New Trends in Diaziridine Formation and Transformation (a Review)

This review focuses on diaziridine, a high strained three-membered heterocycle with two nitrogen atoms that plays an important role as one of the most important precursors of diazirine photoaffinity probes, as well as their formation and transformation. Recent research trends can be grouped into three categories, based on whether they have examined non-substituted, N-monosubstituted, or N,N-disubstituted diaziridines. The discussion expands on the conventional methods for recent applications, the current spread of studies, and the unconventional synthesis approaches arising over the last decade of publications.


Introduction
An important intermediate and precursor in organic chemistry, diaziridine [1] is a highly strained three-membered heterocycle with two nitrogen atoms [2]. The other excellent properties of diaziridine include a weak N-N bond, low toxicity, hydrazine aminal duality [3], and neurotropic activity [4]. Diaziridines, independently discovered by three research groups (Schmitz's, Paulsen's, and Abendroth and Henrich's research groups) between 1958 and 1959, progressively achieved popularity in the field of chemistry over the two decades following these first publications [5]. Non-substituted diaziridine (diaziridine without any substituent on the nitrogen atom, 1) was developed as a reagent for a variety of oxidative transformations [6] and employed in the synthesis of carbene-mediated photoaffinity-labeled photophores of 3H-diazirines [7][8][9][10]. The trend of using diaziridine 1 as a precursor for the diazirine photoaffinity probe has been progressively updated until the present day, and a series of reviews have discussed it since the 2010s [7,[11][12][13][14][15]. Although the chemistry of N-monosubstituted diaziridine 2 has not been studied as extensively as that of non-substituted diaziridine 1, there are examples documenting its application as an N-transfer reagent with α,β-unsaturated amides to form stereopure aziridines [16]. As for N,N-disubstituted diaziridine 3, these valuable heterocycles have also been used as a versatile reagent via selective C-N or N-N cleavage in organic synthesis, particularly their bicyclic analogues of 1,5-diazabicyclo[3.1.0]-hexanes, which possess a strained cis-N,Ndisubstituted diaziridine fragment for 1,3-dipolar cycloaddition [17]. The advancements in substituted diaziridine with respect to its nitrogen atom(s) synthesis and applications have been summarized in several reviews [3][4][5][18][19][20]. On the basis of these excellent reviews, only a few studies have been fully dedicated to investigating the potential properties diaziridine with respect to its monocyclic synthetic methods [20] or its reactivity

The Chemistry of Diaziridines
Three key approaches are known for the construction of monocyclic diaziridines 4, and these were summarized by Makhova et al. in their previous 2008 review of diaziridine ( Figure 2) [20]. First, the reaction of primary aliphatic amines or ammonia 5 with the condensation products of carbonyl compounds 6 and aminating reagents. Second, the reaction of imines 7 (the condensation product of carbonyl compounds and primary aliphatic amines) is conducted with aminating reagent 8. Last, a three-component condensation reaction involving the carbonyl compound 9, primary aliphatic amines or ammonia 10, and aminating reagents (hydroxylamine-O-sulfonic acid (HOSA) or halo(alkyl)amine, 11). In addition, in their summary, Meijler et al. [7] emphasized that diaziridine synthesis as a precursor of 3-aryl-3-trifluoromethyl-3H-diazirine can start from the preparation of corresponding α,α,α-trifluoroacetophenone via oximation and tosylation (or mesylation)the condensation products of carbonyl compounds 6-followed by the treatment of ammonia. In consequence, these known approaches can be described as the "conventional" synthesis methods that have generally been used for the synthesis of diaziridine up until the most recent past. The reactivity of diaziridine was then pursued in order to broaden the advanced applications of these three-membered heterocycles, with reactions that can take place with or without any ring cleavage [1], or the transformation of its unprotected form into respective diazirines through oxidation. Diaziridine transformation induced by electrophilic reagents started being studied in the early 1950s and these reactions are primarily associated with the steric strain of the diaziridine ring and the presence of its two nitrogen atoms [5].

The Chemistry of Diaziridines
Three key approaches are known for the construction of monocyclic diaziridines 4, and these were summarized by Makhova et al. in their previous 2008 review of diaziridine ( Figure 2) [20]. First, the reaction of primary aliphatic amines or ammonia 5 with the condensation products of carbonyl compounds 6 and aminating reagents. Second, the reaction of imines 7 (the condensation product of carbonyl compounds and primary aliphatic amines) is conducted with aminating reagent 8. Last, a three-component condensation reaction involving the carbonyl compound 9, primary aliphatic amines or ammonia 10, and aminating reagents (hydroxylamine-O-sulfonic acid (HOSA) or halo(alkyl)amine, 11). In addition, in their summary, Meijler et al. [7] emphasized that diaziridine synthesis as a precursor of 3-aryl-3-trifluoromethyl-3H-diazirine can start from the preparation of corresponding α,α,α-trifluoroacetophenone via oximation and tosylation (or mesylation)-the condensation products of carbonyl compounds 6-followed by the treatment of ammonia. In consequence, these known approaches can be described as the "conventional" synthesis methods that have generally been used for the synthesis of diaziridine up until the most recent past. The reactivity of diaziridine was then pursued in order to broaden the advanced applications of these three-membered heterocycles, with reactions that can take place with or without any ring cleavage [1], or the transformation of its unprotected form into respective diazirines through oxidation. Diaziridine transformation induced by electrophilic reagents started being studied in the early 1950s and these reactions are primarily associated with the steric strain of the diaziridine ring and the presence of its two nitrogen atoms [5]. The rapid improvement in the quality of analysis instrumentation for experimental structure identification and detailed stereocenter has lead to the intensive study of the detailed structure determination of diaziridine. Experimental data regarding the structures of diaziridines are important for achieving deeper insight into the previously elucidated features of the diaziridine ring structure, in particular, for the comparison of its corresponding N-N or C-N bond length [21]. Recently, experimental data were obtained The rapid improvement in the quality of analysis instrumentation for experimental structure identification and detailed stereocenter has lead to the intensive study of the detailed structure determination of diaziridine. Experimental data regarding the structures of diaziridines are important for achieving deeper insight into the previously elucidated features of the diaziridine ring structure, in particular, for the comparison of its corresponding N-N or C-N bond length [21]. Recently, experimental data were obtained for the structural determination of N,N-disubstituted diaziridine [22] and its trisubstituted form, which possesses an additional alkyl group at position 3 [23,24], bis-diaziridine [25], and bicyclic diaziridine [26] derivatives by the method of gas electron diffraction. Most diaziridine derivatives are liquids; thus, the recent experimental determination of its structures on the basis of X-ray diffraction studies [21,27] has only been performed in a few cases. Investigation of conformational and configurational changes in order to understand the effect of the interconversion barrier on the steric hindrance of the diaziridine substituent has also been conducted using dynamic gas chromatography [28][29][30]. The identification of equilibrium (molecular) structures using joint analysis of gas phase electron diffraction, quantum chemistry, and spectroscopic data [25,26] is becoming a trend and has made diaziridine stereochemical study more visible. Table 1 summarizes the details of recent experimental structure identification studies of several diaziridine derivatives.  The rapid improvement in the quality of analysis instrumentation for experimental structure identification and detailed stereocenter has lead to the intensive study of the detailed structure determination of diaziridine. Experimental data regarding the structures of diaziridines are important for achieving deeper insight into the previously elucidated features of the diaziridine ring structure, in particular, for the comparison of its corresponding N-N or C-N bond length [21]. Recently, experimental data were obtained for the structural determination of N,N-disubstituted diaziridine [22] and its trisubstituted form, which possesses an additional alkyl group at position 3 [23,24], bis-diaziridine [25], and bicyclic diaziridine [26] derivatives by the method of gas electron diffraction. Most diaziridine derivatives are liquids; thus, the recent experimental determination of its structures on the basis of X-ray diffraction studies [21,27] has only been performed in a few cases. Investigation of conformational and configurational changes in order to understand the effect of the interconversion barrier on the steric hindrance of the diaziridine substituent has also been conducted using dynamic gas chromatography [28][29][30]. The identification of equilibrium (molecular) structures using joint analysis of gas phase electron diffraction, quantum chemistry, and spectroscopic data [25,26] is becoming a trend and has made diaziridine stereochemical study more visible. Table 1 summarizes the details of recent experimental structure identification studies of several diaziridine derivatives.  The rapid improvement in the quality of analysis instrumentation for experimental structure identification and detailed stereocenter has lead to the intensive study of the detailed structure determination of diaziridine. Experimental data regarding the structures of diaziridines are important for achieving deeper insight into the previously elucidated features of the diaziridine ring structure, in particular, for the comparison of its corresponding N-N or C-N bond length [21]. Recently, experimental data were obtained for the structural determination of N,N-disubstituted diaziridine [22] and its trisubstituted form, which possesses an additional alkyl group at position 3 [23,24], bis-diaziridine [25], and bicyclic diaziridine [26] derivatives by the method of gas electron diffraction. Most diaziridine derivatives are liquids; thus, the recent experimental determination of its structures on the basis of X-ray diffraction studies [21,27] has only been performed in a few cases. Investigation of conformational and configurational changes in order to understand the effect of the interconversion barrier on the steric hindrance of the diaziridine substituent has also been conducted using dynamic gas chromatography [28][29][30]. The identification of equilibrium (molecular) structures using joint analysis of gas phase electron diffraction, quantum chemistry, and spectroscopic data [25,26] is becoming a trend and has made diaziridine stereochemical study more visible. Table 1 summarizes the details of recent experimental structure identification studies of several diaziridine derivatives. * GED (gas electron diffraction), XRD (X-ray diffraction), DGC (dynamic gas chromatography), QC (quantum calculation), S (spectroscopy data).
Since the strained ring compound exhibits high detonation performance when releasing a large amount of strain energy during ring opening, diaziridine properties were taken into consideration in this study. The design and theoretical investigation of a series * GED (gas electron diffraction), XRD (X-ray diffraction), DGC (dynamic gas chromatography), QC (quantum calculation), S (spectroscopy data).
Since the strained ring compound exhibits high detonation performance when releasing a large amount of strain energy during ring opening, diaziridine properties were taken into consideration in this study. The design and theoretical investigation of a series Since the strained ring compound exhibits high detonation performance when releasing a large amount of strain energy during ring opening, diaziridine properties were taken into consideration in this study. The design and theoretical investigation of a series of trinitromethane derivatives of diaziridines as candidates for high-energy-density materials were conducted [31]. A computational study of several properties of diaziridines was performed by using Density Functional Theory-B3LYP functional and the aug-cc-pVDZ basis set with the Gaussian 09 program. The formation heat, energetic properties, stability, impact sensitivity, and the calculation of vibrational frequency were studied, and it was found that the trinitromethane substituent was beneficial for enhancing the detonation properties. Among the diaziridines tested, 12 ( Figure 3A) and 1-(trinitromethyl)diaziridine (13, Figure 3B) were confirmed to possess good potential as a high-density materials, possessing good detonation performance and higher stability.
Since the strained ring compound exhibits high detonation performance when releasing a large amount of strain energy during ring opening, diaziridine properties were taken into consideration in this study. The design and theoretical investigation of a series of trinitromethane derivatives of diaziridines as candidates for high-energy-density materials were conducted [31]. A computational study of several properties of diaziridines was performed by using Density Functional Theory-B3LYP functional and the aug-cc-pVDZ basis set with the Gaussian 09 program. The formation heat, energetic properties, stability, impact sensitivity, and the calculation of vibrational frequency were studied, and it was found that the trinitromethane substituent was beneficial for enhancing the detonation properties. Among the diaziridines tested, 12 ( Figure 3A) and 1-(trinitromethyl)diaziridine (13, Figure 3B) were confirmed to possess good potential as a high-density materials, possessing good detonation performance and higher stability.

Conventional Method for Recent Uses
The concept of using the conventional method for the advanced synthesis and application of diaziridines that are non-substituted at their N-terminal started with the use of a programmable batch of synthesis robots to design and develop a diazirine-based photoreactive compound [32]. This recent study mimicked the manual organic synthesis workflow by first synthesizing the 3H-diazirine-based crosslinker that mediates the for-

Conventional Method for Recent Uses
The concept of using the conventional method for the advanced synthesis and application of diaziridines that are non-substituted at their N-terminal started with the use of a programmable batch of synthesis robots to design and develop a diazirine-based photoreactive compound [32]. This recent study mimicked the manual organic synthesis workflow by first synthesizing the 3H-diazirine-based crosslinker that mediates the formation of diaziridine from ketone. The automatization was constructed through the addition of methanol-NH 3 and NH 2 OSO 3 H to the ketone, filtration and evaporation of the resulting diaziridine, all followed by the formation of 3H-diazirine by an I 2 -Et 2 O system at low temperature, ready for the next reaction process. The feasibility of the robotic synthesis workflow is possibly due to the convenient formation of diaziridine as an intermediate for the synthesis of diazirine, which can be formed using commercial starting materials and universal reagents. Therefore, the recent automatization of the conventional method for synthesis of 3H-diazirine broadens the potential of the formation of diaziridine as an intermediate for advanced uses.
In continuation of the oxidation of diaziridine followed by oxidation into diazirine, it is possible to construct the 15 N-15 N moiety when synthesizing the three-membered heterocycle diazirine (Figure 4). The conventional transformation of ketone 17 into diaziridine 18 can result in the formation of 15 N2-diazirine 19 molecular tags-hyperpolarized heteronuclei-contained in the diazirine moiety, supporting its potential as a molecular tag for NMR and MRI [34,35]. The readily oxidized 15 N2-diaziridine 18 was possible to synthesize using 15 NH3 and 15 N-labeled hydroxylamine O-sulfonic acid ( 15 NH2OSO3H), whereby the common I2-Et3N system was used for the formation of the final 15 N2-diazirine product. Although the overall yield achieved for the synthesized 15 N2-diazirine molecular tag was less than 50%, this is sufficient for further modification and analysis. Therefore, the development of subsequent utilizations of this isotope-labeled compound is to be expected.  In continuation of the oxidation of diaziridine followed by oxidation into diazirine, it is possible to construct the 15 N-15 N moiety when synthesizing the three-membered heterocycle diazirine ( Figure 4). The conventional transformation of ketone 17 into diaziridine 18 can result in the formation of 15 N 2 -diazirine 19 molecular tags-hyperpolarized heteronuclei-contained in the diazirine moiety, supporting its potential as a molecular tag for NMR and MRI [34,35]. The readily oxidized 15 N 2 -diaziridine 18 was possible to synthesize using 15 NH 3 and 15 N-labeled hydroxylamine O-sulfonic acid ( 15 NH 2 OSO 3 H), whereby the common I 2 -Et 3 N system was used for the formation of the final 15 N 2 -diazirine product. Although the overall yield achieved for the synthesized 15 N 2 -diazirine molecular tag was less than 50%, this is sufficient for further modification and analysis. Therefore, the development of subsequent utilizations of this isotope-labeled compound is to be expected.
the Pd(0)-catalyzed cross-coupling with 4-bromotoluene 15-resulting in the product 4,4'-(ethene-1,1-diyl)bis(methylbenzene) 16-under oxidative conditions following the addition of Ag2O as an oxidant (Scheme 1). The Pd(0)-catalyzed cross-coupling is the first example of a transition-metal-catalyzed reaction of diazirines supported by combination with the conventional oxidation of diaziridine, and significantly expands the chemistry of three-membered heterocycles. In continuation of the oxidation of diaziridine followed by oxidation into diazirine, it is possible to construct the 15 N-15 N moiety when synthesizing the three-membered heterocycle diazirine ( Figure 4). The conventional transformation of ketone 17 into diaziridine 18 can result in the formation of 15 N2-diazirine 19 molecular tags-hyperpolarized heteronuclei-contained in the diazirine moiety, supporting its potential as a molecular tag for NMR and MRI [34,35]. The readily oxidized 15 N2-diaziridine 18 was possible to synthesize using 15 NH3 and 15 N-labeled hydroxylamine O-sulfonic acid ( 15 NH2OSO3H), whereby the common I2-Et3N system was used for the formation of the final 15 N2-diazirine product. Although the overall yield achieved for the synthesized 15 N2-diazirine molecular tag was less than 50%, this is sufficient for further modification and analysis. Therefore, the development of subsequent utilizations of this isotope-labeled compound is to be expected.  The synthesis of spirocyclic 3H-diazirine-containing building blocks has been discussed in the literature to a lesser extent [36]; however, it can potentially be employed to probe underexplored parts of proteome with libraries derived from structurally similar scaffolds of the parent's analogues [13,14,37]. Currently, spirocyclic 3H-diazirines can be found in steroid [38][39][40], proline [41,42], the simplified structure of chamuvarinin [43] analogues, and 1,5-disubsituted tetrazoles containing 3H-diazirine [44]. In a process with fewer steps, the crude diaziridine formed using the conventional method can be used directly for the synthesis of functionalized spirocyclic 3H-diazirine without using the chromatographic technique [36]. The transformation of the five-to seven-membered heterocycle or bicycle ketone 20 ( Figure 5A) into diazirine 21 via NH 3 and NH 2 OSO 3 H can be used for the formation of diaziridine 22, when subjected to an I 2 -Et 3 N system after filtration and concentration. Despite the use of the conventional NH 2 OSO 3 H as a reagent for the formation of diaziridine as an intermediate, four-membered heterocyclic 3H-diazirine 23 can be achieved by the sequential formation of oxime 24 from ketone 25 and O-sulfonylation for the formation of diaziridine 26, followed by oxidation into diazirine 23 ( Figure 5B). This method is commonly used for the synthesis of 3-phenyl-3-(trifluoromethyl)-3H-diazirine (TPD) instead of spirocyclic (aliphatic skeleton) 3H-diazirine. Both conventional methods can be used to achieve scles of up to 50 g when synthesizing functionalized spirocyclic 3H-diazirine mediated by diaziridine formation. By using this one-pot approach, two types of spirocyclic compounds (compound 47g-h, Table 2, Entries 7-8) can also be successfully synthesized, and will be discussed in next section.
for the formation of diaziridine 26, followed by oxidation into diazirine 23 ( Figure 5B). This method is commonly used for the synthesis of 3-phenyl-3-(trifluoromethyl)-3H-diazirine (TPD) instead of spirocyclic (aliphatic skeleton) 3H-diazirine. Both conventional methods can be used to achieve scles of up to 50 g when synthesizing functionalized spirocyclic 3H-diazirine mediated by diaziridine formation. By using this one-pot approach, two types of spirocyclic compounds (compound 47g−h, Table 2, Entries 7-8) can also be successfully synthesized, and will be discussed in next section.  An ambient light stabile-favored photoaffinity labeling probe comprising 3-pyridyland 3-pyrimidyl-substituted 3-trifluoromethyl-diazirines 27 [45] was synthesized from alcohols 28, which directly transformed into an important scaffold representative, ketone 29 (Scheme 2). The replacement of the phenyl group with an electron-withdrawing pyridine or pyrimidine ring indicates that there were no obstacles during the sequential process of oxime formation and O-sulfonylation for diaziridine 30 formation. The conventional methods offered by the study showed that the 3-pyridyl-and 3-pyrimidyl-substituted 3-trifluoromethyl-diaziridines were stable and could be readily oxidized into diazirine 27 with Ag 2 O-ether system. An ambient light stabile-favored photoaffinity labeling probe comprising 3-pyridyland 3-pyrimidyl-substituted 3-trifluoromethyl-diazirines 27 [45] was synthesized from alcohols 28, which directly transformed into an important scaffold representative, ketone 29 (Scheme 2). The replacement of the phenyl group with an electron-withdrawing pyridine or pyrimidine ring indicates that there were no obstacles during the sequential process of oxime formation and O-sulfonylation for diaziridine 30 formation. The conventional methods offered by the study showed that the 3-pyridyl-and 3-pyrimidyl-substituted 3trifluoromethyl-diaziridines were stable and could be readily oxidized into diazirine 27 with Ag2O-ether system. The novel asymmetric synthesis of trifluoromethyldiazirine-based lactisole derivatives 31 occurs as a result of the preparation of trifluoroacetyl modified on the aromatic ring of lactisole, which then introduces the diazirinyl three-membered ring on the trifluoroacetyl group [46]. However, to synthesize the starting material, advanced methods are required; since the 2-, 3-, and 4-trifluoroacetyl lactisole derivatives 32 (Scheme 3) need to consider the optical retention of the protected lactate counterpart, the conventional diazirine 31 construction via diaziridine 33 formation can be easily conducted, starting with oximation with hydroxylamine hydrochloride, tosylation for the hydroxyl group of oxime, diaziridine formation with liquid ammonia, and a final step of oxidation with activated MnO2 to obtain diazirine. The chiral center configuration was checked for every step, and asymmetric 2-, 3-, and 4-trifluoromethyldiazirine-based lactisole 31 were able The novel asymmetric synthesis of trifluoromethyldiazirine-based lactisole derivatives 31 occurs as a result of the preparation of trifluoroacetyl modified on the aromatic ring of lactisole, which then introduces the diazirinyl three-membered ring on the trifluoroacetyl group [46]. However, to synthesize the starting material, advanced methods are required; since the 2-, 3-, and 4-trifluoroacetyl lactisole derivatives 32 (Scheme 3) need to consider the optical retention of the protected lactate counterpart, the conventional diazirine 31 construction via diaziridine 33 formation can be easily conducted, starting with oximation with hydroxylamine hydrochloride, tosylation for the hydroxyl group of oxime, diaziridine formation with liquid ammonia, and a final step of oxidation with activated MnO 2 to obtain diazirine. The chiral center configuration was checked for every step, and asymmetric 2-, 3-, and 4-trifluoromethyldiazirine-based lactisole 31 were able to be synthesized with fine yields.
The novel asymmetric synthesis of trifluoromethyldiazirine-based lactisole derivatives 31 occurs as a result of the preparation of trifluoroacetyl modified on the aromatic ring of lactisole, which then introduces the diazirinyl three-membered ring on the trifluoroacetyl group [46]. However, to synthesize the starting material, advanced methods are required; since the 2-, 3-, and 4-trifluoroacetyl lactisole derivatives 32 (Scheme 3) need to consider the optical retention of the protected lactate counterpart, the conventional diazirine 31 construction via diaziridine 33 formation can be easily conducted, starting with oximation with hydroxylamine hydrochloride, tosylation for the hydroxyl group of oxime, diaziridine formation with liquid ammonia, and a final step of oxidation with activated MnO2 to obtain diazirine. The chiral center configuration was checked for every step, and asymmetric 2-, 3-, and 4-trifluoromethyldiazirine-based lactisole 31 were able to be synthesized with fine yields. 3.1.2. Diaziridine as an Intermediate for "Minimalist" into "All-in-One" 3H-Diazirine The term "minimalist" aliphatic diazirine-based probe for photoaffinity labeling was popularized by Yao's group in 2013 [47], and while it was describes as "minimalist" diazirine linkers in a recent review [48]. The first generation [47] of so-called "minimalist" diazirine-based linkers was able to minimize the interference towards target binding and was built upon an alkyl diazirine and a terminal alkyne connected by short aliphatic chains [47,49,50]. These "minimalist" linkers 34 were made possible by synthesized representative aliphatic ketone containing alkyne 35, which had previously been transformed 3.1.2. Diaziridine as an Intermediate for "Minimalist" into "All-in-One" 3H-Diazirine The term "minimalist" aliphatic diazirine-based probe for photoaffinity labeling was popularized by Yao's group in 2013 [47], and while it was describes as "minimalist" diazirine linkers in a recent review [48]. The first generation [47] of so-called "minimalist" diazirine-based linkers was able to minimize the interference towards target binding and was built upon an alkyl diazirine and a terminal alkyne connected by short aliphatic chains [47,49,50]. These "minimalist" linkers 34 were made possible by synthesized representative aliphatic ketone containing alkyne 35, which had previously been transformed from ethyl acetoacetate 36 as the starting material (Scheme 4A). The minimum length was limited to 2 carbons on both sides of the diazirine moiety in the linker in order to enable the linker to possess different functional groups and to prevent any side reaction during the requisite NH 3 /NH 2 SO 3 H step in diaziridine 37 formation. Subsequently, the first-generation "minimalist" diazirine linker's 34 alkyne terminal was changed into cyclopropenes, which are similar in size, by rhodium-catalyzed reaction of α-diazo esters with alkynes, which have since been claimed to be the second generation of minimalist linkers [51,52].
from ethyl acetoacetate 36 as the starting material (Scheme 4A). The minimum length was limited to 2 carbons on both sides of the diazirine moiety in the linker in order to enable the linker to possess different functional groups and to prevent any side reaction during the requisite NH3/NH2SO3H step in diaziridine 37 formation. Subsequently, the first-generation "minimalist" diazirine linker's 34 alkyne terminal was changed into cyclopropenes, which are similar in size, by rhodium-catalyzed reaction of α-diazo esters with alkynes, which have since been claimed to be the second generation of minimalist linkers [51,52].
The strategy for the adjustment of fluorine into the "minimalist" aliphatic diazirine linker can be initiated by the reaction of ester 38 and monobromodifluoroalkyne 39 in order to form an equimolar mixture of difluoroketone 40 along with in situ formation of its hydrate 41, depending on the electrophilicity of the difluoroketone (Scheme 4B). This 1:1 mixture is then treated with hydroxylamine, followed by tosyl chloride in pyridine The strategy for the adjustment of fluorine into the "minimalist" aliphatic diazirine linker can be initiated by the reaction of ester 38 and monobromodifluoroalkyne 39 in order to form an equimolar mixture of difluoroketone 40 along with in situ formation of its hydrate 41, depending on the electrophilicity of the difluoroketone (Scheme 4B). This 1:1 mixture is then treated with hydroxylamine, followed by tosyl chloride in pyridine and ammonia in sequence [53], thus forming difluorodiaziridine 42 as an intermediate prior to oxidation with the I 2 -Et 3 N system, which results in 3H-diazirine 43. From this approaches, the trend of "minimalist" diazirine-based compounds has shifted towards: (1) the synthesis of aliphatic 3H-diaziridine via activation of tosyl oxime formation, in contrast to the conventional methods; and (2) addition of difluoro moiety into the "minimalist" diazirinebased compounds as an approach to mimicking the superior stability and selectivity [54] of 3-phenyl-3-(trifluoromethyl)-3H-diazirine (TPD).
The compact, "all-in-one" structure of the diaziridine-mediated radioisotope-free photoaffinity labeling probe can be categorized as a "minimalist" aliphatic 3H-diazirine that includes the aromatics, as well as the addition of the fluorine moiety. The parts of the "all-in-one" photoaffinity labeling probe comprise a diazirine as a photo-crosslinker (a carbene-generating group), a fluorinated carbon at the aliphatic 3H-diazirine side chain of the aromatics for mimicking TPD, and an alkyne [55] or azide [56] as a tag for the attachment of a detectable group via bioorthogonal click chemistry. "All-in-one" 3H-diazirine 44 containing both alkyne and azide are constructed from representative ketone 45 containing aromatics, fluorine moiety, and alkyne or azide terminal in advance, before transformation into the diaziridine 46 intermediate via tosyl oxime formation. The Swern oxidationdimethylsulfoxide and oxalyl chloride followed by the addition of triethylamine-can be used for the oxidation of the diaziridine 46 intermediate instead of Ag 2 O-Et 2 O, resulting in the "all-in-one" 3H-diazirine 44 (Scheme 4C). oxidation-dimethylsulfoxide and oxalyl chloride followed by the addition of triethylamine-can be used for the oxidation of the diaziridine 46 intermediate instead of Ag2O-Et2O, resulting in the "all-in-one" 3H-diazirine 44 (Scheme 4C). oxidation-dimethylsulfoxide and oxalyl chloride followed by the addition of triethylamine-can be used for the oxidation of the diaziridine 46 intermediate instead of Ag2O-Et2O, resulting in the "all-in-one" 3H-diazirine 44 (Scheme 4C). oxidation-dimethylsulfoxide and oxalyl chloride followed by the addition of triethylamine-can be used for the oxidation of the diaziridine 46 intermediate instead of Ag2O-Et2O, resulting in the "all-in-one" 3H-diazirine 44 (Scheme 4C). oxidation-dimethylsulfoxide and oxalyl chloride followed by the addition of triethylamine-can be used for the oxidation of the diaziridine 46 intermediate instead of Ag2O-Et2O, resulting in the "all-in-one" 3H-diazirine 44 (Scheme 4C). oxidation-dimethylsulfoxide and oxalyl chloride followed by the addition of triethylamine-can be used for the oxidation of the diaziridine 46 intermediate instead of Ag2O-Et2O, resulting in the "all-in-one" 3H-diazirine 44 (Scheme 4C). oxidation-dimethylsulfoxide and oxalyl chloride followed by the addition of triethylamine-can be used for the oxidation of the diaziridine 46 intermediate instead of Ag2O-Et2O, resulting in the "all-in-one" 3H-diazirine 44 (Scheme 4C). The dehydrogenation of the NH−NH bond in aliphatic diaziridine is a crucial transformation for generating the N=N double bond that acts as the main skeleton of aliphatic 3H-diazirine [57]. In the conventional method, different oxidants, including silver oxide tBuOK (2.3 equiv.) [57] 47f KOH (2.3 equiv.) [58] 7 47c KOH (3.3 equiv.) [58] 4 tBuOK (4.3 equiv.) [57] 47d KOH (4.3 equiv.) [ The dehydrogenation of the NH−NH bond in aliphatic diaziridine is a crucial transformation for generating the N=N double bond that acts as the main skeleton of aliphatic 3H-diazirine [57]. In the conventional method, different oxidants, including silver oxide tBuOK (2.3 equiv.) [57] 47g KOH (2.3 equiv.) [58] 8 47c KOH (3.3 equiv.) [58] 4 tBuOK (4.3 equiv.) [57] 47d KOH (4.3 equiv.) [ The dehydrogenation of the NH−NH bond in aliphatic diaziridine is a crucial transformation for generating the N=N double bond that acts as the main skeleton of aliphatic 3H-diazirine [57]. In the conventional method, different oxidants, including silver oxide tBuOK (3.3 equiv.) [57] 47h KOH (3.3 equiv.) [58] 3.1.3. In Situ Formation of Diaziridines in One-Pot Synthesis of 3H-Diazirine The dehydrogenation of the NH-NH bond in aliphatic diaziridine is a crucial transformation for generating the N=N double bond that acts as the main skeleton of aliphatic 3H-diazirine [57]. In the conventional method, different oxidants, including silver oxide or iodine in the presence of triethylamine, are introduced in order to transform diaziridines into 3H-diazirine following the removal of the ammonia [14,[58][59][60]. Diaziridines are basic and form salts, and in several cases, the pure form of diaziridines can be difficult to isolate [59]. During the synthesis of 3H-diazirine as a photoaffinity labeled-based photophore, 3H-diazirine can be readily used for the further post-functional synthesis of the corresponding probe [8], and "bypassing" the prior synthesis steps of 3H-diazirine is the ideal way to run. Thus, the strategy for the current development of 3H-diazirine synthesis is the in situ formation of diaziridine, and approaches for one-pot synthesis of 3H-diazirine take advantage of this more comprehensive method.
Aliphatic diaziridine is generally synthesized from ketone treated with liquid ammonia to form the imine, followed by reaction with hydroxylamine-O-sulfonic acid (HOSA, NH 2 OSO 3 H), enabling intramolecular cyclization to the diaziridine. The addition of a base to the synthesis process of conventional aliphatic diaziridine from aliphatic ketone can provide the direct dehydrogenation of the in situ formed diaziridine into 3H-diazirine. The alternative method for dehydrogenation of hydroazobenzene, combining the least expensive bulk chemicals of liquid NH 3 as a solvent and the readily available tBuOK system as a base, could be applied for the dehydrogenation of diaziridine [57]. Following this improvement, the use of base that can be easily handled and stored, as well as being highly available, such as KOH could enable gram-scale production [58]. Table 2 (Entries 1-8) shows the representative in situ formation of diaziridine 47a-h for the synthesis of 3H-diazirine 48. Kinetic study of the KOH-mediated direct transformations of diaziridine 47f into 3H-diazirine 48 ( Table 2, Entry 6) based on 1 H-NMR analysis indicated that diaziridine possessed appropriate reactivity for ready transformation into 3H-diazirine [58]. When adding HOSA to liquid ammonia in ketone at room temperature for 12 h, the corresponding diaziridine 47f (Table 2, Entry 6) was detected, as well as a trace amount of its 3H-diazirine form. Upon further treatment with KOH for 2 h, the 3H-diazirine was dramatically improved, indicating that diaziridine, as a precursor, can be converted directly, with the detection of no other by-products.
A carbene precursor, 3-phenyl-3-(trifluoromethyl)-3H-diazirine (TPD) derivatives are known for their ability to not promote cell death in the generation of active species in in vitro photoaffinity experiments [8]. Unlike the conventional synthesis of 3H-diazirine from diaziridine as an intermediate, the multistep reaction of TPD derivatives is performed from a phenyl trifluoromethyl ketone, which is transformed into the active species tosyl oxime, which is treated with an ammonia-Et 2 O solution at −78 • C, then brought to room temperature to allow the formation of diaziridine, which is oxidized with the I 2 -Et 3 N system as a final step to result in TPD [7,14,54]. Since the treatment of TPD after oxidation is time-consuming and yield-diminishing, the inevitable isolation of diaziridines can be skipped by using an alternative one-pot synthesis starting from tosyl oxime [61].
The treatment of tosyl oxime 49 with conventional reagents, depending on the temperature and the reaction time, can result in the formation of diaziridine 50 and/or its direct transformation into 3H-diazirine 51 [61]. The proposed mechanism for the transformation of tosyl oxime into diaziridine in past decades described the formation of the intermediate gem-diamine [62] following attack by NH 3 , and by removing the tosyl group and the proton, diaziridine is formed [61]. The current developments suggest that the neceesity of using liquid ammonia for the generation of NH 2 − species can elongate the deprotonation of diaziridine to form diazirine. The self-ionization of liquid NH 3 into NH 2 − species seems crucial for this reaction, as demonstrated by the search for additives to increase this species, which has determined in studies that LiNH 2 is superior to the inhibitor of NH 4 Cl ( Figure 6). It should be noted that diaziridine formation is crucial, and the aim to achieve diaziridine isolation by removing the ammonia from the reaction, in terms of the conventional method, overlooks the important involvement of ammonia in the transformation of diaziridine 50 into 3H-diazirine 51 using tosyl oxime 49 as the starting material. In order to broaden the applications of diaziridine-intermediated 52, and the one-pot synthesis TPD 54 from tosyl oxime 53, there are several viable substituents in the aromatic moiety of the starting material. Optically pure (trifluoromethyl)diazirinylphenylalanine ((Tmd)Phe) has been used as important building block in synthesis involving tosyl oxime as a precursor following the one-pot reaction method [61]. Method A prolongs the optical retention of (Tmd)Phe 55 and 56, while the addition of LiNH2 in Method B results in the racemization of the product 55. (Tmd)Phe 57, deuterated at the aromatic moiety, was synthesized via Method A, and its optical activity was retarded. Furthermore, the synthesis of 3-nitro 58 or 3-aminol 59 and 3-/4-methyl TPD 60−61 for the construction of phenylthiourea derivatives [63] and saccharin derivatives [64], respectively, using a one-pot (method A or B) system resulted in an almost quantitative yield compared with the con-  In order to broaden the applications of diaziridine-intermediated 52, and the one-pot synthesis TPD 54 from tosyl oxime 53, there are several viable substituents in the aromatic moiety of the starting material. Optically pure (trifluoromethyl)diazirinylphenylalanine ((Tmd)Phe) has been used as important building block in synthesis involving tosyl oxime as a precursor following the one-pot reaction method [61]. Method A prolongs the optical retention of (Tmd)Phe 55 and 56, while the addition of LiNH 2 in Method B results in the racemization of the product 55. (Tmd)Phe 57, deuterated at the aromatic moiety, was synthesized via Method A, and its optical activity was retarded. Furthermore, the synthesis of 3-nitro 58 or 3-aminol 59 and 3-/4-methyl TPD 60-61 for the construction of phenylthiourea derivatives [63] and saccharin derivatives [64], respectively, using a one-pot (method A or B) system resulted in an almost quantitative yield compared with the conventional stepwise Method C (Figure 7).

Improved Method for the Synthesis of 3-[3-(Trifluoromethyl)-3H-Diazirin-3yl]Aniline Derivatives
The needs of the aniline skeleton as a precursor for the multistep synthesis of the 3phenyl-3-(trifluoromethyl)-3H-diazirine-based photoaffinity labeling probe faces an obstacle with respect to obtaining high overall yields. Studies describing the synthesis methods employed in previous decades [65][66][67][68] provide limited experimental details or analytical data; thus, it has become necessary to improve on these methods. In a brief ( Figure  8), recent study has successfully synthesized 3-[3-(trifluoromethyl)-3H-diazirin-3-yl]aniline 62 with excellent yield through the reduction of nitrobenzene derivatives following the formation of 3H-diazirine 63a−b [63] or the protection of the amino group from undergoing 3H-diazirine formation, followed by its deprotection, resulting in 63c−e [63,69]. This new improvement showed that it is preferable to protect the amino group at the 3position with -Boc (63c), enabling convenent acidic deprotection after 3H-diazirine formation [63,69]. Meanwhile, the amino group at the 4-position can be subjected to two types of protecting group (-Boc 63d or -phthalimide 63e), and in the case ofphthalimide group (63e), this protecting group can be directly oxidized in conjunction with the diaziridine 64 moiety by MnO2-CH2Cl2 into a final product of 3-[3-(trifluoromethyl)-3H-diazirin-3-yl]aniline derivative 62 [63].

Improved Method for the Synthesis of 3-[3-(Trifluoromethyl)-3H-diazirin-3-yl]aniline Derivatives
The needs of the aniline skeleton as a precursor for the multistep synthesis of the 3phenyl-3-(trifluoromethyl)-3H-diazirine-based photoaffinity labeling probe faces an obstacle with respect to obtaining high overall yields. Studies describing the synthesis methods employed in previous decades [65][66][67][68] provide limited experimental details or analytical data; thus, it has become necessary to improve on these methods. In a brief (Figure 8), recent study has successfully synthesized 3-[3-(trifluoromethyl)-3H-diazirin-3-yl]aniline 62 with excellent yield through the reduction of nitrobenzene derivatives following the formation of 3H-diazirine 63a-b [63] or the protection of the amino group from undergoing 3H-diazirine formation, followed by its deprotection, resulting in 63c-e [63,69]. This new improvement showed that it is preferable to protect the amino group at the 3-position with -Boc (63c), enabling convenent acidic deprotection after 3H-diazirine formation [63,69]. Meanwhile, the amino group at the 4-position can be subjected to two types of protecting group (-Boc 63d or -phthalimide 63e), and in the case of -phthalimide group (63e), this protecting group can be directly oxidized in conjunction with the diaziridine 64 moiety by MnO 2 -CH 2 Cl 2 into a final product of 3-[3-(trifluoromethyl)-3H-diazirin-3-yl]aniline derivative 62 [63]. A few studies have performed the final step of forming the 3-[3-(trifluoromethyl)-3H-diazirin-3-yl] aniline derivatives from nitrobenzene derivatives through the reduction of the nitro moiety in sodium dithionite [68,70]. During the synthesis of photoreactive 2propoxyaniline derivatives as artificial sweeteners [71], the reduction by sodium dithionite after 3H-diazirine formation did not take place, and the diazirinyl moiety was unable to tolerate this condition, causing decomposition to occur. A possible route for this was diaziridine 65 formation following reduction with sodium dithionite (Figure 8). A moderate yield was obtained without breaking the diaziridinyl moiety, and validated the essential aspects of diaziridine formation, enabling a better understanding of the improved method for NH2-substituted 3-phenyl-3-(trifluoromethyl)-3H-diazirine 62.

Expansion of Fluorous 3H-Diaziridine as a Basis for 3H-Diazirine Application
A new fluorous 3H-diazirine-based photoaffinity labeling probe taking advantage of fluorous chromatography and fluorous solid phase extraction was developed. These techniques aim to retard fluorinated compounds on fluorinated silica gel, while all other organic material is washed off the column with the appropriate organic mobile phase. A new fluorous 3H-diaziridine-based photoaffinity labeling probe, with a longer perfluoroalkyl residue substituted for the trifluoromethyl group in the non-radioactive photoaffinity labeling probe, can be synthesized starting from the transformation of perfluoroalkylated ketone 66 (perfluorobutyl and perfluorooctyl ( Figure 9A) [72]) into diaziridine 67 through the conventional approach of oxime formation, tosylation, and treatment with liquid ammonia. The temporary silylation of the diaziridine moiety of compound 68 was performed by means of trimethylsilyl triflate, bromide-lithium exchange, and carboxylation with carbon dioxide for the conversion of benzoic acid. The final product was observed after the oxidation of diaziridine 68 into diazirine 69 with I2-Et3N. Prior to the study reporting the perfluoroalkylated 3H-diaziridine-based photoaffinity labeling probe, the perfluoropropyl and perfluorohexyl [73] residues had also been studied using the conventional approach, starting from the modification of perfluoroalkylated ketone 70 to result in diaziridine 71, which can readily be oxidized to 3H-diazirine 72 ( Figure 9B).  A few studies have performed the final step of forming the 3-[3-(trifluoromethyl)-3H-diazirin-3-yl] aniline derivatives from nitrobenzene derivatives through the reduction of the nitro moiety in sodium dithionite [68,70]. During the synthesis of photoreactive 2propoxyaniline derivatives as artificial sweeteners [71], the reduction by sodium dithionite after 3H-diazirine formation did not take place, and the diazirinyl moiety was unable to tolerate this condition, causing decomposition to occur. A possible route for this was diaziridine 65 formation following reduction with sodium dithionite (Figure 8). A moderate yield was obtained without breaking the diaziridinyl moiety, and validated the essential aspects of diaziridine formation, enabling a better understanding of the improved method for NH 2 -substituted 3-phenyl-3-(trifluoromethyl)-3H-diazirine 62.

Expansion of Fluorous 3H-Diaziridine as a Basis for 3H-Diazirine Application
A new fluorous 3H-diazirine-based photoaffinity labeling probe taking advantage of fluorous chromatography and fluorous solid phase extraction was developed. These techniques aim to retard fluorinated compounds on fluorinated silica gel, while all other organic material is washed off the column with the appropriate organic mobile phase. A new fluorous 3H-diaziridine-based photoaffinity labeling probe, with a longer perfluoroalkyl residue substituted for the trifluoromethyl group in the non-radioactive photoaffinity labeling probe, can be synthesized starting from the transformation of perfluoroalkylated ketone 66 (perfluorobutyl and perfluorooctyl ( Figure 9A) [72]) into diaziridine 67 through the conventional approach of oxime formation, tosylation, and treatment with liquid ammonia. The temporary silylation of the diaziridine moiety of compound 68 was performed by means of trimethylsilyl triflate, bromide-lithium exchange, and carboxylation with carbon dioxide for the conversion of benzoic acid. The final product was observed after the oxidation of diaziridine 68 into diazirine 69 with I 2− Et 3 N. Prior to the study reporting the perfluoroalkylated 3H-diaziridine-based photoaffinity labeling probe, the perfluoropropyl and perfluorohexyl [73] residues had also been studied using the conventional approach, starting from the modification of perfluoroalkylated ketone 70 to result in diaziridine 71, which can readily be oxidized to 3H-diazirine 72 ( Figure 9B). Diazirine-based crosslinkers (synthesized from the counterpart diaziridine) have been explored due to their ability to act as carbene-generating reagents. Since the 3-trifluoromethyl 3H-diazirine can be photoreactivated with light at 350 nm to generate carbene, this photophore is categorized as a high reactive species, and is able to rapidly form crosslinks to biomolecules with short photoirradiation times [8]. This universal crosslinker for aliphatic polymers, the simple bis-diazirine reagent, contains the known compound 1,3-bis(3-(trifluoromethyl)-3H-diazirin-3-yl)benzene or its pyridyl analog 73, which is volatile, and is prone to explosion ( Figure 10A) [74]. Thus, the bis-diazirine crosslinker was improved by the addition of an electron-deficient linker at the para position of diazirine compound 74 [74], which can be handled under ambient conditions, preventing any selfreaction due to the absence of any aliphatic C-H bonds ( Figure 10B). The so-called secondgeneration bis-diazirine 75 is an elongated perfluoroalkylated chain inspired by the firstgeneration bis-diazirine 74 [75]. The highly fluorinated bis-diazirines designed in the study can be developed into a flexible covalent adhesive ( Figure 10C). The simple 1stgeneration and 2nd-generation bis-diazirines are highly useful as crosslinkers for a broad range of feasible synthesis applications applications starting from representative ketone 76−78 into diaziridine 79−81, which can be directly oxidized by the I2−Et3N system.  Diazirine-based crosslinkers (synthesized from the counterpart diaziridine) have been explored due to their ability to act as carbene-generating reagents. Since the 3trifluoromethyl 3H-diazirine can be photoreactivated with light at 350 nm to generate carbene, this photophore is categorized as a high reactive species, and is able to rapidly form crosslinks to biomolecules with short photoirradiation times [8]. This universal crosslinker for aliphatic polymers, the simple bis-diazirine reagent, contains the known compound 1,3-bis(3-(trifluoromethyl)-3H-diazirin-3-yl)benzene or its pyridyl analog 73, which is volatile, and is prone to explosion ( Figure 10A) [74]. Thus, the bis-diazirine crosslinker was improved by the addition of an electron-deficient linker at the para position of diazirine compound 74 [74], which can be handled under ambient conditions, preventing any self-reaction due to the absence of any aliphatic C-H bonds ( Figure 10B). The so-called second-generation bis-diazirine 75 is an elongated perfluoroalkylated chain inspired by the first-generation bis-diazirine 74 [75]. The highly fluorinated bis-diazirines designed in the study can be developed into a flexible covalent adhesive ( Figure 10C). The simple 1st-generation and 2nd-generation bis-diazirines are highly useful as crosslinkers for a broad range of feasible synthesis applications applications starting from representative ketone 76-78 into diaziridine 79-81, which can be directly oxidized by the I 2− Et 3 N system.  Diazirine-based crosslinkers (synthesized from the counterpart diaziridine) have been explored due to their ability to act as carbene-generating reagents. Since the 3-trifluoromethyl 3H-diazirine can be photoreactivated with light at 350 nm to generate carbene, this photophore is categorized as a high reactive species, and is able to rapidly form crosslinks to biomolecules with short photoirradiation times [8]. This universal crosslinker for aliphatic polymers, the simple bis-diazirine reagent, contains the known compound 1,3-bis(3-(trifluoromethyl)-3H-diazirin-3-yl)benzene or its pyridyl analog 73, which is volatile, and is prone to explosion ( Figure 10A) [74]. Thus, the bis-diazirine crosslinker was improved by the addition of an electron-deficient linker at the para position of diazirine compound 74 [74], which can be handled under ambient conditions, preventing any selfreaction due to the absence of any aliphatic C-H bonds ( Figure 10B). The so-called secondgeneration bis-diazirine 75 is an elongated perfluoroalkylated chain inspired by the firstgeneration bis-diazirine 74 [75]. The highly fluorinated bis-diazirines designed in the study can be developed into a flexible covalent adhesive ( Figure 10C). The simple 1stgeneration and 2nd-generation bis-diazirines are highly useful as crosslinkers for a broad range of feasible synthesis applications applications starting from representative ketone 76−78 into diaziridine 79−81, which can be directly oxidized by the I2−Et3N system.

Unconventional Non-Substituted Diaziridine Synthesis Approaches
Recently, there have been two methods that have taken advantage of the conventional concept and turned it into brand new approaches to developing diaziridine synthesis. The first is the use of resin-bound sulfonyl oximes for the synthesis of 3-trifluoromethyl-3phenyldiaziridine [76]. A commercially available polystyrene-sulfonyl chloride 82, used as an equivalent to replace the common reagents mesyl or tosyl chloride, was previously reacted with oxime 83 to provide the desired solid-supported sulfonyl oxime. The conventional-like active species sulfonyl oxime 84-86 were then transformed by ammonia/dioxane solution to obtain a set of substituted diaziridines 87. The presence of the trifluoromethyl group has a role in the cleavage of the immobilized sulfonyl oxime precursors from their solid supports, therefore allowing good results for diaziridine 87 formation. The compatibility of the immobilization and cleavage protocols in this method was tested with several aromatic building blocks and alkyne groups ( Figure 11). An optical retention study of the optical active-aromatic substituents or building blocks remains to be performed for this method in the future.

Unconventional Non-Substituted Diaziridine Synthesis Approaches
Recently, there have been two methods that have taken advantage of the conventional concept and turned it into brand new approaches to developing diaziridine synthesis. The first is the use of resin-bound sulfonyl oximes for the synthesis of 3-trifluoromethyl-3-phenyldiaziridine [76]. A commercially available polystyrene−sulfonyl chloride 82, used as an equivalent to replace the common reagents mesyl or tosyl chloride, was previously reacted with oxime 83 to provide the desired solid-supported sulfonyl oxime. The conventional-like active species sulfonyl oxime 84−86 were then transformed by ammonia/dioxane solution to obtain a set of substituted diaziridines 87. The presence of the trifluoromethyl group has a role in the cleavage of the immobilized sulfonyl oxime precursors from their solid supports, therefore allowing good results for diaziridine 87 formation. The compatibility of the immobilization and cleavage protocols in this method was tested with several aromatic building blocks and alkyne groups ( Figure 11). An optical retention study of the optical active-aromatic substituents or building blocks remains to be performed for this method in the future.  The second unconventional method is the ammonia-free synthesis of 3-trifluoromethyl-3-phenyldiaziridine 88 [77]. The study started with the preparation of trifluoromethyl phenyl imines 89 using lithium bis(trimethylsilyl)amide [78] into trifluoromethyl phenyl ketone 90, resulting in N-TMS-ketimine 91 ( Figure 12). The solvolysis of this N-TMS-ketimine with methanol provides the representative imine for direct diaziridine formation. Since the use of the conventional reagent HOSA, which acts as the O-sulfonyl hydroxylamine source, did not yield the desired diaziridine product due to the reduced nucleophilicity of the amine function of the formd zwitterions, this study therefore then reacted p-toluenesulfonyl hydroxylamine with trifluoromethyl phenyl imines 89 as an advanced ammonia-free methodology for the synthesis of diaziridine 88 (Figure 12). The ammoniafree synthesis was carried out in significantly fewer reaction steps and with less purification of the intermediate compared to the multiple overnight steps of the conventional method. Various 3-trifluoromethyl-3-phenyldiaziridine derivatives can be explored for further study based on ammonia-free methods, despite the difficulty of synthesizing the imine intermediate. In addition, both of the unconventional methods described here successfully oxidized the resulting 3-trifluoromethyl-3-phenyldiaziridine into representative diazirine using the common oxidation reagents MnO 2 [76] or Ag 2 O [77]. The second unconventional method is the ammonia-free synthesis of 3-trifluoromethyl-3-phenyldiaziridine 88 [77]. The study started with the preparation of trifluoromethyl phenyl imines 89 using lithium bis(trimethylsilyl)amide [78] into trifluoromethyl phenyl ketone 90, resulting in N-TMS-ketimine 91 ( Figure 12). The solvolysis of this N-TMSketimine with methanol provides the representative imine for direct diaziridine formation. Since the use of the conventional reagent HOSA, which acts as the O-sulfonyl hydroxylamine source, did not yield the desired diaziridine product due to the reduced nucleophilicity of the amine function of the formd zwitterions, this study therefore then reacted p-toluenesulfonyl hydroxylamine with trifluoromethyl phenyl imines 89 as an advanced ammonia-free methodology for the synthesis of diaziridine 88 (Figure 12). The ammonia-free synthesis was carried out in significantly fewer reaction steps and with less purification of the intermediate compared to the multiple overnight steps of the conventional method. Various 3-trifluoromethyl-3-phenyldiaziridine derivatives can be explored for further study based on ammonia-free methods, despite the difficulty of synthesizing the imine intermediate. In addition, both of the unconventional methods described here successfully oxidized the resulting 3-trifluoromethyl-3-phenyldiaziridine into representative diazirine using the common oxidation reagents MnO2 [76] or Ag2O [77].

Conventional Method for Recent Uses
In general, conventional methods for the synthesis of diaziridines with HOSA have been performed in various solvents, such as water [79], methanol [80], or pure liquid ammonia [81]. When conventional methods were used for the reaction of cyclooctanone 92, benzylamine 93, and HOSA, the corresponding bicyclic diaziridine, 1,2 diazaspiro [2,7]decane 94 (Figure 13), was produced with quite a low yield (~20%) [81]. In order to achieve a better understanding of this, the solvent dependency of the N-monosubstituted diaziridine 94 yield was studied by means of GC-MS [82]. The highest yield of the product N-monosubstituted diaziridine 94 (~42%) corresponded to the use of an apolar aprotic solvent, such as cyclohexane or toluene. The reactions of nucleophilic diaziridines with electrophilic alkynes were established decades ago [83], and by means of the 15 N-labeling experiment, it was shown that the mechanism of the reaction could be assumed to involve the initial addition of an alkylated

Conventional Method for Recent Uses
In general, conventional methods for the synthesis of diaziridines with HOSA have been performed in various solvents, such as water [79], methanol [80], or pure liquid ammonia [81]. When conventional methods were used for the reaction of cyclooctanone 92, benzylamine 93, and HOSA, the corresponding bicyclic diaziridine, 1,2 diazaspiro[2,7]decane 94 (Figure 13), was produced with quite a low yield (~20%) [81]. In order to achieve a better understanding of this, the solvent dependency of the N-monosubstituted diaziridine 94 yield was studied by means of GC-MS [82]. The highest yield of the product N-monosubstituted diaziridine 94 (~42%) corresponded to the use of an apolar aprotic solvent, such as cyclohexane or toluene.
The second unconventional method is the ammonia-free synthesis of 3-trifluoromethyl-3-phenyldiaziridine 88 [77]. The study started with the preparation of trifluoromethyl phenyl imines 89 using lithium bis(trimethylsilyl)amide [78] into trifluoromethyl phenyl ketone 90, resulting in N-TMS-ketimine 91 ( Figure 12). The solvolysis of this N-TMSketimine with methanol provides the representative imine for direct diaziridine formation. Since the use of the conventional reagent HOSA, which acts as the O-sulfonyl hydroxylamine source, did not yield the desired diaziridine product due to the reduced nucleophilicity of the amine function of the formd zwitterions, this study therefore then reacted p-toluenesulfonyl hydroxylamine with trifluoromethyl phenyl imines 89 as an advanced ammonia-free methodology for the synthesis of diaziridine 88 (Figure 12). The ammonia-free synthesis was carried out in significantly fewer reaction steps and with less purification of the intermediate compared to the multiple overnight steps of the conventional method. Various 3-trifluoromethyl-3-phenyldiaziridine derivatives can be explored for further study based on ammonia-free methods, despite the difficulty of synthesizing the imine intermediate. In addition, both of the unconventional methods described here successfully oxidized the resulting 3-trifluoromethyl-3-phenyldiaziridine into representative diazirine using the common oxidation reagents MnO2 [76] or Ag2O [77].

Conventional Method for Recent Uses
In general, conventional methods for the synthesis of diaziridines with HOSA have been performed in various solvents, such as water [79], methanol [80], or pure liquid ammonia [81]. When conventional methods were used for the reaction of cyclooctanone 92, benzylamine 93, and HOSA, the corresponding bicyclic diaziridine, 1,2 diazaspiro [2,7]decane 94 (Figure 13), was produced with quite a low yield (~20%) [81]. In order to achieve a better understanding of this, the solvent dependency of the N-monosubstituted diaziridine 94 yield was studied by means of GC-MS [82]. The highest yield of the product N-monosubstituted diaziridine 94 (~42%) corresponded to the use of an apolar aprotic solvent, such as cyclohexane or toluene. The reactions of nucleophilic diaziridines with electrophilic alkynes were established decades ago [83], and by means of the 15 N-labeling experiment, it was shown that the mechanism of the reaction could be assumed to involve the initial addition of an alkylated The reactions of nucleophilic diaziridines with electrophilic alkynes were established decades ago [83], and by means of the 15 N-labeling experiment, it was shown that the mechanism of the reaction could be assumed to involve the initial addition of an alkylated nitrogen atom (N-monosubstituted diaziridine counterpart) to provide an intermediate that could subsequently undergo ring-opening and proton transfer, resulting in the adduct product [84]. The trapping reaction resulted in thermally generated benzyne species 95a-f with heteroatom-rich diaziridine 96 leading to N-arylated hydrazones 97a-f in a single step, while these could be converted into fused-ring indole derivatives 97c-e in some cases (Scheme 5). The conventional method for the synthesis of diaziridines has been used in recent years to form N-ethyl diaziridine 98a in quantitive yield from the reaction of 2-adamantane-2,3-[3H]-diazirine 99 with alkyl Grignard reagents (Scheme 6). Despite this success, the use of aryl Grignard reagents did not lead to N-phenyl diaziridine, and the expected diaziridine 98b was obtained only upon the addition of phenyl lithium. The direct reaction with acetylacetone was then conducted from the pure resulting N-phenyl diaziridine 98b, allowing pyrazole 100 and adamantanone 101 to be obtained with excellent yields (Scheme 6) [85].
nitrogen atom (N-monosubstituted diaziridine counterpart) to provide an intermediate that could subsequently undergo ring-opening and proton transfer, resulting in the adduct product [84]. The trapping reaction resulted in thermally generated benzyne species 95a−f with heteroatom-rich diaziridine 96 leading to N-arylated hydrazones 97a−f in a single step, while these could be converted into fused-ring indole derivatives 97c−e in some cases (Scheme 5). The conventional method for the synthesis of diaziridines has been used in recent years to form N-ethyl diaziridine 98a in quantitive yield from the reaction of 2-adamantane-2,3-[3H]-diazirine 99 with alkyl Grignard reagents (Scheme 6). Despite this success, the use of aryl Grignard reagents did not lead to N-phenyl diaziridine, and the expected diaziridine 98b was obtained only upon the addition of phenyl lithium. The direct reaction with acetylacetone was then conducted from the pure resulting N-phenyl diaziridine 98b, allowing pyrazole 100 and adamantanone 101 to be obtained with excellent yields (Scheme 6) [85]. nitrogen atom (N-monosubstituted diaziridine counterpart) to provide an intermediate that could subsequently undergo ring-opening and proton transfer, resulting in the adduct product [84]. The trapping reaction resulted in thermally generated benzyne species 95a−f with heteroatom-rich diaziridine 96 leading to N-arylated hydrazones 97a−f in a single step, while these could be converted into fused-ring indole derivatives 97c−e in some cases (Scheme 5). The conventional method for the synthesis of diaziridines has been used in recent years to form N-ethyl diaziridine 98a in quantitive yield from the reaction of 2-adamantane-2,3-[3H]-diazirine 99 with alkyl Grignard reagents (Scheme 6). Despite this success, the use of aryl Grignard reagents did not lead to N-phenyl diaziridine, and the expected diaziridine 98b was obtained only upon the addition of phenyl lithium. The direct reaction with acetylacetone was then conducted from the pure resulting N-phenyl diaziridine 98b, allowing pyrazole 100 and adamantanone 101 to be obtained with excellent yields (Scheme 6) [85].

Base Addition for Enhancement of N-Monosubstituted Diaziridine Formation
It is known that the formation of monocyclic diaziridine the three-component condensation of carbonyl compounds, primary aliphatic amines, and HOSA in protic medium is substantially dependent on pH value. A possible pathway for this is through the generation of carbenium-iminium cations, which subsequently react with the aminating reagent (HOSA) to form an intermediate compound of an aminal type. The presence of base would rapidly cyclize this intermediate to result in diaziridine [20]. The addition of base to the process was followed by diastereoselective synthesis of N-monosubstituted diaziridines coupled with neurotransmitter amino acid 102 [86]. The pH can be adjusted with the simultaneous addition of HOSA (1 equiv.) and 30% aqueous NaOH in order to neutralize the H 2 SO 4 that formed during the reaction, and the requirement vary depending on the substrate. Moreover, the new hybrid structure of N-monosubstituted diaziridine 102 can be prepared from the reaction of aldehydes or ketones 103 and amino acid ethyl esters 104 under mild conditions, with the major diastereomer corresponding to the racemic mixture of two meso-forms, 1R*, 2R*, 3S* (Scheme 7). Scheme 6. Diaziridine 98a−b synthesis from Grignard reaction of diazirine 99 and its reaction, resulting in pyrazole 100 and adamantanone 101. Condition: (i) EtMgBr or PhLi, Et2O, 0 °C or −78 °C, 2 h; (ii) acetylacetone, p-TsOH, EtOH, 80 °C, 24 h.

Base Addition for Enhancement of N-Monosubstituted Diaziridine Formation
It is known that the formation of monocyclic diaziridine the three-component condensation of carbonyl compounds, primary aliphatic amines, and HOSA in protic medium is substantially dependent on pH value. A possible pathway for this is through the generation of carbenium-iminium cations, which subsequently react with the aminating reagent (HOSA) to form an intermediate compound of an aminal type. The presence of base would rapidly cyclize this intermediate to result in diaziridine [20]. The addition of base to the process was followed by diastereoselective synthesis of N-monosubstituted diaziridines coupled with neurotransmitter amino acid 102 [86]. The pH can be adjusted with the simultaneous addition of HOSA (1 equiv.) and 30% aqueous NaOH in order to neutralize the H2SO4 that formed during the reaction, and the requirement vary depending on the substrate. Moreover, the new hybrid structure of N-monosubstituted diaziridine 102 can be prepared from the reaction of aldehydes or ketones 103 and amino acid ethyl esters 104 under mild conditions, with the major diastereomer corresponding to the racemic mixture of two meso-forms, 1R*, 2R*, 3S* (Scheme 7). Scheme 7. The pH-controlled diastereoselective synthesis of N-monosubstituted diaziridines coupled with neurotransmitter amino acids 102. Condition: H2NOSO3H in water-ethanol mixture at 0-5 °C, (i) pH 8-8.5 or (ii) pH 9.5-10.0.
The use of N-monosubstituted diaziridines as N-transfer reagents to α,β-unsaturated amides to form stereopure aziridines has been reported [16]. Taking advantage of the reactivity of diaziridine as an essential precursor, diastereoselective synthesis of N-monosubstituted diaziridine 105 can be conducted from simple aldehydes or ketones 106 with amines 107 [87]. The reaction takes place in the presence of hydroxylamine O-sulfonic acid (HOSA), a conventional aminating reagent. The addition of NaHCO3 results in a major product of N-monosubstituted diaziridine 105, suppressing the formation of N-monosubstituted imine (108, Figure 14). This weak inorganic base also showed high product yield compared with K3PO4 or Et3N, and can be used to replace an excess of amine counterparts. Scheme 7. The pH-controlled diastereoselective synthesis of N-monosubstituted diaziridines coupled with neurotransmitter amino acids 102. Condition: H 2 NOSO 3 H in water-ethanol mixture at 0-5 • C, (i) pH 8-8.5 or (ii) pH 9.5-10.0.
The use of N-monosubstituted diaziridines as N-transfer reagents to α,β-unsaturated amides to form stereopure aziridines has been reported [16]. Taking advantage of the reactivity of diaziridine as an essential precursor, diastereoselective synthesis of N-monosubstituted diaziridine 105 can be conducted from simple aldehydes or ketones 106 with amines 107 [87]. The reaction takes place in the presence of hydroxylamine O-sulfonic acid (HOSA), a conventional aminating reagent. The addition of NaHCO 3 results in a major product of Nmonosubstituted diaziridine 105, suppressing the formation of N-monosubstituted imine (108, Figure 14). This weak inorganic base also showed high product yield compared with K 3 PO 4 or Et 3 N, and can be used to replace an excess of amine counterparts. The method provides the resulting N-monosubstituted diaziridines 105 with a single diastereomer and a wide variety of aromatic and aliphatic aldehydes or ketones 106 and amines 107. The method provides the resulting N-monosubstituted diaziridines 105 with a single diastereomer and a wide variety of aromatic and aliphatic aldehydes or ketones 106 and amines 107.

Conventional Method for Recent Uses
N,N-disubstituted diaziridines containing trifluoromethyl at the 3-position 117 can be synthesized using conventional conditions. Various trifluoromethyl imines 118 have been used in amination reactions with NsONHCO 2 Et as the aminating agent [88]. A twofold excess of NsONHCO 2 Et in CH 2 C1 2 without any addition of base at room temperature can give the corresponding N,N-disubstituted diaziridines 117 (Scheme 8A). N,N-Disubstituted diaziridines 119 were also successfully synthesized by the reaction of trifluoromethyl imines 120 with NsONHCO 2 t-Bu, a carbamate, which is known to give amination reactions only by an ionic pathway involving the corresponding aza-anion (Scheme 8B). The advantage of using conventional methods for the synthesis of N,N-disubstituted diaziridines was also observed when synthesizing bidiaziridine 121 from α-diimines 122 [89]. A two-phase H 2 O/CH 2 Cl 2 system and the portion-wise addition of both amination agent and base (NsONHCO 2 Et and CaO) is considered to favor the formation of the monodiaziridine (E)-3-(iminomethyl)diaziridine-1-carboxylates 123, rather than its bidiaziridine 121 ( Figure 16A). Further functionalization of this monodiaziridine, 123a,c,d, can be performed to obtain a hybrid compound containing an diaziridine and oxaziridine ring in one molecule of 3-(diaziridin-3-yl)oxaziridines 124 ( Figure 16B) [89].   In line with the synthesis of the hybrid compound, a diastereoselective method for the synthesis of diaziridines with N-and/or C-cyclopropyl substituents (125 and/or 126) was developed [90] using the conventional methods. A one-pot, three-component condensation of cyclopropyl-containing carbonyl compounds 127, primary aliphatic amines, including cyclo propylamine 128, and N-chloroalkylamines 129 was conducted in the organic solvents. This typical reaction was carried out under mild conditions and in the presence of bases (Scheme 9), resulting in the predominance of diaziridine product 125 and/or 126, with the major diastereomer being the racemic mixture of two meso-forms, and the racemic mixtures of two enantiomers for the minor diastereomer. The use of K2CO3 as a base, and an aprotic solvent (CHCl3) obtained from equimolar amounts of aldehyde, cyclopropylamine, and pre-synthesized N-chloroalkylamines can provide access to compounds with cyclopropyl substituents on the nitrogen atom of the diaziridine ring. As for the enantio-and diastereoselective synthesis of diaziridines 130 via aziridination of N-tosyl aldimines 131 while applying modified hydroxylamine 132 In line with the synthesis of the hybrid compound, a diastereoselective method for the synthesis of diaziridines with Nand/or Ccyclopropyl substituents (125 and/or 126) was developed [90] using the conventional methods. A one-pot, three-component condensation of cyclopropyl-containing carbonyl compounds 127, primary aliphatic amines, including cyclo propylamine 128, and N-chloroalkylamines 129 was conducted in the organic solvents. This typical reaction was carried out under mild conditions and in the presence of bases (Scheme 9), resulting in the predominance of diaziridine product 125 and/or 126, with the major diastereomer being the racemic mixture of two meso-forms, and the racemic mixtures of two enantiomers for the minor diastereomer. The use of K 2 CO 3 as a base, and an aprotic solvent (CHCl 3 ) obtained from equimolar amounts of aldehyde, cyclopropylamine, and pre-synthesized N-chloroalkylamines can provide access to compounds with cyclopropyl substituents on the nitrogen atom of the diaziridine ring. As for the enantioand diastereoselective synthesis of diaziridines 130 via aziridination of N-tosyl aldimines 131 while applying modified hydroxylamine 132 under asymmetric phase-transfer catalysis 133, it was recognized that K 2 CO 3 was too weak to mediate this reaction [91]. Thus, K 2 PO 4 was then utilized, and the reaction rate was significantly enhanced, and gave diaziridine with similar selectivity. By taking advantage of a phase-transfer catalyzed nitrogen insertion into the π-system of N-tosyl aldimines 131 and the use of N-transfer agent of N-benzyl-O-benzoyl hydroxylamine 133, the afforded N-tosyl-N -benzyl-diaziridines 130 can be synthesized as a single diastereomer in up to high yields with high to excellent enantioselectivity (up to 96% ee, Scheme 10). under asymmetric phase-transfer catalysis 133, it was recognized that K2CO3 was too weak to mediate this reaction [91]. Thus, K2PO4 was then utilized, and the reaction rate was significantly enhanced, and gave diaziridine with similar selectivity. By taking advantage of a phase-transfer catalyzed nitrogen insertion into the π-system of N-tosyl aldimines 131 and the use of N-transfer agent of N-benzyl-O-benzoyl hydroxylamine 133, the afforded N-tosyl-N′-benzyl-diaziridines 130 can be synthesized as a single diastereomer in up to high yields with high to excellent enantioselectivity (up to 96% ee, Scheme 10).  Figure 17). In [92,93], mild conditions were represented by the use of ionic liquid medium, and it was found that the reaction could be managed by ionic liquid, rather than the organic solvent, of MeCN [94]. In some case, heating was required (40 or 50 °C) to to initiate the reaction with olefins 136, which resulted in the [3 + 2] [93]. The transformation of diaziridine 134 into active species of azomethine imines 135 showed different reactivity when reacted with arylidenemalononitrile 138 (Figure 17). The presence of an electron-withdrawing NO2 substituent in the aromatic ring of arylidenemalononitrile, as the starting material, resulted in pyrazoline 139, and the isolation of arylidenemalononitriles containing aromatic fragments of the starting bicyclic diaziridines 140 was also achieved [95]. The annulations of  Figure 17). In [92,93], mild conditions were represented by the use of ionic liquid medium, and it was found that the reaction could be managed by ionic liquid, rather than the organic solvent, of MeCN [94]. In some case, heating was required (40 • C or 50 • C) to to initiate the reaction with olefins 136, which resulted in the [ [93]. The transformation of diaziridine 134 into active species of azomethine imines 135 showed different reactivity when reacted with arylidenemalononitrile 138 (Figure 17). The presence of an electron-withdrawing NO 2 substituent in the aromatic ring of arylidenemalononitrile, as the starting material, resulted in pyrazoline 139, and the isolation of arylidenemalononitriles containing aromatic fragments of the starting bicyclic diaziridines 140 was also achieved [95]. The annulations of azomethine imines 135, derived from the representative diaziridine 134 with 1H-indole-2,3-diones 141, can occur on the basis of the reaction between azomethine imines and carbonyl compounds. There are two types of product introduced in the ionic liquid of [bmim][BF4] systems: pyrazolines 142, which are proposed to be proced by the induction of a formal 1,4-H shift in azomethine imine; and pyrazoles 143 (Figure 17), which are most likely to emerge as a result of the oxidation of pyrazolines by air oxygen [96]. Moreover, the reaction between 6-aryl-1,5-diazabicyclo[3.1.0]hexanes and 1,3-diarylpropenones was also conducted under microwave irradiation (110 • C), which is compliant with the principles of green chemistry in organic synthesis [97]. The [3 + 2] cycloaddition products of perhydropyrazolopyrazoles were formed in fine yields as single diastereomers.
[bmim][BF4] systems: pyrazolines 142, which are proposed to be proced by the induction of a formal 1,4-H shift in azomethine imine; and pyrazoles 143 (Figure 17), which are most likely to emerge as a result of the oxidation of pyrazolines by air oxygen [96]. Moreover, the reaction between 6-aryl-1,5-diazabicyclo[3.1.0]hexanes and 1,3-diarylpropenones was also conducted under microwave irradiation (110 °C), which is compliant with the principles of green chemistry in organic synthesis [97]. The [3 + 2] cycloaddition products of perhydropyrazolopyrazoles were formed in fine yields as single diastereomers.

Metal Catalysis of Diaziridines Ring Opening
A single reagent that is able catalyze multiple mechanistically distinct processes in a chemical reaction known as an auto-tandem catalyst [98], and the transition metal used for this process is gold(I). The ring opening of diaziridines [99] is started by the synthesis of N-monosubstituted diaziridine by the conventional method of reacting ketone 144, benzyl, and the aminating reagent NH2OSO3H. A minimal modification at the free N-terminal of diaziridine resulted in 1-benzyl-1,2-diazaspiro [2,5]octane 145, which was then used as the starting material for an auto-tandem catalysis reaction mediated by gold(I). The model reaction was conducted by reacting diaziridine 145 with phenylacetylene 146, and it was found that the product 3-pyrazoline 147 was preferentially obtained using Ph3AuNTf2 as the catalyst, rather than other catalysts. The alkyne insertion product 146 was possibly an intermediate in the process, since it can be directly transformed into the product 3-pyrazoline 147 by the use of Ph3AuNTf2. Taken together, gold(I) as an auto-tandem catalyst is capable of being used to pursue the typical subsequent ring opening of diaziridine 145 and the cyclization of 148 ( Figure 18).

Metal Catalysis of Diaziridines Ring Opening
A single reagent that is able catalyze multiple mechanistically distinct processes in a chemical reaction known as an auto-tandem catalyst [98], and the transition metal used for this process is gold(I). The ring opening of diaziridines [99] is started by the synthesis of N-monosubstituted diaziridine by the conventional method of reacting ketone 144, benzyl, and the aminating reagent NH 2 OSO 3 H. A minimal modification at the free Nterminal of diaziridine resulted in 1-benzyl-1,2-diazaspiro [2,5]octane 145, which was then used as the starting material for an auto-tandem catalysis reaction mediated by gold(I). The model reaction was conducted by reacting diaziridine 145 with phenylacetylene 146, and it was found that the product 3-pyrazoline 147 was preferentially obtained using Ph 3 AuNTf 2 as the catalyst, rather than other catalysts. The alkyne insertion product 146 was possibly an intermediate in the process, since it can be directly transformed into the product 3-pyrazoline 147 by the use of Ph 3 AuNTf 2 . Taken together, gold(I) as an autotandem catalyst is capable of being used to pursue the typical subsequent ring opening of diaziridine 145 and the cyclization of 148 ( Figure 18). in iron salt can be processed into [1,2,4]-triazines 151a,b as a single diastereoisomer by using FeCl3 (Scheme 11). The chelation of aziridines with FeCl3 can lead to stereospecific ring opening using azomethine imine intermediate derived from diaziridine and the diasteroselectivity potentially obtained by the steric factors during the approaches of aziridine with the azomethine imine. Diaziridine 149 was tested using optically active aziridine 150b, demonstrating the stereoselectivity of this typical iron-catalyzed reaction [100]. The one-pot reaction of bicyclic diaziridines 152 and (2-bromo-2-nitrovinyl)arenes 153 resulting in bicyclic cationic 154 (2,3-dihydro-1H-pyrazolo[1,2-a]pyrazol-4-ium as cation and [Ce 3+ (NO3)6] 3− as anion) can only be conducted under the action of ceric ammonium nitrate (CAN) and MeCN ( Figure 19). CAN as the catalyst can trigger in situ diaziridine ring opening of bicyclic diaziridines or metathesis of azomethine imine, the occurrence of [3+2] cycloaddition of (2-bromo-2-nitrovinyl)arenes, followed by the aromatization of the formed pyrazolidine ring [101]. This metal catalysis of diaziridine ring opening approaches (Scheme 11 and Figure 19) provides the advantage of simplicity, and is a powerful tool for the synthesis of hydrazine bicyclic compounds.  Figure 19). CAN as the catalyst can trigger in situ diaziridine ring opening of bicyclic diaziridines or metathesis of azomethine imine, the occurrence of [3+2] cycloaddition of (2-bromo-2-nitrovinyl)arenes, followed by the aromatization of the formed pyrazolidine ring [101]. This metal catalysis of diaziridine ring opening approaches (Scheme 11 and Figure 19) provides the advantage of simplicity, and is a powerful tool for the synthesis of hydrazine bicyclic compounds.

Diaziridine Reaction with Donor-Acceptor Cyclopropanes/Cyclopropenes
The first [3+3]-annulation of two different three-membered rings of bicyclic diaziridines 154a−n and donor-acceptor cyclopropanes 155 was reported in 2018 [102]. The reaction afforded perhydropyridazine derivatives 156 in high yields and diastereoselectivity under mild Lewis acid catalysis of Ni(ClO4)2·6H2O ( Figure 20). Under the same conditions, the difference of alkyl substituent(s) at the C(6) atom of bicyclic diaziridine 154k,o−u can prevent (3+3)-annulation. The spiro-[cyclohexane-1,6′-(1,5-diazabicyclo[3.1.0]hexane)] and other bulky substituents at the C(3) atom of the diaziridine ring of 1,5-diazabicyclo[3.1.0]hexanes (154k,o−u,v) did not produce the corresponding hexahydropyridazine 156 and afford 1-alkylated 2,3-dihydropyrazoles 157 or 158 in the reaction with donor-acceptor cyclopropanes 155 [103]. The reaction possibly proceeds via the alkylation of a diaziridine derivative with a Lewis acid-activated cyclopropane, followed by hydra-  [103]. The reaction possibly proceeds via the alkylation of a diaziridine derivative with a Lewis acid-activated cyclopropane, followed by hydration of the formed 1,6-zwitterion, producing hemiaminal. Following this process, the elimination of the carbonyl compound and the air oxidation of the formed pyrazolidine accomplishes the synthesis of 1-alkylated 2,3-dihydropyrazole derivatives (157 or 158, Figure 20).  Since diaziridine is a strained ring system that can undergo N−N bond cleavage, the ring opening of bicyclic diaziridine 159 was continued for its reaction with enoldiazoace- Since diaziridine is a strained ring system that can undergo N-N bond cleavage, the ring opening of bicyclic diaziridine 159 was continued for its reaction with enoldiazoacetates 160, which resulted in the cycloadduct 161 (Scheme 12). The metallo-enolcarbenes was initially generated to undergo the novel [3 + 2]-cycloaddition. The asymmetric synthesis process is able to produce the cycloaddition product 161 with 31% ee or 95% ee, depending on the isomeric mixture of the starting material. The metallocarbene source of donor-acceptor cyclopropene 162 is also able to form the cycloaddition product 161 in 95% ee (Scheme 12), suggesting that the initially generated cycloaddition of metalloenolcarbenes is possible at a faster rate than the formation of the corresponding donoracceptor cyclopropene 162 [104]. Since diaziridine is a strained ring system that can undergo N−N bond cleavage, the ring opening of bicyclic diaziridine 159 was continued for its reaction with enoldiazoacetates 160, which resulted in the cycloadduct 161 (Scheme 12). The metallo-enolcarbenes was initially generated to undergo the novel [3 + 2]-cycloaddition. The asymmetric synthesis process is able to produce the cycloaddition product 161 with 31% ee or 95% ee, depending on the isomeric mixture of the starting material. The metallocarbene source of donor-acceptor cyclopropene 162 is also able to form the cycloaddition product 161 in 95% ee (Scheme 12), suggesting that the initially generated cycloaddition of metallo-enolcarbenes is possible at a faster rate than the formation of the corresponding donor-acceptor cyclopropene 162 [104].

Unconventional N,N-Disubstituted Diaziridine Synthesis Approach
An unconventional nonmetallic and photocatalytic approach to N,N-disubstituted diaziridine synthesis was developed [105], excluding hydroxylamine-O-sulfonic acid [20] and ethyl nosyloxycarbamate [18] for the mediation of condensations of carbonyl compounds, amines, or ammonia. A blue LED, an organic photocatalyst (rose Bengal 163), and a Lewis acid such as the oxidant PhI(OAc) 2 164 were used to generate functionalized diaziridines with excellent reaction rates and yields that also showed high stereoselectivities for the synthesis of diaziridines 165 with chiral substituents. The reaction proceeded through the in situ formation of nitrene 166 and an imine 167 intermediate, whereby their formation involved the light-activated Rose Bengal in order to convert related species from the combination of PhI(OAc) 2 164, amine 168, with 1,2-diol 169 or the simultaneous combination of PhI(OAc) 2 directly with amine. The typical N,N-disubstituted diaziridine 165 synthesized using this novel and extraordinary method is summarized in Scheme 13. ziridines with excellent reaction rates and yields that also showed high stereoselectivities for the synthesis of diaziridines 165 with chiral substituents. The reaction proceeded through the in situ formation of nitrene 166 and an imine 167 intermediate, whereby their formation involved the light-activated Rose Bengal in order to convert related species from the combination of PhI(OAc)2 164, amine 168, with 1,2-diol 169 or the simultaneous combination of PhI(OAc)2 directly with amine. The typical N,N-disubstituted diaziridine 165 synthesized using this novel and extraordinary method is summarized in Scheme 13.

Conclusions
The non-, N-mono-, and N,N-disubstituted diaziridines are attractive skeletons as building blocks in the synthesis of important intermediates and precursors with excellent stereochemical properties. The trend of diaziridine formation is still following the conventional concept, wherein valuable synthesized diaziridine derivatives are added together with various substituents. More unconventional approaches are limited to the period of the last decade, and further studies aiming to extend these unconventional methods remain to be performed. The study of diaziridine transformation in the field of organic and pharmaceutical chemistry-especially to become a precursor in diazirine-based photoaffinity labeling probes for drug design-as well as its stereochemistry, offer great opportunities for further exploration.