Synthetic reactions driven by electron-donor–acceptor (EDA) complexes

The reversible, weak ground-state aggregate formed by dipole–dipole interactions between an electron donor and an electron acceptor is referred to as an electron-donor–acceptor (EDA) complex. Generally, upon light irradiation, the EDA complex turns into the excited state, causing an electron transfer to give radicals and to initiate subsequent reactions. Besides light as an external energy source, reactions involving the participation of EDA complexes are mild, obviating transition metal catalysts or photosensitizers in the majority of cases and are in line with the theme of green chemistry. This review discusses the synthetic reactions concerned with EDA complexes as well as the mechanisms that have been shown over the past five years.


Introduction
Electron transfer (ET) is a very common occurrence in the field of natural science, including photochemical, electrochemical, and enzymatic reactions and even major organic synthesis. From 1950 to 1952, Mulliken suggested an electron transfer hypothesis that could more precisely explain electron transfer phenomena based on the electron-donor-acceptor (EDA) complex [1][2][3]. Significantly, a broad absorption peak unrelated to the structure, called charge-transfer band, is typically located in the visible region of the UV-vis spectrum [4], which manifests the color variability of the mixed solution of the electron donor (D) and electron acceptor (A). The two components A and D may not absorb visible light, but the resulting EDA complex does [5]. If the EDA complex is irradiated with a particular wavelength (or heated to a corresponding temperature), the complex could be excited to the state [D, A]*, causing electron transfer and forming a pair of radical ions trapped in the solvent cage. The pair of radical ions escapes the solvent cage by diffusion to give radical ions, which could initiate chemical reactions or reverse electron transfer (Scheme 1) [6]. The continuously increasing demand for sustainable synthesis has encouraged chemists to pursue more efficient methods to manufacture fine and usable chemicals [7]. The reactions that EDA complexes participate in have been shown to be an enormous success, mainly due to the fact that they obviate photoredox catalysts or transition metal catalysts in the vast majority cases.
Moreover, in line with the theme of green chemistry, light is the sole external energy source in EDA complex pathways. Except for the pioneering research on EDA complexes in the 20th century, there was not much progress in the follow-up. Until the past few years, EDA-complex photochemistry has attracted more and more chemists and provided new opportunities for synthetic chemistry [8]. Moreover, diverse photocatalyst-free photochemical reactions have been employed to construct carbon-carbon and carbon-heteroatom bonds [9]. Among these methods, the product formations by aid of EDA complexes are the simplest and most rapid way. In this review, the focus lies on cyclization reactions, C-C-, C-S-, C-B-, C-N-, C-P-, C-O-, and C-H bond formation, primarily summarizing the chemical reaction step involving the EDA complex (Table 1) as well as the underlying mechanisms that have appeared over the last five years.   [58] Cyclization reactions In the pharmaceutical industry, retail drugs with a heterocyclic composition have exceeded 60% of the market volume. Hence, cyclization reaction innovation seems to be a requisite for pharmaceutical industry and human health. As an outstanding way, free-radical cascade reactions could efficiently construct various carbocycles and heterocycles with multifarious structures and complexity [59][60][61]. Centered on this context, we give a clear overview on a variety of novel cyclization reactions initiated by EDA complexes from the recent years. In 2016, Lakhdar and colleagues [10] obtained the target product 3 with LED (5 W) irradiation of a solution containing arylphosphine oxide 2, alkynes 1, eosin Y (EY, 4 mol %), N-ethoxy-2-methylpyridinium (4), and sodium bicarbonate in DMF (Scheme 2). As a distinct example of EDA complexes, the process efficiency depends on the association of eosin Y and oxidant 4 to a donor-acceptor EY-4 ground-system complex (high reactivity). Due to the ability of aryl groups to stabilize the formed alkenyl radical, this protocol could control regiose-lectivity efficiently with unsymmetrical alkynes. In addition, EPR spectroscopy shows that phosphono radicals could proceed throughout the reaction.
A halogen bond (XB) is a noncovalent interaction formed between a halogen atom and a neutral or negatively charged Lewis base. It is a kind of weak intermolecular interaction analogous to a hydrogen bond and basically can be considered as a specific EDA complex [62]. In 2016, Yu and colleagues [33] employed perfluoroalkyl iodide 6 as halogen-bond donor (electron acceptor) and the organic base dibenzylamine as the halogenbond acceptor (electron donor) to form the XB complex 8, and then a fluoroalkyl radical was given via visible-light-induced single-electron-transfer process. 1,2-Diisocyanato-4,5-xylene (5) was able to capture the fluoroalkyl radical, eventually providing the quinoxaline derivative 7 (Scheme 3).
In 2017, Fu and colleagues [20]  In 2017, Chen and colleagues [47] accomplished the cyclization through the EDA complex formed by N-tosyl-2-vinylaniline (19) and the Umemoto reagent 20 (CF 3 radical source) in CH 2 Cl 2 under blue LED irradiation. In the presence of base, 21 was produced with 98% yield after degassing. Along with straightforward posttreatment, the corresponding reduction product 22 can be afforded easily (Scheme 7). This procedure offers a novel cyclization method with bifunctionalization, causing a multicomponent reaction of vinylaniline, halide, and sulfonylate to give corresponding indole derivatives. Furthermore, a wide variety of applicable substrates and good functional-group tolerance are provided by this approach, yielding multiple indole analogues with biological activity. variety of perfluorinated chains were assembled with methylene compounds and guanidines or amidines, giving the corresponding perfluoroalkylated pyrimidines in good to excellent yield.
In 2017, Chen and colleagues [34] prepared the phenanthridine derivative 29 with CFL (25 W) irradiation of a solution containing 27, perfluoroalkyl iodide 28, amine additive N,N,N´,N´tetraethylethylenediamine (TEEDA) in THF (Scheme 9). TEEDA and perfluoroalkyl iodide form a halogen-bond adduct, and then light-induced electron transfer happens in order to give a perfluoroalkyl radical. The protocol can realize alkene-and alkyne iodide perfluoroalkylation and C-H perfluoroalkylation of electron-rich heteroaromatic hydrocarbons, providing a novel protocol for the synthesis of perfluoroalkyl-substituted phenanthridines.
Scheme 10: Synthesis of cis-tetrahydroquinoline derivative 32 initiated by an EDA complex.
In 2018, Sundén and Hsu [31] proposed a method of adding an α-aminoalkyl radical to maleimide via an EDA complex based on previous work (Scheme 10). The corresponding products can be given in good yield by modifying substituents on the N-alkyl moiety in 31 or N,N-dimethylaniline (30). This approach utilizes N,N-dimethylaniline (30) as electron donor and N-methylmaleimide (31) as electron acceptor to form an EDA complex, so that single-electron transfer occurs under ultraviolet-light irradiation. Subsequently, intermolecular proton transfer takes place, giving radicals 33 and 34. Radical 34 is quenched by oxygen, and radical 33 attacks 31 in order to form radical 35. Intermediate 36 is achieved by cyclization of radical 35, followed by hydrogen-atom removal, providing the cistetrahydroquinoline 32 (Scheme 11). It is worth noting that the EDA complex not only undergoes charge transfer but also proton transfer in this approach. The optimization experiment showed that the wavelength of the light source must overlap with the absorption spectrum of the EDA complex. Most impor-tantly, given that the best yield was achieved when the molar concentration of 30 was 7 times that of 31, the concentration of the EDA complex was essential for a high reaction rate.
In 2018, Yu and colleagues [22] discovered a method that employed O-aryloxime 37 and triethylamine as substrates at room temperature and blue-light irradiation to give phenanthridine 38 (also including quinoline products, Scheme 12). In this way, a nitrogen-centered radical was given via the EDA complex that was initiated by single-electron transfer, accomplishing the synthesis of a variety of highly functionalized nitrogen-containing aromatics with excellent yield. In 2019, Liang and colleagues [24] reported a method for preparing perfluoroalkyl-s-triazine via visible-light-promoted [5 + 1] cyclization initiated by an EDA complex. Perfluoroalkyl-striazine derivative 45 was synthesized by the reaction of biguanidine derivative 44 and perfluoroalkyl iodide 28 in the presence of sodium hydroxide (Scheme 15). Considering that oxygen played an indispensable role in the process, the authors supposed that it may facilitate single-electron transfer between biguanidine anion and perfluoroalkyl halide. By constructing two C-N bonds at the same time, the triazine heterocyclic structure that is commonly utilized in medical and material fields was accomplished by [5 + 1] cyclization. In 2020, Taylor and colleagues [26] proposed a reaction for the preparation of spirocyclic indoline derivative 47 from indolylynone 46 and thiophenol under blue-light irradiation (Scheme 16). An abundant range of products was given to test various indole-tethered ynones and thiols, confirming that the reaction is broad in scope. Remarkably, C-S bonds and spiro compounds have been constructed simultaneously in this approach, which are promising for drug synthesis. In 2020, Alemán and colleagues [53] proposed an approach in which ketene 48 and diene 49 condense with the help of diamine 51 to afford cyclobutane product 50 (Scheme 18 In 2020, Zhang and colleagues [25] developed a visible-lightinduced [3 + 2] cycloaddition reaction between glycine derivatives 57 and aryl epoxides 58, which can efficiently prepare a series of multisubstituted 1,3-oxazolidines 59 at room tempera- ture (Scheme 20). The strategy can be applied smoothly to an extensive range of glycine derivatives, including electron-donating or electron-withdrawing substituent groups in the paraor meta positions at the benzene rings, giving corresponding products in moderate yield. This protocol is also suitable for the structural diversity of epoxides, providing a new activation approach for C(sp 3 )-H-functionalization of glycine derivatives.
The construction of C-C bonds As a crucial element in the construction of various organic scaffolds, the formation of C-C bonds remains a hot topic in the field of synthetic organic chemistry. The conventional approaches of C-C-bond construction typically employ transitionmetal catalysts, such as in the Suzuki-Miyaura and Heck coupling reactions. Methodologies for forming different C-C bonds have recently been developed in the field of single-electron chemistry [63][64][65]. Considering that EDA-complex-initiated free-radical reactions are carried out under mild conditions, more attention has been paid to this efficient strategy for C-Cbond formation.
In 2015, Yu and colleagues [27] proposed a method for direct C-H trifluoromethylation of aromatic hydrocarbons through an EDA complex. Trifluoromethylated product 61 was synthesized by employing tryptamine derivative 60 and Umemoto reagent 20 as substrates as well as N-methylmorpholine (NMM) as organic base additive at room temperature (Scheme 21). The highly functionalized indole, pyrrole, benzofuran, and electronrich benzene containing CF 3 can be given in good yield. Given the redox potential of NMM and Umemoto reagent, directly conducting thermodynamic intermolecular SET is impossible. Thus, it is worth noting that the SET in this approach can be carried out only at room temperature without visible light.
In 2015, Melchiorre and colleagues [28] proposed a visiblelight-induced reaction to synthesize indole alkylation product 64 by exploiting the EDA complex formed by 3-methylindole (62) and 2,4-dinitrobenzyl bromide (63), with 2,6-dimethylpyridine as additive at room temperature (Scheme 22). The substrates with different substituents at position C2 and C3 of indole have been synthesized smoothly, including cis-fused pyrrolo-and furanoindolines. The X-ray single-crystal analysis showed that the EDA complex is received in the form of a faceto-face π-π complex, and the ratio of donor to acceptor is 1:1.
In the same year, based on previous experimental phenomena and data, Melchiorre and colleagues [45] designed a reaction, with indanone derivatives 65 and perfluorohexyl iodide (66) as substrates and a phase-transfer catalyst (PTC) to give perfluoroalkylation product 67 under white-light irradiation (Scheme 23). A variety of electron-withdrawing substituents on the aromatic ring of 65 were well tolerated; however, the presence of electron-donating substituents lowered the reactivity due to a negative impact on the EDA complex formation and led to a low yield. It is worth noting that the phase-transfer catalyst employed in this experiment is a suitable donor for the photosensitive EDA complex while at the same time providing effective asymmetric induction in the capture of the resulting radical along with enantioselectivity of the product.
In 2016, based on the experimental work in 2015 [27], Yu and colleagues [29] reported a type of EDA complex that could complete the hydrotrifluoromethylation of unactivated olefins and alkynes. This approach employed 68 and Togni reagent 69 (electron acceptor) as substrates, NMM as electron donor, and pyrrolidin-2-one as solvent to give hydrotrifluoromethylated product 70 at room temperature (Scheme 24). CF 3 was added to a variety of terminal alkenes, leading to corresponding hydrotrifluoromethylation products with moderate to good yield.
In 2017, Yu and colleagues [30] proposed an EDA-complex-induced alkyne trifluoromethylation reaction. The EDA complex formed by a catalytic quantity of Togni reagent 69 and NMM initiated the chain propagation, causing the final alkyne trifluoromethylation (Scheme 25). A variety of olefins, such as ene carbamates, styrene, aliphatic olefins, vinyl ethers, and acrylates are compatible in this approach, affording corresponding β-(trifluoromethyl)alkynes with good to excellent yield. The bifunctionalization was achieved by an EDA-complex-initiated three-component reaction in the absence of light, which is of great significance for the later study of temperature-driven EDA complexes.
In 2017, Konig and colleagues [42] discovered an EDA complex 75 formed by bromothiophene 72, aniline (73), and N,Ndiisopropylethylamine (DIPEA) as organic base additive to give corresponding thiophene radical 76 and aniline radical cation under irradiation with light. Then, 76 reacted with 73, giving rise to corresponding radical 77. Finally, product 74 was given via hydrogen atom transfer (Scheme 26). In contrast to (hetero)aryl halides with indispensable electron-withdrawing groups, the scope of the reaction comprises anilines including electron-withdrawing or electron-donating substituents in the arene, except N-acetylated or ortho-halogenated anilines.
In 2017, Chen and colleagues [21] reported a method that uptake of iodine. Finally, the dealkylation product 86 is given by removing iodide anion (Scheme 30). Various β-naphthols with different substituents in the 1-and 3-positions were tolerated, providing the corresponding products with excellent yield.
In 2018, Chen and colleagues [18] reported a method to realize C(sp 3 )-H allylation by generating aryl carboxyl radical from EDA complex based on previous work in 2017 [21]. The reaction is initiated by the formation of EDA complex between electron acceptor N-acyloxyphthalimide 90 and electron donor HE 79, completing regio-and chemoselective C(sp 3 )-H allylation or olefin bifunctionalization (Scheme 31).

Scheme 31: Synthesis of C(sp 3 )-H allylation product 91 initiated by an EDA complex.
In 2018, Tang and Studer [32] found a bifunctional group reaction of perfluoroalkylation and β-alkenylation by a perfluoroalkyl radical. Perfluoroalkylation product 93 was synthesized by utilizing (E)-3-methyl-1-phenylhept-1,6-dien-3-ol (92) and perfluorobutyl iodide (28) as substrates and potassium phosphate and DABCO as additives at 50 °C and under irradiation with light (Scheme 32). The reaction is compatible with phenyl substituents with high steric hindrance, indicating that steric effects of the aryl moiety in the migrating styrenyl group do not play a major role. In 2018, You and colleagues [19] reported the discovery of an EDA complex formed by indole derivative 94 and Umemoto reagent 20, which provided the trifluoromethyl-substituted spirocyclic indolene 95 with stereoisomeric center in good yield (up to 90%) under blue-light irradiation (Scheme 33). A variety of groups have been tolerated at the C2 position of indole, including phenyl groups with electron-donating or electron-withdrawing substituents, as well as the alkyl moiety. To further investigate the practicability of this approach, 95 was synthesized smoothly on the gram scale with a yield of 70%.
In 2019, Czekelius and colleagues [43] found that the perfluoroalkylation of unactivated olefins can be realized with phosphine catalyst and perfluorobutyl iodide (28) under visible-light irradiation. The EDA complex formed by perfluorobutyl iodide (28) and phosphine catalyst induced SET, affording a perfluoroalkyl radical, and then perfluoroalkylation product 97 was yielded by addition of perfluoroalkyl radical with olefin 96 (Scheme 34). Upon the termination of the reaction, the desired product can be given by removing the solvent and precipitating the catalyst. The comparison experiments and electronic absorption spectra showed that the efficiency of the catalyst was related to enhancement of selective absorption, considering the use of a visible-light source.
In 2019, Glorius and colleagues [11] proposed a method of employing an EDA complex formed by indole derivative 98 and the Katritzky salt 99 as well as morpholine as organic base to coupled electron transfer (PCET) with EDA complex 102 formed by morpholine and 99 (Scheme 36). As a rare example of EDA photochemistry, two kinds of EDA complexes were involved in this approach, explaining the reason why the yield increased significantly when morpholine was employed as an organic base additive, which was exploited in the screening stage of the reaction conditions.
In 2019, Xia and colleagues [46] reported that the EDA complex formed by aryl halide 106 and oxindole 107 under alkaline conditions allowed single-electron transfer under irradiation with light, eventually affording arylated oxidized indole product 108 (Scheme 37). This reaction provides an effective method to construct various 3-arylindoles with medicinal value at ambient temperature, which has a wide range of substrates, including various (hetero)aryl halides and substituted oxindoles.
In 2019, Gilmour and colleagues [12] transformed the classical Stetter reaction into a radical approach, solving the longstanding problem of chemical selectivity to convert α,β-unsaturated aldehydes selectively into 4-ketoaldehydes (Scheme 38). The imine salt (electron acceptor) that forms EDA complex 112 with electron donor α-keto acid 109 is synthesized by second- (Scheme 41). The reaction is compatible with various substrates, including alkenes, secondary alkylpyridinium ions, benzylic pyridinium ions, and primary alkylpyridinium ions, which can be considered an effective method for the generation of alkyl radicals without catalyst. In 2019, Yu and Zhang [15] reported a radical acylation reaction initiated by an EDA complex promoted by visible light. Imine 122 was employed as electron acceptor with α-keto acid 109 as electron donor to form the EDA complex, affording acylation product 123 under blue-light irradiation (Scheme 42). The quantum yield of the reaction was determined to be 0.08, suggesting that the reaction proceeded via radical coupling rather than a radical propagation. Moreover, the reaction was compatible with amides, cyanides, esters, ethers, halides, and heterocycles, and various α-aminoketones (32 examples) can be yielded in 90% isolated yield. According to the author, the EDA complex had a six-membered-ring transient state, and the imine also acted as an organic base (abstracting proton from α-keto acid), proving that electron transfer is accompanied by proton transfer in the process (Scheme 43).
In 2020, Stephenson and colleagues [14] employed 2-methoxynaphthalene (124) and acylated ethyl isonicotinate N-oxide obtained from 125 and trifluoroacetic acid anhydride to form EDA complexes for the preparation of trifluoromethylated product 126 (Scheme 44). As a rare example of EDA photochemistry in the catalytic system, only a catalytic equivalent of the electron donor was employed in this approach. Further experiments showed that the addition of inorganic salts, calcium chloride and lithium chloride, could increase the absorption of EDA complex in the visible-light region. In 2020, Xu and colleagues [39] proposed a visible-lightpromoted alkylation reaction using Katritzky salts such as 128 and glycine derivative 127 (or glycine segments in peptides) initiated by an EDA complex. This successfully realized the simple synthesis of unnatural α-amino acids 129 and precise alkylation modification of peptides in the later stage (Scheme 45). Even in the presence of other amino acid residues, this protocol has excellent regio-and chemoselectivity, providing a sequence of novel corresponding dipeptides with good yield. The construction of C-S bonds C-S bonds are commonly present in amino acids, proteins, glycosides, nucleic acids, and other biological macromolecules.
In recent years, photocatalyst-and transition-metal strategies have been employed to construct C-S bonds [66][67][68][69]. The C-S bond synthesis via EDA-complex pathways has the advantages of mild reaction conditions and a high tolerance to functional groups, which can be exploited for artificial syntheses of biological macromolecules.
In 2017, Miyake and colleagues [54] designed a type of C-S cross-coupling reaction initiated by an EDA complex promoted by visible light. In this approach, halogenated aromatic 130 was employed as electron acceptor with thiophenol (131) as electron donor to form an EDA complex. Light-promoted intermolecular electron transfer took place to give corresponding radicals, respectively, in the presence of base, and then cross-coupling between radicals was carried out, affording thioether derivative 132 (Scheme 46). It has been proved by UV-vis spectroscopy and TDDFT calculations that the EDA complex was formed between an electron-rich mercaptan anion and electrondeficient aryl halides. Most importantly, this approach can be successfully applied to the gram scale, providing a step towards assorted aryl sulfide structural units with medicinal value. In 2019, Yang and colleagues [52] developed a method for preparing S-aryl dithiocarbamates 135 by a multicomponent reaction of an EDA complex under visible-light irradiation (Scheme 47). A number of aryl halides reacted smoothly, providing moderate to good yields for analogous S-aryl dithiocarbamates. To further demonstrate the synthetic application of this protocol, a gram scale of 135 has been tested, giving a yield of 72%. By constructing C-N-and C-S bonds simultaneously in one step without any transition-metal catalyst, ligand, or photocatalyst, this method possesses a splendid application prospect. In 2019, Liao and colleagues [13] utilized Katritzky salt 139 and thiobenzoic acid (140) to form an EDA complex, providing thioether derivative 141 with DIPEA as an organic base additive (Scheme 49). This reaction offers a novel and simple approach for the synthesis of α-mercapto acid derivatives under mild reaction conditions and demonstrates strong compatibility to the functional group. In addition, a gram-scale reaction also gives the desired thioether product in a yield of 99%.

The construction of C-B bonds
The C-B bond can be converted into a wide range of other functional groups by the conversion of alkyl borane [70][71][72].
Hence, it has become imperative to pursue more efficient syntheses for constructing C-B bonds. In recent years, the construction of C-B bonds via EDA complexes has attracted more chemists' attention.
In 2017, Glorius and colleagues [51]  Finally, radical 146 undergoes decarboxylation to afford an aryl radical and then combines with radical cation 147, yielding product 144 (Scheme 50). It should be noted that only when NHPI is firstly activated can it turn into an electron acceptor, and thus further combines with the electron donor to form an EDA complex, mainly due to the fact that the electron acceptor in an excited state allows for stronger oxidation, to integrate with the electron donor.
In 2018, Glorius and colleagues [16] reported a method for the preparation of boron-substituted product 148 by employing Katritzky salt 119 as electron acceptor as well as the complex formed by bis(catecholato)diboron (B 2 cat 2 ) and solvent DMA as electron donor to afford an EDA complex (Scheme 51). This approach can effectively convert primary-, benzyl-, and secondary amines into corresponding borated products, with only a coordinating solvent, DMA. Furthermore, functionalization of natural products and drug molecules has been accomplished smoothly with excellent yields.
In 2018, Aggarwal and colleagues [17] proposed a method for preparing alkyl borate derivative 150 by employing Katritzky alkylpyridinium salt 149 and B 2 cat 2 as substrates as well as DMA as coordination solvent under blue-light irradiation, followed by subsequent reaction with pinacol to afford boration product 151 (Scheme 52). A number of secondary alkylamines, even those that have carbamate-or phthalimide-protected amines, have been efficiently transformed to suitable pinacol boronic esters. This simple operation without transition-metal catalysis will be widely promoted in the synthesis of important boron-containing molecules in medicine and biology.
In 2019, Aggarwal and colleagues [55] proposed that the EDA complex was formed by 2-iodophenyl thiocarbonate 152, bis(catecholato)diboron, and triethylamine, which afforded boronic acid ester derivative 153 under blue-light irradiation. Simultaneously, pinacol boronic acid ester derivative 154 can be yielded by subsequent processing (Scheme 53). The protocol reveals a high functional-group tolerance that permits the trans-formation into boronic esters of natural alcohol products with high stereocontrol.

The construction of C-N bonds
The development of efficient methods to construct C-N bonds is an essential scheme in organic synthesis due to its widespread presence in pharmaceutical-, agrochemical-, and materials sciences [73][74][75]. At present, most of the C-N-bonding reactions require transition-metal catalysis, and the reaction conditions are more stringent; however, the EDA-complex pathway proceeds under mild, catalyst-free conditions, promoted by irradiation with visible light.
In 2017, Shirke and Ramaastry [40] proposed an organic catalyzed β-azide reaction of ketene 155 initiated by the EDA complex formed by DABCO and Zhdankin reagent 156 (Scheme 54). A variety of β-azidoketones was conveniently ob- tained with good to excellent yield with electron-rich as well as electron-poor arenes and heteroarenes. Subsequently, in order to prove the practicability of this approach, 1,2,3-triazoles were assembled by reaction of 157 with alkynes.
In 2019, Bosque and Bach [41] reported that 3-acetoxyquinuclidine (q-OAc) could be utilized as an electron-donor catalyst to form an EDA complex with electron acceptor 158, and then a molecule of carbon dioxide was removed under 455 nm light irradiation, giving decarboxylation product 159 (Scheme 55). It was found that many ester groups can be activated by the structural motif of tetrachlorophthalimide in 158. Significantly, in contrast to most traditional EDA complex approaches that consume the DA pair, the electron-donor catalyst q-OAc in this method could be regenerated.
In 2019, Frontera and colleagues [49] obtained target product 162 with blue LEDs irradiation of a solution containing electron-poor N-aryloxyamides 160, indole derivative 161, and carbonate or other multicharge anions in CH 3 CN (Scheme 56). The corresponding products can be given in good yield by modifying substituents on the amide moiety in 160 or N-substituted indoles. Inorganic-base electron donors formed transient complexes with N-aryloxyamides, driven by noncovalent anion-π interactions, which has been described for the first time in a light-promoted process.

The construction of C-P bonds
Many compounds contain phosphorus, which has gained a high degree of interest in materials, agriculture, medical science, and biology [76]. Cases of C-P bond construction employing photoredox [77,78] or photoredox/nickel dual catalysis [79] have been identified in the field of photochemistry. However, here we introduce the methods initiated by EDA complexes for C-P bond construction.
In 2018, Lakhdar and colleagues [44] reported a visible-lightmediated synthesis approach of arylphosphonates initiated by an EDA complex. Diethyl phenylphosphonate (165) was given by exploiting diphenyliodonium trifluoromethanesulfonate (163) as electron acceptor, triethylphosphite (164) as electron donor, potassium carbonate as base, and CH 3 CN as solvent (Scheme 57). The complex is bound together by weak halogen bonds, in which phosphorus lone-pair electrons interact with σ* orbitals of C-I bonds. A variety of arylphosphonates can be directly afforded by the simple combination of diaryliodonium salts and phosphite esters. In addition, calculations including EPR, NMR, and DFT have been carried out to prove that the reaction mechanism is consistent with inference (Scheme 58).

The construction of C-O bonds and C-H bonds
Although there have been few cases of constructing C-O bonds and C-H bonds via EDA-complex pathways in recent years, we also summarized them in view of their great significance in organic synthesis.
In 2018, Miyake and colleagues [50] found a protocol for the preparation of (Z)-2-iodovinyl phenyl ether 168 by utilizing ethynylbenziodoxol(on)e (EBX) 167 and phenol derivative 166 (Scheme 59). Due to the lack of significant electronic effects of phenol, a variety of phenols, including electron-donor and electron-withdrawing groups, were been converted into corresponding 2-iodovinyl phenyl ethers in moderate to excellent yield with high regio-and stereoselectivities.
According to the analysis of the mechanism (Scheme 60), a molecule of phenol anion is first added to the alkyne group of an EBX, forming electron acceptor 169, which causes the destabilization of the C-I bond. Then, electron acceptor 169 forms an EDA complex with phenol anion, along with light-promoted electron transfer occurring. Thereby, the C-I bond and the I-O bond break to afford the final product (Z)-2-iodovinyl phenyl ether 168. The electron acceptor can only be provided by the addition of phenol to the EBXs since an EDA complex cannot be directly formed from the original substrates, which means that the effect of the two-component ratio of the EDA complex must be taken into account.
In 2019, Rathnayake and Weaver, III [37] designed a method of visible-light-promoted EDA-complex-mediated dehalogenation of haloalkanes 170. The dehalogenation product 171 was afforded based on the presence of the EDA complex formed by DIPEA and haloalkanes 170 under blue-light irradiation (Scheme 61). It was worth mentioning that longer reaction times and increased DIPEA loading were required owing to the inactivity of α-bromoketones, esters, and nonactivated sulfones; however, corresponding products could be given in high yield. When the DIPEA molarity was double that of haloalkanes, the highest yield was given. Since a marked yellow color appeared immediately upon mixing substrates, the existence of an EDA complex could be confirmed by UV-vis spectroscopy.
Scheme 61: Dehalogenation reaction initiated by an EDA complex.

Conclusion
In this review, reactions and mechanisms of EDA complexes were discussed from the aspects of cyclization reactions, C-C-, C-S-, C-B-, C-N-, C-P-, C-O-, and C-H bond formations. The absence of transitional-metal catalysts and photosensitizers is the most profound feature of EDA-complex-mediated reactions in most cases. On the other hand, the reaction conditions are mild, and light is utilized as the only external energy source, which is consistent with the theme of green chemistry. However, the comprehension of EDA complexes was established relatively late, mainly owing to the fact that the formation of EDA complexes was regarded as a unique chemical reaction rather than a branch of photochemistry; in addition, for the sake of avoiding BET processes, reactions involving EDA complexes require substrates with corresponding leaving groups, which also significantly limits the development of EDA complexes. In conclusion, although the research on EDA complexes is still in the initial stage, with many challenges to be solved in response, there is no doubt that the future of green chemical synthesis will surely have a very wide prospect for this strategy.