Monitoring intracellular pH fluctuation with an excited-state intramolecular proton transfer-based ratiometric fluorescent sensor

Intracellular pH is a key parameter related to various biological and pathological processes. In this study, a ratiometric pH fluorescent sensor ABTT was developed harnessing the amino-type excited-state intramolecular proton transfer (ESIPT) process. Relying on whether the ESIPT proceeds normally or not, ABTT exhibited the yellow fluorescence in acidic media, or cyan fluorescence in basic condition. According to the variation, ABTT behaved as a promising sensor which possessed fast and reversible response to pH change without interference from the biological substances, and exported a steady ratiometric signal (I₄₇₈/I₅₄₆). Moreover, due to the ESIPT effect, large Stokes shift and high quantum yield were also exhibited in ABTT. Furthermore, ABTT was applied for monitoring the pH changes in living cells and visualizing the pH fluctuations under oxidative stress successfully. These results elucidated great potential of ABTT in understanding pH-dependent physiological and pathological processes.     

Femtosecond dynamics of excited-state intramolecular proton transfer in o-tosylaminobenzoic and o-acetylaminobenzoic acids

The dynamics of excited-state intramolecular proton transfer (ESIPT) and of relaxation processes in o-tosylaminobenzoic acid (TAC) and o-acetylaminobenzoic acid (AAC) have been studied by femtosecond absorption spectroscopy with a time resolution of 30 fs. The ESIPT characteristic time in the TAC dimer and monomer and in AAC monomer is 50 fs. The excited product of photoinduced proton transfer in the monomer undergoes effective radiationless deactivation with a characteristic time of 30 ps, one of the channels of which is internal rotation followed by intersystem crossing and internal conversion. The product of ESIPT in the TAC dimer deactivates preferentially into the ground state via radiative transition with a time of 291 ps. ESIPT in the AAC dimer is thermodynamically unfavorable and occurs with a low yield.     

Opposite ESIPT characteristic of two AIE-active isomers with different linkage sites

In this work, we report two isomers composed of 1-phenyl-1H-phenanthro[9,10-d]imidazole (PI), hydroxyl and tetraphenylethylene (TPE), abbreviated as m-PITPE and p-PITPE. It is found that they exhibit similar aggregation-induced emission (AIE) behavior but totally different excited-state intramolecular proton transfer (ESIPT) characteristic, as a result of the different linkage sites of PI on TPE moiety. Theoretical calculations and their different experimental responses to F^? demonstrate that only the para-linkage isomer displays ESIPT. In m-PITPE with meta-linkage, the electron cloud distribution only locates at the TPE part in the singlet excited (S₁) states, which results in the localized excited state without ESIPT characteristic.     

An ESIPT-based NIR-fluorescent probe for exosome labeling and in situ imaging

Exosomes play significant roles in physiological and tumorigenic processes and it is desirable to visualize and track the exosomes. Herein, a novel amphiphilic fluorescent probe HBT-Exo based on excited-state intramolecular proton transfer (ESIPT) mechanism is reported for exosome-labeling. Its ESIPT characteristics were confirmed by both theory calculation and experimental observation, which enable the probe to show a large Stokes shift as well as near-infrared (NIR) keto-form emission. HBT-Exo displayed excellent biocompatibility and remarkable efficiency for exosome-labeling in gastric cancer cells. Furthermore, the labeled exosomes were successfully applied for the real-time in situ imaging in mouse models.     

Rational design of shortwave infrared (SWIR) fluorescence probe: Cooperation of ICT and ESIPT processes for sensing endogenous cysteine

Cysteine is well-known to be an important biothiol and related to many diseases. However, the in vivo detection of endogenous cysteine still suffers from lacking small-molecule fluorophores with both excitation and emission in the near-infrared (650-900 nm)/shortwave-infrared region. Herein, we report a molecular engineering strategy for shortwave infrared (SWIR, 900-1700 nm) sensing of cysteine, which integrated an excited-state intermolecular proton transfer (ESIPT) building block into the intramolecular charge transfer (ICT) scaffold. The obtained novel fluorophore SH-OH displays a maximum absorption at the NIR region, and emission at the SWIR region. We introduce the cysteine-recognition moiety to SH-OH structure, and demonstrate sensing of endogenous cysteine in living animals, using the SWIR emission as a reliable off-on fluorescence signal. This fluorophore design strategy of cooperation of ICT and ESIPT processes expands the in vivo sensing toolbox for accurate analysis in clinical applications.     

A turn on ESIPT probe for rapid and ratiometric fluorogenic detection of homocysteine and cysteine in water with live cell-imaging

5(Benzothiazol-2-yl)-4-hydroxyisophthalaldehyde (BHI), an intense ESIPT containing molecule in mixed media loses its properties due to resonance-assisted H-bond (RAHB) in absolute water. Due to resonance-assisted H-bond the o-aldehyde is more reactive than the other one. With addition of cysteine/homocysteine into this solution the o-aldehyde group gets transformed into thiazolidine/thiazine ring, respectively, and the phenolic proton becomes free enough for transfer to nitrogen of the benzothiazole ring in excited state, that is, the ESIPT of BHI is turned on. Thus we can detect cysteine/homocysteine in water as well as in live cells.     

Location of Solubilization of 2′-ethylhexyl Salicylate in Micelles

Absorption and excited state intramolecular proton transfer (ESIPT) fluorescence of 2′-ethylhexyl salicylate (EHS) were examined in the presence of cationic, non-ionic, and anionic surfactants. It was found that linear EHS molecule was solubilized in micelles with its flexible and hydrophobic 2′-ethylhexyl chain toward the micellar core and with its rigid salicyl moiety toward the micelle-water interface. The UV absorption of EHS was improved and the intramolecular hydrogen bonding formation of EHS was favored, resulting in greatly enhanced ESIPT fluorescence. The excited EHS molecules decay via visible luminescence and non-radiative deactivation. The binding sites of EHS in micelles were explained at a molecular level in terms of molecular structures and sizes of EHS and surfactants. Dynamic fluorescence quenching and spectral measurements of ester hydrolysis of EHS provide further evidences for the binding sites of EHS in different micelles.     

Ab initio study of the solvent H-bonding effect on ESIPT reaction and electronic transitions of 3-hydroxychromone derivatives

The electronic transitions occurring in 4-(N,N-dimethylamino)-3-hydroxyflavone (DMAF) and 2-furanyl-3-hydroxychromone (FHC) were investigated using the TDDFT method in aprotic and protic solvents. The solvent effect was incorporated into the calculations via the PCM formalism. The H-bonding between solute and protic solvent was taken into account by considering a molecular complex between these molecules. To examine the effect of the H-bond on the ESIPT reaction, the absorption and emission wavelengths as well as the energies of the different states that intervene during these electronic transitions were calculated in acetonitrile, ethanol and methanol. The calculated positions of the absorption and emission wavelengths in various solvents were in excellent agreement with the experimental spectra, validating our approach. We found that in DMAF, the hydrogen bonding with protic solvents makes the ESIPT reaction energetically unfavourable, which explains the absence of the ESIPT tautomer emission in protic solvents. In contrast, the excited tautomer state of FHC remains energetically favourable in both aprotic and protic solvents. Comparing our calculations with the previously reported time-resolved fluorescence data, the ESIPT reaction of DMAF in aprotic solvents is reversible because the emitting states are energetically close, whereas in FHC, ESIPT is irreversible because the tautomer state is below the corresponding normal state. Therefore, the ESIPT reaction in DMAF is controlled by the relative energies of the excited states (thermodynamic control), while in FHC the ESIPT is controlled probably by the energetic barrier (kinetic control).     

Effects of electronic delocalization on intramolecular proton transfer

The effects of molecular size, conjugation length, and competition with excimer formation on excited state intramolecular proton transfer (ESIPT) in conjugated polymers, in which the intramolecularly hydrogen-bonded moieties reside in the main chain, were examined. A large extent of π-electron delocalization is found to inhibit the ESIPT process. Excimer formation is found to be competitive with ESIPT in the polymers studied, whereas molecular size does not inhibit ESIPT.     

Unraveling solvent-dependent hydrogen bonding interaction and excited-state intramolecular proton transfer behavior for 2-(benzo[d]thiazol-2-yl)-4-(9H-carbazol-9-yl)phenol: A theoretical study

Organic chemosensors with excited-state intramolecular proton transfer (ESIPT) behavior have attracted much attention because it has great potential in a wide range of applications. Considering the paramount behavior of excited-state relaxation, in this work, we mainly focus on deciphering photo-induced hydrogen bonding effects and ESIPT mechanism for the novel 2-(benzo[d]thiazol-2-yl)-4-(9H-carbazol-9-yl)phenol (mCzOH) dye. Considering the effects of different solvents on excited-state dynamics of mCzOH flurophore, we adopt four solvents with different polarities. Analyses of fundamental structural changes, infrared (IR) vibrational spectra, and core valence partition index between S₀ and S₁ state, we confirm hydrogen bond O H···N of mCzOH should be enhanced via photoexcitation. Especially, the increase of solvent polarity could promote hydrogen bonding strengthening degree. Intramolecular charge transfer (ICT) resulting from photoexcitation qualitatively facilitates the ESIPT occurrence to a large extent. For further checking and probing into ESIPT mechanism, via constructing potential energy curves (PECs) in four solvents, we clarify the ESIPT behavior for mCzOH. Most worthy of mention is that polar solvent plays critical roles in lowering potential barrier of ESIPT reaction and in facilitating ESIPT process. We not only clarify the detailed excited-state process, but also present the solvent-polarity-dependent ESIPT mechanism for mCzOH fluorophore.     

Excited-State Intramolecular Proton Transfer: A Short Introductory Review

In this short review, we attempt to unfold various aspects of excited-state intramolecular proton transfer (ESIPT) from the studies that are available up to date. Since Weller’s discovery of ESIPT in salicylic acid (SA) and its derivative methyl salicylate (MS), numerous studies have emerged on the topic and it has become an attractive field of research because of its manifold applications. Here, we discuss some critical aspects of ESIPT and tautomerization from the mechanistic viewpoint. We address excitation wavelength dependence, anti-Kasha ESIPT, fast and slow ESIPT, reversibility and irreversibility of ESIPT, hydrogen bonding and geometrical factors, excited-state double proton transfer (ESDPT), concerted and stepwise ESDPT.     

Different ESIPT Mechanisms for Angular‐Shaped Quinacridone in Toluene and Dimethyl Formamide (DMF) Solvents: A Theoretical Study

Adopting density functional theory (DFT) and time‐dependent density functional theory (TDDFT) methods, we investigat and present two different excited‐state intramolecular proton transfer (ESIPT) mechanisms of angular‐quinacridone (a‐QD) in both toluene and DMF,theoretically. Comparing the primary structural variations of a‐QD involved in the intramolecular hydrogen bond, we conclude that N1–H2⋯O3 should be strengthened in the S₁ state, which may facilitate the ESIPT process. Particularly, in toluene, the S₁‐state‐stable a‐QD enol* could not be located because of the non‐barrier ESIPT process. Concomitantly, infrared vibrational spectral analysis further verified the stability of the hydrogen bond. In addition, the role of charge–transfer interaction has been addressed under the frontier molecular orbitals (MOs), which depicts the nature of the electronic excited state and supports the ESIPT reaction. The potential energy curves according to variational N1–H2 coordinate demonstrates that the proton transfer process should occur spontaneously in toluene; however, in DMF, a low potential energy barrier of 0.493 kcal/mol is needed to complete the ESIPT reaction. Although this barrier of 0.493 kcal/mol is too low to make an important impact on the ESIPT reaction, just because of the existence of barrier, ESIPT mechanisms in toluene and DMF are different.     

Fluorescent sensing of anions based on excited state intramolecular proton transfer in <Emphasis Type="Italic">N</Emphasis>-(3-hydroxy-2-naphthamido)-<Emphasis Type="Italic">N</Emphasis>′-phenylthiourea

A neutral N-amidothiourea-based excited state intramolecular proton transfer (ESIPT) anion receptor bearing an o-hydroxynaphthamide fluorophore and a thiourea binding site, N-(3-hydroxy-2-naphthamide)-N′-phenylthiourea (1a), was designed and synthesized. Fluorescence and absorption response of 1a toward anions were assessed in acetonitrile. IR and NMR experiments indicated that the “OH⋯O=C” intramolecular hydrogen bond (IHB) in 1a was weak so that it only exhibited the short-wavelength normal emission other than ESIPT fluorescence. Due to the high anion binding affinity of the N-amidothiourea binding site and the formation of a hydrogen binding network in the 1a-anion complex, 1a underwent structural change upon anion binding that strengthens the “OH⋯O=C” IHB, leading to the ESIPT and the observation of the long-wavelength ESIPT emission whereas the normal fluorescence is quenched. On the basis of NMR and fluorescence titrations and control experiments with model compounds, a sensing mechanism of the anion-binding-induced ESIPT was proposed. Supported by the National Natural Science Foundation of China (Grant Nos. 20425518, 20675069 & 20835005) and the National Fund for Fostering Talents of Basic Science (Grant No. J0630429)     

Influence of the Intramolecular Hydrogen Bond on the Fluorescence of 2-ortho-Aminophenyl Pyridines

The dynamic nature of excited-state intramolecular proton transfer (ESIPT) and its effect on emission spectra is an attractive strategy to create multi-emissive dyes. Here we describe the behavior of a series of hydrogen-bonded triphenylpyridines with a set of donor–acceptor combinations that allowed us to perceive the influence of each substitution on the photophysical properties of the dyes. The susceptibility of these ESIPT moieties to pH variations was also studied, elucidating that the level of protonation had a significant effect on the emission color. The assignment of each emission band was made by using DFT and td-DFT calculations that were in agreement with the experimental results. This study emphasizes the versatility of triphenylpyridines that can be synthesized effortlessly with a logical and independent C-2, C-4 and C-6 substitution in order to have the desired ESIPT modulation and subsequent multi-emission response.     

Total Syntheses of the Isomeric Aglain Natural Products Foveoglin A and Perviridisin B: Selective Excited‐State Intramolecular Proton‐Transfer Photocycloaddition

Selective excited‐state intramolecular proton‐transfer (ESIPT) photocycloaddition of 3‐hydroxyflavones with trans , trans ‐1,4‐diphenyl‐1,3‐butadiene is described. Using this methodology, total syntheses of the natural products (±)‐foveoglin A and (±)‐perviridisin B were accomplished. Enantioselective ESIPT photocycloaddition using TADDOLs as chiral hydrogen‐bonding additives provided access to (+)‐foveoglin A. Mechanistic studies have revealed the possibility for a photoinduced electron‐transfer (PET) pathway.     

Substituent Modulation from ESIPT to ICT Emission in Benzoimidazolphenyl-methanones Derivatives: Synthesis,Photophysical and DFT Study

Design and synthesis of five new derivatives of benzophenone based imidazole dyes is presented. Synthesized dyes were well characterized by ¹H NMR, ¹³C NMR, FT-IR and mass analysis. Dyes contain a secondary acceptor, ESIPT core and different donors forming (D-ESIPT core-A) as basic skeleton in order to study both ESIPT and ICT systematically in this same class of dyes. Dyes without a donor substituent showed ESIPT emission while dyes with a substituted strong donor showed intramolecular charge transfer (ICT) emission. Moreover emission properties of methoxy analogue dyes has been studied to further confirm non-ESIPT emission in dyes without donors and ICT emission in strong donor substituted dyes. All dyes exhibited long range emissions from 392 to 567 nm. Dyes exhibiting ESIPT emission showed negative solvatochromism while ICT emission exhibiting dyes shows positive solvatochromism. ICT and ESIPT characteristics are well correlated with polarity functions plots and Mulliken–Hush analysis. Experimental observations are well supported by TD–DFT and computed energies. The electrophilicity index has been calculated to get details of the stabilities of possible tautomers.     

Excited state intramolecular proton transfer in 5-hydroxy flavone: A DFT study

Potential energy surfaces (PES) for the ground and excited state intramolecular proton transfer (ESIPT) processes in 5-hydroxy-flavone (5HF) were studied using DFT-B3LYP/6-31G(d) and TD-DFT/6-31G(d) level of theory, respectively. Our calculations suggest the non-viability of ground state intramolecular proton transfer (GSIPT) in 5HF. Excited states PES calculations support the existence of ESIPT process in 5HF. ESIPT in 5HF has been explained in terms of HOMO, LUMO electron density of the enol and keto tautomer of 5HF. PES scan by phenyl group rotation suggests that the twisted form, i.e., phenyl group rotated by 18.7° out of benzo-γ-pyrone ring plane is the most stable conformer of 5HF.     

The investigation of proton transfer and fluorescence‐sensing mechanisms of [2‐(2‐hydroxy‐phenyl)‐1H‐benzoimidazol‐5‐yl]‐phenyl‐methanone

Given the tremendous potential of fluorescence sensors in recent years, in this present work, we theoretically explore a novel fluorescence chemosensor [2‐(2‐Hydroxy‐phenyl)‐1H‐benzoimidazol‐5‐yl]‐phenyl‐methanone (HBPM) about its excited state behaviors and probe‐response mechanism. Using density functional theory (DFT) and time‐dependent density functional theory (TDDFT) methods, we explore the S₀‐state and S₁‐state hydrogen bond dynamical behaviors and confirm that the strengthening intramolecular hydrogen bond in the S₁ state may promote the excited state intramolecular proton transfer (ESIPT) reaction. In view of the photoexcitation process, we find that the charge redistribution around the hydroxyl moiety plays important roles in providing driving force for ESIPT. And the constructed potential energy curves further verify that the ESIPT process of HBPM should be ultrafast. That is the reason why the normal HBPM fluorescence cannot be detected in previous experiment. Furthermore, with the addition of fluoride anions, the exothermal deprotonation process occurs spontaneously along with the intermolecular hydrogen bond O–H?F. It reveals the uniqueness of detecting fluoride anions using HBPM molecules. As a whole, the fluoride anions inhibit the initial ESIPT process of HBPM, which results in different fluorescence behaviors. This work presents the clear ESIPT process and fluoride anion‐sensing mechanism of a novel HBPM chemosensor.