlet energy, error ± 0.03 eV, T1—triplet energy, error ± 0.03 eV, ΔEST—energy splitting, error ± 0.03 eV, Zeonex®—Cyclo Olefin Polymer is an engineered plastic that provides “glass-like” transparency, low protein absorption, high purity, low water absorption, and excellent moisture barrier. All parameters were estimated at 300 K.
Compounds 56–58 manifest emissions in two different time domains. The first component is the prompt fluorescence (PF) from the singlet excited state (S1), with a lifetime in the nanosecond time delay, and the second components are the delayed emissions from the high triplet excited state (T2) (as theoretical calculations revealed), decaying in micro to millisecond delay time.Georgescu et al. [49,50,51] studied the synthesis and fluorescence of 3-aryl-7-benzoyl-pyrrolo[1,2-c]pyrimidines in order to determinate the influence of the chemical structure and of solvent polarity on their optical properties.The authors used, for the synthesis of 3-biphenyl-pyrrolo[1,2-c]pyrimidines, a one-pot, three-component procedure [49,50], which involve a 1,3-dipolar cycloaddition reaction of a 4-biphenyl pyrimidinium-N-ylide with an activated alkyne 65 in 1,2-epoxybutane at reflux. The ylide is generated “in situ” from the corresponding pyrimidinium salts that was formed by the N-alkylation of the pyrimidine 63 with halogenoketone 64. The advantage of performing the reaction in a one-pot three-component approach is the direct formation of the final aromatic compounds 66a–j, avoiding the formation of dipyrimidino-pyrazinic inactivated products (see Scheme 20).
Scheme 20
One-pot, three-component synthesis of 3-biphenyl-pyrrolo[1,2-c]pyrimidines 66a–j.
The absorption and emission spectra of compounds 66a–j were recorded in acetonitrile:chloroform (1:1) (3.5 * 10−6 mol/L) solutions. The fluorescence quantum yield has been calculated (Table 11) for all compounds 66a–j using Equation (1) using quinine sulphate as standard.
Table 11
The main spectral features of the compounds 4a–j in acetonitrile:chloroform (1:1).
Compound
Absorption
Emission
Reference
λabs1[nm]
ε1[L/(mol cm)]
λabs2[nm]
ε2[L/(mol cm)]
λex1[nm]
λem1[nm]
λex2[nm]
λem2[nm]
Δν1[cm−1]
Δν2[cm−1]
Φfl[%]
66a
293
49,337
386
105,456
268
453
383
454
15,238
4083
4.64
[50]
66b
263
25,640
389
34,200
262
459
354
466
16,381
6789
6.42
[50]
66c
262
87,480
381
144,430
262
462
381
463
16,552
4648
19.02
[50]
66d
266
43,920
384
68,180
2658
462
389
466
15,668
4536
6.35
[50]
66e
270
18,880
399
20,706
270
457
400
462
15,155
3354
0.18
[50]
66f
290
38,272
383
68,795
290
435
380
446
11,494
3894
55.27
[50]
66g
268
34,200
398
44,780
262
451
360
463
15,994
6179
3.47
[50]
66h
262
65,250
380
77,820
263
430
380
460
14,767
4576
8.91
[50]
66i
292
39,784
380
34,836
264
455
380
464
15,900
4764
15.37
[50]
66j
260
40,740
381
44,950
329
478
358
472
9860
6740
11.85
[49]
λabs—the maximum wavelength of absorption, ε—the molar absorption coefficient, λex—excitation wavelength, λem—the maximum wavelength of photoluminescence, Φfl—photoluminescence quantum yield, Δν—Stokes shifts.
In order to calculate the quantum yield (Φfl), according to the Equation (1) we need to determine the maximum value of the absorbance at the emission wavelength λem2, (A), area of the emission peak (I), and refractive index (n) for the solution of investigated compound, and quantum yield (Φref), maximum value of the absorbance at the emission wavelength λem2 (Aref), area of the emission peak (Iref), and refractive index (nref) for the standard solution (quinine sulphate), respectively.Looking at the values from Table 11, it can be seen that two of the compounds (66c p-flouoro substituted and 66f 3,4-dimethoxy substituted) have higher values of quantum yield. These higher values of quantum yield can be explained by a more extended π electron conjugated system in the case of this compound. Ethyl 3-(4-biphenylyl)-7-(3,4-dimethoxybenzoyl)pyrrolo[1,2-c]pyrimidine-5-carboxylate was found to have the highest quantum yield value (55%). These higher quantum yield values suggest that the studied compounds are promising candidates for fluorescent chemical sensors.In view of future exploitation of pyrrolo[1,2-c]pyrimidine compounds in the field of bio-imaging investigations Georgescu et al. [51] synthesized a series of new pyrrolo[1,2-c]pyrimidine derivatives and studied their photophysical properties. The synthetic approach was similar with the one described above, but this time did not use the one pot strategy, but only by the 1,3-dipolar cycloaddition of the pyrimidinium ylides generated “in situ” from the corresponding pyrimidinium bromides 67 with the alkyne dipolarophiles 68 in 1,2-epoxybutane as reaction medium and acid scavenger (see Scheme 21).
Scheme 21
Synthesis of pyrrolo[1,2-c]pyrimidine 69a–j by 1,3-dipolar cycloaddition.
The photophysical properties of fused derivatives 69a–j were investigated by using different sorts of solvents (see Table 12). In chloroform, compounds derived from the ethyl propiolate, 69a–d, present better fluorescence yield than the compounds derived from the symmetric alkynes 69e–j. The excitation, during the recording of the emission spectra, was performed at λabs2 at which a higher intensity of the fluorescence was obtained. A main emission band is located in the blue region of the visible spectrum in 437–463 nm region.
Table 12
The spectroscopic features for absorption and fluorescence of 69a–j in chloroform solution (10−6 M).
Compound
R4
Absorption
Emission
λabs1[nm]
ε1[L/(mol cm)]
λabs2[nm]
ε2[L/(mol cm)]
λex[nm]
λem[nm]
Δν1[cm−1]
Δν2[cm−1]
Φfl[%]
69a
H
268
23,300
396
39,100
396
462
15,668
3608
51.77
69b
H
265
25,200
400
36,800
400
462
16,091
3355
38.26
69c
H
275
29,090
397
47,900
397
458
14,530
3355
61.35
69d
H
258
42,300
405
53,800
405
437
15,876
1808
42.40
69e
CO2Me
261
44,620
386
46,960
386
463
16,716
6786
11.04
69f
CO2Et
252
39,520
390
50,630
390
539
21,130
7088
2.64
69g
CO2Me
242
42,770
392
57,930
392
440
18,595
6957
6.63
69h
CO2Et
250
61,060
395
65,910
395
456
18,070
3387
2.99
69i
CO2Me
242
25,600
396
27,850
396
450
19,100
3030
27.46
69j
CO2Me
268
56,200
388
47,200
388
535
18,622
7116
3.24
λabs—the maximum wavelength of absorption, ε—the molar absorption coefficient, λex—excitation wavelenght, λem—the maximum wavelength of photoluminescence, Φfl—photoluminescence quantum yield calculated using quinine sulphate standard, Δν—Stokes shifts.
The authors [51] investigate the influence of all R1, R2, R3 and R4 substituents on the fluorescence properties of the synthesized compounds and concluded that a substituent that determine the growth of conjugation inside the pyrrolo[1,2-c]pyrimidine fragment lead to an increase of the fluorescence, while a substituent that determine the decrease of conjugation inside the pyrrolo[1,2-c]pyrimidine fragment lead to decrease of the fluorescence.Tomashenko et al. [52] obtained new pyrido[2,1-a]pyrrolo[3,2-c]isoquinoline 76a–c heterocyclic system by using Pd to catalyze the intramolecular cyclization of 1-[1-benzyl-2-(2-bromophenyl)-1H-pyrrol-3-yl]pyridin-1-ium bromides 74a–c (see Scheme 22).
Scheme 22
Pd catalyzed synthesis of pyrido[2,1-a]pyrrolo[3,2-c]isoquinolines 76a–c.
The obtained compounds 76a–c have fluorescent properties in solutions, with quantum yields for 76c in methanol reaching 81%. Photophysical data were studied in toluene, acetonitrile, dichloromethane (DCM) and methanol, respectively (Table 13). The obtained compounds display moderate to strong fluorescence in solution, giving minor variations in emission maxima position with changes in solvent polarity. The biggest effect was shown in methanol solutions and upon addition of proton donors to aprotic solvents.
Table 13
Photophysical properties of compounds 76a–c in toluene, acetonitrile, dichloromethane (DCM) and methanol solutions at room temperature, λex = 420 nm. Lifetimes (τ) were determined at λmax of the emission bands.
Nitrogen ylide chemistry is a traditional research area in our group, professors Zugravescu and Petrovanu being the pioneer of this field [53]. Several compounds with complex azaheterocyclic skeleton were synthesized through the N-ylides. Many of these compounds present practical importance either to their biological activities, having antimicrobial [40,41], anticancer [42,54,55,56,57,58], antitubercular [58,59,60,61] or anti-leishmaniasis [62] activity, or to their optical properties (some of this compound presenting intense blue fluorescence) [63,64,65,66,67,68,69]. Here we will present our recent (last 12 years) achievements in the synthesis of fluorescent azaheterocyclic compound.In one extensive work [63,64], we carried out a comprehensive investigation into the synthesis of fluorescent pyrrolodiazine (PD). All PD derivatives 78–82 were produced using a methodology which involve two steps. In the first stage, diazinium salts 78a–h were obtained by quaternization of diazine [pyridazine (PY) or phthalazine (PH)] with halogenated derivatives with increased reactivity. In the 2nd stage, a typical Huisgen [3+2] dipolar cycloaddition of diazinium ylides 78′ to the corresponding dipolarophiles were performed (see Scheme 23).
Scheme 23
Synthesis of fluorescent pyrrolodiazines 79–82 by 1,3-dipolar cycloaddition.
The synthesis of the desired pyrrolodiazine derivatives 79–82 was performed under conventional thermal heating (TH) and using MW irradiation, by a typical Huisgen [3+2] dipolar cycloaddition. The reactions under MW irradiation have shown some important advantages such as significantly higher yields, decreasing the reaction time from hours to 5 min and five times less amount of solvent is needed.To obtain a perspective on the effect that the C-7 substituent of the pyrrolodiazine skeleton the photoluminescent properties of the obtained compounds were measured in different solvents and are presented in Table 14.
Table 14
λmax (nm) of absorption spectra, fluorescence spectra, and relative quantum yields (%) of PD compounds 79–82.
Compound
Fluorescence (λmax, nm) (Quantum Yields (%))
Absorption (λmax, nm)
EtOH
CHCl3
Cyclohexane
EtOH
CHCl3
Cyclohexane
79a
431 (70)
430 (90)
430 (83)
343
351
355
79b
431 (70)
429 (90)
430 (83)
343
352
355
79c
429 (63)
431 (82)
434 (76)
356
362
366
79d
446 (1)
436 (8)
433 (11)
334
335
329
79e
448 (2)
439 (3)
434 (-)
334
334
329
79f
451 (1)
438 (7)
436 (10)
332
333
327
79g
487 (1)
471 (1)
insoluble
374
375
insoluble
79h
448 (4)
431 (5)
434 (8)
314
319
322
80a
430 (66)
423 (91)
416 (85)
349
357
361
80b
429 (66)
422 (91)
416 (85)
349
358
361
80c
436 (89)
437 (76)
insoluble
365
370
insoluble
80d
442 (1)
436 (5)
insoluble
333
335
insoluble
80e
430 (2)
436 (7)
insoluble
330
332
insoluble
80f
433 (1)
437 (4)
432 (8)
333
334
329
80g
446 (4)
430 (5)
432 (9)
315
319
322
80h
446 (4)
430 (4)
432 (8)
316
320
322
80i
448 (3)
432 (2)
insoluble
319
322
insoluble
81b
442 (2)
439 (2)
insoluble
326
321
insoluble
81c
427 (1)
439 (5)
insoluble
316
304
insoluble
82a
430 (9)
427 (18)
415 (40)
470
479
496
82b
430 (9)
427 (18)
415 (40)
470
479
496
82c
432 (3)
424 (4)
420 (4)
485
488
508
82d
433 (4)
424 (4)
419 (4)
484
488
508
While the partially saturated dihydro-pyrrolo-PY (82a–d) are red-shifted and have a poor or moderate quantum yield (around 5–40%), the tetrahydro-pyrrolodiazine (81b,c) have a negligible quantum yield (less than 5%). The fully aromatized pyrrolo-PY (79a–c and 80a–c) are highly powerful blue emitters with extremely high quantum yields (up to 90%). The highly blue emitters of completely aromatized pyrrolo-PH (79h and 80g–i) exhibit a low quantum yield of less than 10% and an unusual, blue-shifted absorption with λmax of absorption around 314–322 nm.Regarding the effect of the substituent from the 7th position of the pyrrolodiazine skeleton, the pyrrolo-PY compounds exhibit intense blue fluorescence and have a very high quantum yield when the substituent is an ester or amide group, whereas the quantum yield is negligibly low when the substituent is a ketone (see Scheme 24).
Scheme 24
Influence of the substituents on the fluorescence of the pyrrolo-PY compounds.
We confirmed the experimental results through theoretical calculations into another study from our group [65]. According to computational study, the first nπ* state may be significantly stabilized when the carbonyl group from the 7th position of the pyrrolo-PY moiety is oriented so that it faces the diazine nitrogen. Given the lower (fluorescent) ππ* state expected for all conformations, such an effect does not seem to affect the fluorescence of the ester derivative. On the other hand, we found that the same nπ* state is predicted to have a lower energy than the first ππ* state for the most stable conformation of the benzoyl-substituted derivative, which is consistent with the weak fluorescence that was experimentally seen.We demonstrate how the highly fluorescent ester-substituted pyrrolopyridazine’s solvent-dependent photophysical characteristics can be accurately predicted by TD-DFT in SS-PCM solvation when hybrid functionals such as B3LYP or PBE0 are used, together with a reasonable basis set.In order to increase the fluorescent properties of the pyrrolo-PY derivatives, we studied the influence of the substituent from phenyl ring on the 2nd position of pyrrolo-PY skeleton [66], and used the strategies adopted for construction of fluorescent pyrrolo-PY derivatives are similar to those presented in the previous study [64] (see Scheme 25).
Scheme 25
Synthesis of aryl substituted pyrrolopyridazines 86–87 by 1,3-dipolar cycloaddition.
The reactions under MW irradiation have shown some important advantages such as slightly higher yields and decreasing of the reaction time from 2 h to 5 min in liquid phase and 15 minutes in solid phase.For the obtained compounds 86 and 87, we investigated the photoluminescent properties (see Table 15).
Table 15
The spectroscopic features for absorption and fluorescence intensity of 86a–d and 87a–d in in acetonitrile solution (5 × 10−5 M).
Compound
λmax (nm) [ε (L mol−1 cm−1) × 103]
Fluorescence Intensity
Number of Absorption Maxima
I
II
III
IV
V
86a
356.00 [2.65]
347.00 [2.33]
277.00 [30.33]
264.00 [25.02]
225.00 [11.30]
6276.11
86b
357.00 [2.93]
337.00 [2.58]
280.00 [32.95]
263.00 [26.00]
226.00 [11.90]
6554.21
86c
355.00 [2.93]
341.00 [2.80]
284.00 [30.23]
265.00 [24.15]
228.00 [11.91]
7510.05
86d
356.00 [3.00]
340.00 [2.73]
284.00 [31.68]
264.00 [24.73]
227.00 [11.75]
8264.76
87a
344.00 [3.50]
340.00 [3.46]
276.00 [31.15]
264.00 [26.75]
226.00 [7.45]
5016.82
87b
350.00 [3.18]
335.00 [2.95]
276.00 [32.38]
264.00 [26.75]
226.00 [11.51]
5269.64
87c
350.00 [3.18]
335.00 [3.01]
282.00 [30.21]
265.00 [25.68]
227.00 [6.00]
6018.34
87d
350.00 [3.31]
334.00 [3.06]
276.00 [34.46]
264.00 [29.01]
228.00 [12.33]
6304.55
The pyrrolo-PY substituents had some effect on the absorbance and fluorescence properties. Thus, the cycloadducts with carboethoxy groups, in the seventh position have a more fluorescence than those with a carbomethoxy groups, in the same position and also the cycloadducts with a para-chlorophenyl substituent in the second position of pyrrolo-PY moiety have a more fluorescence than those para-bromophenyl substituted.Continuing our studies [67], we synthesized a new class of fused pyrrolodiazines 91–95 in order to obtain new fluorescent compounds by the same strategy-obtaining of the N-ylides fallowed by their cycloaddition with activated alkynes (see Scheme 26). The reactions were conducted both under conventional TH and MW irradiation. The reactions under MW irradiation have shown a series of advantages such as decreasing the reaction time from 6 hours to 10 minutes and slightly higher yields.
Scheme 26
Synthesis of fluorescent fused pyrrolodiazines 91–95 by 1,3-dipolar cycloaddition.
After the synthesis of the desired pyrrolodiazines, we investigated their photoluminescent properties in non-polar solvents cyclohexane and dichloromethane. The measured parameters are presented in Table 16.
Table 16
λmax (nm) of absorption spectra, λmax (nm) of emission spectra, and relative quantum yields (%) of compounds 91–95.
Compound
Fluorescence (λmax, nm) (Quantum Yields (%))
Absorption (λmax, nm)
Cyclohexane
Dichloromethane
Cyclohexane
Dichloromethane
91
426 (24)
432 (21)
360
358
92
422 (25)
426 (26)
356
354
93
428 (7)
441 (5)
327
325
94
439 (6)
446 (4)
324
322
95
491
-
374
372
λexe = 360 nm for samples 91 and 92; λexe = 320 nm for samples 93 and 94; λexe = 370 nm for sample 95.
A relationship between structure of cycloadducts and fluorescence quantum yields was founded. Thus, the compounds with pyrrolo-pyridazine skeleton showed good quantum yield (around 25%), while compounds with pyrrolophthalazine skeleton showed a lower quantum yield.In the next step we obtained some new bromoderivatives with increased reactivity by bromination of fluorescent pyrrolodiazines in heterogeneous catalysis in the presence of copper (II) bromide (see Scheme 27). These bromo-derivatives can fluorescently label biological macromolecules due to their increased reactivity, being easily incorporated in those bio-macromolecules.
Scheme 27
Derivatization of fluorescent pyrrolodiazines 91–94 by bromination.
Having in view the results of the previous studies, we prepared a new family of pyrrolobenzo[f]quinoline derivatives [68] in order to obtain blue fluorescent azaheterocyclic derivatives. The pyrrolobenzo[f]quinolines 102a–c, 103a–c and 104c were obtained by the same setup. In the first stage, benzo[f]quinolinium salts 100a–c were obtained by quaternization of benzo[f]quinoline with bromoketones. In the 2nd stage, a typical Huisgen [3+2] dipolar cycloaddition of benzo[f]quinolinium ylides 101a–c to the alkyne as dipolarophiles was performed (see Scheme 28). A comparative study of these reactions was carried out under conventional thermal heating and under ultrasound (US) irradiation. The reactions under US irradiation have shown a series of advantages such as decreasing the reaction time from 2 days to 2 hours and slightly higher yields.
Scheme 28
Synthesis of blue fluorescent azaheterocyclic derivatives 102–104 by Huisgen [3+2] dipolar cycloaddition.
The photophysical properties of azatetracyclic derivatives 102a–c, 103a–c and 104c were studied in cyclohexane and trichloromethane, respectively, and are presented in Table 17.
Table 17
λmax (nm) of absorption spectra and λmax (nm) of emission spectra of compounds 102a–c, 103a–c and 104c.
Compound
Fluorescence (λmax, nm)
Absorption (λmax, nm)
Cyclohexane
Trichloromethane
Cyclohexane
Trichloromethane
102a
434
439
399
403
102b
434
440
399
402
102c
440
445
384
386
103a
432
432
378
381
103b
432
433
376
375
103c
451
430
373
370
104c
450
449
374
369
λexc = 396 nm for samples 102a and 102b; λexc = 380 nm for sample 102c; λexc = 370 nm for samples 103a and 103b; λexc = 365 nm for samples 103c and 104c.
The obtained cycloadducts are blue emitters having λmax of fluorescence around 430–450 nm. The cycloadducts with similar structure 102a,b and 103a,b present small differences in their electronic spectra, while the cycloadducts with bulky pivaloyl group 102c and 103c or without keto group in the 3rd position 104c shows more intense fluorescence emission.As a continuation of this work, in another study [69] we derivatized the previously obtained cycloadducts 102a,b and 103a,b in order to use this blue fluorescent azaheterocyclic derivatives as fluorescent biomarkers. In the first step, we applied this functionalization to the tetracyclic cycloadduct products 102a,b and 103a,b by the bromination in heterogeneous catalysis obtaining a mixture of mono or dibrominated product type 105a–d and 106a–d (see Scheme 29). This bromo-derivatives can fluorescently label biological macromolecules (peptides, proteins, DNA) due to their increased reactivity, being easily incorporated in those bio-macromolecules.
Scheme 29
Derivatization of blue fluorescent azaheterocyclic derivatives 102–103.
In the next step, by a nucleophilic substitution, the monobrominated cycloadducts 105a–d were used as starting materials for the synthesis of corresponding azides 107a–d. The reaction was carried out in tetrabutylammonium bromide (TBAB) as phase transfer catalyst and in a chloroform/water mixture (see Scheme 29).For the new fluorophores (bromides 105a–d and azides 107a–d) we investigated optical properties on chloroform diluted solutions (see Table 18).
Table 18
λmax (nm) of absorption spectra, λmax (nm) of emission spectra and fluorescence quantum yield (%) of compounds 105a–d and 107a–d.
Compound
Fluorescence(λmax, nm)
Absorption(λmax, nm)
Quantum Yields(%)
105a
443
394
22.11
105b
431
391
18.64
105c
444
412
15.92
105d
433
393
17.09
107a
430
406
9.34
107b
435
387
7.17
107c
430
409
8.99
107d
445
393
5.30
λexc = 380 nm for sample 107b; λexc = 385 nm for samples 105a, 105b, 105d and 107d; λexc = 400 nm for samples 105c, 107a and 107c.
When comparing the fluorescence intensity of the bromides 105a–d to the fluorescence of the azides 107a–d, we observed a decrease in fluorescence, due the alteration of the planar structure of the molecule. The same effect is highlighted when comparing the fluorescence intensity of the underivatized cycloadducts 102a,b and 103a,b with the fluorescence intensity of the derivatized azatetracyclic bromides 105a–d or azides 107a–d.Another research field of interest to us, is of the compounds which contain a pyrrolo[2,1-a]isoquinoline or imidazo[2,1-a]isoquinoline framework, due to their potential biological activity, but also to their extended π-conjugated systems that make them excellent candidates for photophysical applications [70]. Thus, we synthesized several new pyrrolo [2,1-a]isoquinolines and imidazo[2,1-a]isoquinolines in order to realize a complete study regarding their photophysical properties and potential applications in the field.The chosen method for the assembly of fused target polyheterocycles relied on 1,3-dipolar cycloaddition of different isoquinolinium ylides 111a–c (in situ generated in basic medium from corresponding salts 110a–c, which were obtained by isoquinoline 108 alkylation with halides 109a–c) to ethyl propiolate or ethyl cyanoformate. The intermediate dihydropyrrolo[2,1-a]isoquinolines 112′a–c underwent oxidative dehydrogenation under atmospheric conditions, yielding the final compounds 112a–c in good yields (63–80%). Using ethyl cyanoformate as dipolarophile in similar conditions, we obtained imidazo[2,1-a]isoquinolines 113a–c presumably via dihydroderivatives 113′a–c (see Scheme 30).
Scheme 30
Synthesis of fused target polyheterocycles 112–113 by 1,3-dipolar cycloaddition.
The electronic absorption and emission spectra of the obtained azaheterocycles were recorded in dichlorometane (DCM) and dimethylsulphoxide (DMSO), and are presented in Table 19. The substituents on the 1st and 3rd positions of the pyrrole ring (COOMe, COOEt) have a low influence on the spectral pattern of pyrroloisoquinolines 112b and 112c. In addition, the solvent polarities have little to no influence on the electronic absorption spectra of pyrrolo- and imidazo-isoquinolines, suggesting that the ground state of these derivatives is not influenced by the solvent polarity. The extended π-π* conjugation in the imidazoisoquinolines system due to the substituents from the 1st and 3rd positions of the pyrrole ring induced a bathochromic shift of the absorption maxima. In DMSO, in the case of pyrroloisoquinolines, a hypsochromic shift of the absorption band occurs.
Table 19
Photophysical properties of isoquinoline derivatives.
Compound
Solvent
λabs[nm]
λem[nm]
Φfl[%]
τ1[ns]
τ2[ns]
112a
DCM
352, 335, 320, 275, 244
356, 374, 392, 415sh
28.37
DMSO
353, 336, 321, 276
359, 376, 395, 415sh
63.47
0.069
3.115
112b
DCM
358, 341, 325, 274, 246
363, 381, 401, 425sh
20.10
DMSO
358, 341, 325, 275
361, 382, 401, 425sh
53.95
0.866
3.095
112c
DCM
358, 341, 324, 274, 247
363, 381, 401, 425sh
31.28
DMSO
358, 341, 325sh, 275
364, 382, 400, 425sh
55.76
0.112
3.219
113a
DCM
338, 323, 309, 252
340, 356, 375, 395sh
41.04
DMSO
339, 324, 309
345, 361, 378
3.36
0.031
2.785
113b
DCM
338, 323, 309, 251
344, 360, 374, 400sh
18.37
DMSO
338, 324, 309
346, 360, 374
7.96
0.060
2.700
113c
DCM
338, 323, 309, 252
345, 359, 375, 400sh
29.41
DMSO
339, 323, 309
346, 359, 372
15.95
0.036
5.400
λabs—the maximum wavelength of absorption spectra, λem—the maximum wavelength of photoluminescence spectra, Φfl—photoluminescence quantum yield, τ—fluorescence lifetime, sh—shoulder.
In the case of the compound 112a containing CN group on the pyrrole ring, a similar behaviour of the emission spectra to absorption spectra was observed, namely a hypsochromic shift in both DCM and DMSO solvents, and no influence of the solvent polarity on the position of the emission maxima. The substituents on the pyrrole ring have no influence on the position of emission bands for derivatives 113a–c, excepting on the compound 113a which displays a hypsochromic shift in dichloromethane. The emission bands of imidazoisoquinolines 113a–c are hypsochromic shifted in DCM and DMSO comparing with the emission bands of pyrroloisoquinoline derivatives 112a–c. Time-correlated single photon counting (TCSPC) technique was used to determine the luminescence lifetimes. In DMSO, over the entire emission range, a double-exponential function describes better the emission decays for all investigated compounds. In DMSO, pyrroloisoquinolines 112a–c have longer fluorescence lifetime τ1 than those of imidazoisoquinolines 113a–c. The lifetimes of the excited-state for all compounds are in the nanosecond timescale.Indolizine derivatives with phenanthroline skeleton [71,72,73] were another research field in our group due to both their potential biological activities and their extended π-electron system which make them valuable materials in the construction of new optoelectronic devices. Compounds 114a–g and 115a–e were synthesized in our group using the same 3+2 dipolar cycloaddition strategy of cycloimmonium ylides to activated alkynes (see Scheme 31) [71]. In this case 4,7-phenanthrolin-4-ium and 1,7-phenanthrolin-7-ium ylides, generated from the corresponding monoquaternary 116 and 117 salts, were added to ethyl propiolate or dimethyl acetylene dicarboxylate DMAD.
Scheme 31
Synthesis of indolizine derivatives with phenanthroline skeleton 112,113 by 1,3-dipolar cycloaddition.
The absorption spectra of all the compounds present the fine structure specific to phenanthrene spectrum. The extended π-system of the 1,7-phenanthroline compounds explained the bathochromic shift to longer wavelength absorption band as compared to the UV-Vis absorption spectra of 4,7-phenanthroline derivatives. The position of the absorption and emission maxima of phenanthroline derivatives are highly influenced by the substituents on the pyrrole ring, as can be observed from Table 20. The introduction of CN, COOMe and COOEt groups in the 9th and 7th positions of the pyrrole ring determine a hypsochromic shift of the absorption and emission maxima of phenanthroline derivatives (114a, 114b, 115a). The same effect on the absorption and fluorescence spectra is obtained when a third substituent (COOMe) is introduced in the 8th position of the pyrrole ring, only in the case of the compound 114e.
Table 20
Photophysical characteristics of some phenanthroline derivatives.
The phenanthroline derivatives displayed broad and structureless emission band in 425 to 480 nm depending on the substituent nature at the pyrrole moiety. For 1,7-phenanthroline derivatives the emission band vas found in the 440–450 nm region, while for 4,7-phenanthrolines the emission band was found in 425–480 nm region. The position and the nature of the substituent at the pyrrole ring have a great influence on the fluorescence quantum yield of pyrrolo-phenanthroline derivatives. Scheme 32 illustrates the effect of substituents from the pyrrole ring on the fluorescence yield of pyrrolophenanthroline derivatives.
Scheme 32
The influence of substituents from the pyrrole ring on the fluorescence yield of pyrrolophenanthroline derivatives.
The fluorescence emission of disubstituted phenanthroline derivatives (114d, 115c, 115d) is practically quenched by the presence of halogens (Cl, Br) in the para position of phenacyl group (COC6H4) from 9th position of the pyrrole ring. The emission quantum yield decreases significantly (115e−0.044) when COC6H4OMe-(p) group is introduced in the 9th position of the pyrrole ring due to the withdrawing effect of the methoxy group which determines a decrease in conjugation in the 1,7-phenanthroline system. Time-correlated single photon counting method in dichloromethane was used for the fluorescence lifetimes (τ) estimation.The obtaining of small organic molecules capable to be incorporated in specific biomolecules or used in biomedical optical imaging was another research field in our group. A promising scaffold able to fulfil this purpose could be the bipyridyl. Bipyridyl, having two heterocyclic cores, can involve one or both of them in the formation of ylides and/or cycloaddition products. Thus, for these compounds we can obtain mono-salts [74], mono-ylides [74], mono-cycloadducts (indolizines) [74], mono-indolizine mono-salts [75,76,77], mono-indolizine mono-ylides [75,76,77], and theoretically bis-indolizines.In one of our studies [74] we report on the synthesis, fluorescence properties and a preliminary evaluation of pyridyl-indolizine containing anthracene moiety as a DNA binding agent. The conversion of the ethyl ester group from the 1st position of the indolizine into the corresponding propargyl-based indolizine derivative facilitate the addition of anthracenyl group through a “click” reaction. Fluorescent pyridyl-indolizine derivative 124 was synthesized in moderate yield in an adapted four step synthesis. In the first step a cycloaddition of 4,4′-dipyridinium ylide, generated from the corresponding monoquaternary 4,4′-dipyridinium phenacyl salt 118, with ethyl propiolate as activated alkyne gives an indolizine intermediate 119. Isolated indolizine 119 ester was hydrolysed into the corresponding carboxylic acid derivative 120 in the second step, then in the third step was reacted with propargyl amine to yield alkyne-substituted indolizine derivative 121, suitable for further “click” reactions. Separately, chloromethylanthracene 122 was straightforwardly transformed into corresponding azide 123. In the final step, alkyne indolizine 121 was reacted together with azide 123 in a “click” type reaction to yield the final substituted pyridyl-indolizine 124 (see Scheme 33).
Scheme 33
Synthesis of pyridyl-indolizine containing anthracene moiety as a DNA binding agent.
The emission properties of compounds 121 and 124 were investigated in DMF at different pH values using 1xTAE buffer solutions (40 mM Tris, 20 mM acetic acid and 1 mM EDTA), and are presented in Table 21. The excitation wavelength was 395 nm and the emission spectra were recorded in 425–700 nm domain.
Table 21
UV-vis and fluorescent properties of indolizines 121 and 124 in aqueous buffer at different pH.
Compound
pH
λex [nm]
λem [nm]
Stokes Shift [cm−1]
121
2.0
395
521
6123
5.0
539
6764
5.5
539
6764
6.0
539
6764
6.5
539
6764
7.0
539
6764
7.5
539
6764
8.0
539
6764
12.0
491, 526
4950, 6305
124
2.0
395
560
7459
5.0
486, 525
4740, 6269
5.5
480, 513
4483, 5823
6.0
480, 514
4483, 5861
6.5
480
4483
7.0
480
4483
7.5
481
4526
8.0
482
4570
12.0
482
4570
λex—excitation wavelength, λem—the maximum wavelength of photoluminescence, Stokes shifts—Δν = 1/λex − 1/λem.
The emission of precursor alkyne 121 at acidic pH value of 2.0 is 6-fold stronger than at pH values of 5.0–12.0, while the fluorescence intensity of compound 124 at pH = 12.0 is 7-fold greater than at pH = 5.0. In the case of the precursor alkyne 121, the emission spectrum presents a band with a shoulder at 495 nm at pH = 12.0 and a strong bathochromic shift of the emission maximum at pH values from 8.0 to 5.0, while the emission spectrum of compound 124 at pH = 5.0–12.0 presents bands with a shoulder at 475 nm. At pH = 12.0, the solution emits strongly in the green spectral window at 475 nm.Agarose gel electrophoresis analysis and spectroscopic investigations were performed in order to investigate the interaction of nucleic acids with pyridine-indolizines 121 and 124. Thus, deoxyribonucleic acid, low molecular weight from salmon sperm (sDNA) was used as a natural double-stranded DNA to test the binding properties of these compounds by agarose gel electrophoresis. The investigation shows that both investigated compounds 121 and 124 interact with sDNA.The interactions of compounds 121 and 124 with sDNA was examined also by UV-visible and fluorescence investigation. Absorption and emission spectra were recorded before the addition of sDNA, immediately after the addition of sDNA solution and after the incubation of the indolizine-sDNA mixture at room temperature for 24 h. The absorption spectrum of compound 121 changes only after 24 h by the decrease of the absorption band intensity. Contrarily the absorption spectrum of compound 124 showed instantaneous changes in the shape of the band, upon the addition of sDNA, the structured band yielded by anthracene suffering modifications and after 24 h transforming into a broad band with a slightly weaker intensity. Thus, the presence of the anthracene moiety in the structure of indolizine 124 facilitates easier interaction with nucleic acids due to its higher affinity for DNA when compared to the propargyl moiety of the indolizine 121. The same conclusion is obtained after the study of the fluorescence spectra of the mixtures: in case of compound 121, alteration of the initial shape or intensity of the emission band was only observed after addition of sDNA and 24 h of incubation, while for the compound 124 immediate increase in fluorescence intensity of the mixture was observed, followed by additional increase after 24 h.In order to investigate the ability of mono-indolizine mono-salts to interact with DNA, we used spectral methods UV-vis and fluorescence spectrometry [75]. Thus, a series of mono-indolizine mono-salts 125a–e were synthesized starting from the corresponding mono-indolizines 126 by alkylating with halogeno-ketones 127. The monoindolizines 126 were obtained by the cycloaddition of the corresponding ylides, generated in situ from the mono salts 128, with ethyl propiolate (see Scheme 34).
Scheme 34
Synthesis of mono-indolizine mono-salts 125a–e by alkylating with halogeno-ketones.
The absorption spectra of the mono-indolizine mono-salts were recorded in aqueous solution. The electron-donating methyl or methoxy group from the last inserted aromatic ring leads to a small bathochromic shift. DNA solution was progressively added to 125a and the spectra were recorded, in order to study the interaction of compound 125a with DNA. The hypsochromic shift of dye absorption maxima with the progressive addition of the DNA solution reflect the DNA binding to 125a. Moreover, in the UV region (350–360 nm) a hyperchromic effect was observed. This typical hyperchromic effect is caused by the damaging of the DNA double-helix structure due to the intercalation of 125a to DNA.The interaction of 125a with DNA was also investigated by emission spectra in acidic conditions since our investigated dyes display a lower solubility and instability in weakly basic condition. The fluorescence reached a maximum in pH range 1.8–3.6. The fluorescence intensities vary as follow: 125b > 125a > 125e or 125d > 125c, being relatively higher in pH range 2.5–4.5. At higher pH values the solubility of dyes was very low due to the ylide formation.Some preliminary investigation used herring sperm DNA (hsDNA) or control plasmid pUC19 in order to establish the interaction of the dyes with DNA. The fluorescence quenching of 125a upon addition of hsDNA shows that the dye 125a interact with DNA. The fluorescence of 125a-DNA system was investigated at different dye (125a) concentration and quenching extent has a maximum value at 6 μM concentration of dye. Supplementary investigation on the interaction mechanism for binding of 125a to hsDNA showed a similarly interaction way of 125a and ethidium bromide with hsDNA, compound 125a being binded in the minor groove of DNA.Since the solubility the compound 125a is poor, to increase its solubility and to extend its applications as cell staining agent or cell pH sensitive dye, we proposed the incorporation of compound 125a in β-cyclodextrin (β-CD) [76]. The reversible transformation of the pyridinium moiety in compound 125a to the corresponding nitrogen ylide 129a under proper pH condition (see Scheme 35), influence its fluorescence emission spectra, making it a pH sensible fluorescent dye.
Scheme 35
The reversible transformation of the pyridinium moiety in compound 125a to the corresponding nitrogen ylide 129a under proper pH condition.
The inclusion complex of indolizinyl-pyridinium salt in β-cyclodextrin (β-CD) was prepared by heating the equimolar amounts of components in water till 110 °C for 60 min, cooling down the solution under stirring for 6 h to reach the equilibrium followed by filtration through Phenex syringe filters (pore size: 0.45 μm).The ESI-MS experiments and molecular docking studies confirmed the formation of an inclusion complex between indolizine derivative and β-cyclodextrin in 1:1 and 1:2 ratios. The cytotoxicity of the inclusion complex was considerably reduced comparing with the cytotoxicity of free indolizine on both HeLa (human cervix adenocarcinoma) and NHDF (normal human dermal fibroblasts) cells.For the first time we demonstrated that the toxicity of a fluorescent dye was strongly reduced by the formation of cyclodextrin inclusion complex, allowing the successful application in cell staining. The study regarding cell membrane permeability showed that the nontoxic inclusion complexes mixture specifically accumulates in cell acidic organelles since could not pass through the cell plasma membrane.Recent, ref. [77] we prepared three new cyclodextrin encapsulated pH sensitive dyes and investigated their ability for self-aggregation and in vitro assessments as fluorescent cellular probes. The mono-indolizine mono-salts 130a–c (their structures are presented in Scheme 36) were synthesized in moderate yields in an adopted two step strategy based on our methodological background.
Scheme 36
The structure of the mono-indolizine mono-salts 130a–c.
Due to poor solubility in water of the indolizinyl-pyridinium salts 130a–c, these compounds were tested for the formation of inclusion complexes with β-CD. We started with an equivalent of each compound suspended in water, followed by the addition of an excess of β-CD (5 eq.) and heating to 90 °C until the reaction solution became transparent (after 25 min of heating). In case of 130c_CD the solutions remaining completely transparent after cooling down, while in case of 130a_CD and 130b_CD the formation of slightly cloudy solutions was observed. The excess up to 10 equivalents of the CD amount in the reaction mixture still did not change the appearance for the 130a_CD and 130b_CD at room temperature. These solutions were used in the subsequent analyses only after a microfiltration procedure.The ESI-MS experiments and molecular docking studies confirmed a 1:1 and 1:2 ratios between indolizine derivative and β-cyclodextrin in the inclusion complex.Absorption and emission spectra of indolizine derivatives 130a–c and their inclusion complexes 130a–c_CD were recorded at 1.0, 7.4, and 13.0 pH values. (1.0, 7.4, and 13.0) and the results compared. The indolizines 130a and 130b have similar absorption spectra, but slightly different than the absorption spectra of the indolizine 130c. At pH = 13.0, all the investigated indolizines have shown similar spectra. In the case of inclusion complexes 130a–c_CD, their absorption spectra at acidic and neutral pH values (1.0 and 7.4, respectively) are similar for all the investigated complexes, but different compared to the absorption spectra of the starting indolizines 130a–c. At basic pH values (pH = 13.0), the shape of the spectra of all complexes 130a–c_CD is drastically changed in comparison to each other and to the starting indolizines 130a–c.The excitation wavelength was 420 nm when fluorescence spectra of 130a–c and 130a–c_CD were measured at different pH values. Starting indolizines 130a–c exhibited similar emission spectra at acidic and neutral pH values, with an emission band around 550 nm. This band is approximately two times higher in intensity at acidic than neutral pH value. At basic pH values (pH = 13.0), the indolizines shown low to no fluorescence. The reversible transformation of pyridinium salts into analogous non-fluorescent ylides may explain this pH-dependent behaviour. The inclusion complexes 130a–c_CD demonstrated slightly different pH dependent behaviours, showing a similar low intensity at basic pH values, but different intensities at acidic pH values. The fluorescence intensities of the inclusion complexes 130a_CD and 130b_CD at acidic pH are only slightly higher than intensities at neutral pH values, while in the case of the inclusion complex 130c_CD, the fluorescence intensities at both the acidic and neutral pH were comparable. The formation of the inclusion complexes altered the planar structure of the indolizinyl-pyridinium salt molecules due to the specific rotation limitations induced by the steric hindrances with the CD, which determine a decrease of fluorescence intensity of the inclusion complexes at acidic pH values.Supplementary studies shown that the inclusion complexes have no cytotoxicity, they specifically accumulate within acidic organelles or mitochondria due to cellular permeability, and their intracellular fluorescence increase over a 24 hours period with outstanding signal stability.
3. Concluding Remarks
In conclusion, the present review article deals with design, synthesis, and photophysical properties of azaheterocycle-based materials. Several synthetic methodologies were used for the obtaining of fluorescent 5, 6 membered and fused azaheterocycles. The structure-fluorescence relationship of the obtained compound was investigated and allowed the authors to obtain compounds with better fluorescent properties in terms of emission wavelength, emission intensity and quantum yield.The presented approaches regarding the synthesis of fluorescent azaheterocycles, using varied methodologies, enable researchers to create a library of multifunctional derivatives, possessing high efficiency of fluorescence.The tunable emission properties of the azaheterocyclic compound make them valuable materials as potential luminophores in OLED devices, as luminescent solar concentrators or scintillators, as fluorometric (naked-eye chemosensor) molecular sensors for detection of metal ions, strong acids and bases with high selectivity, as thermally activated delayed fluorescence emitters and as fluorescent probe.
Authors: Qiyao Li; Ying Li; Tianliang Min; Junyi Gong; Lili Du; David Lee Phillips; Junkai Liu; Jacky W Y Lam; Herman H Y Sung; Ian D Williams; Ryan T K Kwok; Chun Loong Ho; Kai Li; Jianguo Wang; Ben Zhong Tang Journal: Angew Chem Int Ed Engl Date: 2019-10-22 Impact factor: 15.336
Authors: W Russ Algar; Melissa Massey; Kelly Rees; Rehan Higgins; Katherine D Krause; Ghinwa H Darwish; William J Peveler; Zhujun Xiao; Hsin-Yun Tsai; Rupsa Gupta; Kelsi Lix; Michael V Tran; Hyungki Kim Journal: Chem Rev Date: 2021-07-20 Impact factor: 60.622
Authors: Qiyao Li; Junyi Gong; Ying Li; Ruoyao Zhang; Haoran Wang; Jianquan Zhang; He Yan; Jacky W Y Lam; Herman H Y Sung; Ian D Williams; Ryan T K Kwok; Min-Hui Li; Jianguo Wang; Ben Zhong Tang Journal: Chem Sci Date: 2020-10-19 Impact factor: 9.825
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