Unsubstituted Oximes as Potential Therapeutic Agents

: Oximes, which are highly bioactive molecules, have versatile uses in the medical sector and have been indicated to possess biological activity. Certain oximes exist in nature in plants and animals, but they are also obtained by chemical synthesis. Oximes are known for their anti-inﬂammatory, antimicrobial, antioxidant and anticancer activities. Moreover, they are therapeutic agents against organophosphate (OP) poisoning. Two oximes are already commonly used in therapy. Due to these abilities, new oxime compounds have been synthesized, and their biological activity has been veriﬁed. Often, modiﬁcation of carbonyl compounds into oximes leads to increased activity. Nevertheless, in some cases, oxime activity is connected to the activity of the substrate. Recent works have revealed that new oxime compounds can demonstrate such functions and thus are considered to be potential drugs for pathogenic diseases, as adjuvant therapy in various types of cancer and inﬂammation and as potential next-generation drugs against OP poisoning.


Introduction
The progressive and rampant development of the world, technological advances, overpopulation and environmental issues may cause many threats to human health. We are facing serious problems with a growing number of cancer-related and pathogenic diseases that cannot be effectively treated in traditional ways. Other detrimental factors are dangers from the development of agriculture, especially fertilization and the use of pesticides. The exposure to organophosphates (OPs) results in poisoning, and untreated OPs can lead to death. Obviously, the grand developments in medicine in recent years are undeniable, but drug alternatives have yet to be sought. Research is largely inspired by substances that occur in nature. Since 1960s plant oximes are known as one of the precursors of secondary metabolites in plants both aliphatic and aromatic forms. The majority of oximes are produced by one of the CYP79 family member-cytochrome P450. All flowering plants possessing CYP79 blueprint are, theoretically, able to produce oximes. These metabolites are often elements of the protective systems of plants that act in their defense against herbivores and pests in particular as intermediates in cyanogenic glycosides formation. Most of plant oximes are excreted as volatiles, only those that are converted into glycosides are stored in the plant. Oximes of natural origin often possess biological activities. Their presence in the biological sample might be omitted: oximes are intermediates for biosynthesis of other metabolites and their concentration is often low. [1]. Oximes in animals are, among other things, part of the olfactory communication between the animals. Oximes occur in nature as elements of metabolic pathways and are part of the enzymatic oxidation of amino acids and products of its decarboxylation. Two isomers are possible due to specificity of the C=N double bond; there are two Additionally, one oxime synthetized by Li was found to be a potent compound in blocking NO (IC50 = 6.66 µM) and interleukina 6 (IL-6; IC50 = 5.07 µM) production. IL-6 is one of the proinflammatory cytokines. [8]. The results of the Tharini and Sangeetha study indicate that 3,3dimethyl-2,6-dimethylpiperidine-4-one oxime ( Figure 2) has severe general anti-inflammatory activity in contrast to the typical drug dexamethasone [9]. Additionally, one oxime synthetized by Li was found to be a potent compound in blocking NO (IC 50 = 6.66 µM) and interleukina 6 (IL-6; IC 50 = 5.07 µM) production. IL-6 is one of the proinflammatory cytokines. [8]. The results of the Tharini and Sangeetha study indicate that 3,3-dimethyl-2,6-dimethylpiperidine-4-one oxime ( Figure 2) has severe general anti-inflammatory activity in contrast to the typical drug dexamethasone [9].
Additionally, one oxime synthetized by Li was found to be a potent compound in blocking NO (IC50 = 6.66 µM) and interleukina 6 (IL-6; IC50 = 5.07 µM) production. IL-6 is one of the proinflammatory cytokines. [8]. The results of the Tharini and Sangeetha study indicate that 3,3dimethyl-2,6-dimethylpiperidine-4-one oxime ( Figure 2) has severe general anti-inflammatory activity in contrast to the typical drug dexamethasone [9]. Zeferino-Diaz and coworkers recently presented research on oxocholestane oxime diosgenin derivatives ( Figure 3) as potential anti-inflammatory drugs. In in vivo studies their compounds have been indicated to reduce inflammation and edema triggered in mice ear. The expression of proinflammatory genes such as tumor necrosis factor (TNF-α), prostaglandin-endoperoxide synthase 2 (COX-2) and IL-6, with macrophage migration inhibitory factor (MIF) was repressed by the three most active oximes [10]. Zeferino-Diaz and coworkers recently presented research on oxocholestane oxime diosgenin derivatives ( Figure 3) as potential anti-inflammatory drugs. In in vivo studies their compounds have been indicated to reduce inflammation and edema triggered in mice ear. The expression of proinflammatory genes such as tumor necrosis factor (TNF-α), prostaglandin-endoperoxide synthase 2 (COX-2) and IL-6, with macrophage migration inhibitory factor (MIF) was repressed by the three most active oximes [10]. In their research Liu and colleagues presented in vivo activity of 6-bromoindirubin-3′-oxime ( Figure 4) on the inflammatory reaction. They analyzed response to mastitis induced by lipopolysaccharide and signals of inflammation in mouse mammary epithelial cells (MMECs). Pretreatment with tested oxime led to downregulation of the expression of the proinflammatory factors and reduced inflammatory lesions [11]. Kasare et al. presented studies involving protein denaturation inhibition bioassay of bovine serum albumin to examine if protein is protected from denaturation. Both tested ligands ( Figure 5) acquire remarkable anti-inflammatory activity in comparison to diclofenac sodium, achieving values of IC50 46.76 µM/mL and 55.77 µM/mL respectively [12].  In their research Liu and colleagues presented in vivo activity of 6-bromoindirubin-3 -oxime ( Figure 4) on the inflammatory reaction. They analyzed response to mastitis induced by lipopolysaccharide and signals of inflammation in mouse mammary epithelial cells (MMECs). Pretreatment with tested oxime led to downregulation of the expression of the proinflammatory factors and reduced inflammatory lesions [11]. Zeferino-Diaz and coworkers recently presented research on oxocholestane oxime diosgenin derivatives ( Figure 3) as potential anti-inflammatory drugs. In in vivo studies their compounds have been indicated to reduce inflammation and edema triggered in mice ear. The expression of proinflammatory genes such as tumor necrosis factor (TNF-α), prostaglandin-endoperoxide synthase 2 (COX-2) and IL-6, with macrophage migration inhibitory factor (MIF) was repressed by the three most active oximes [10]. In their research Liu and colleagues presented in vivo activity of 6-bromoindirubin-3′-oxime ( Figure 4) on the inflammatory reaction. They analyzed response to mastitis induced by lipopolysaccharide and signals of inflammation in mouse mammary epithelial cells (MMECs). Pretreatment with tested oxime led to downregulation of the expression of the proinflammatory factors and reduced inflammatory lesions [11]. Kasare et al. presented studies involving protein denaturation inhibition bioassay of bovine serum albumin to examine if protein is protected from denaturation. Both tested ligands ( Figure 5) acquire remarkable anti-inflammatory activity in comparison to diclofenac sodium, achieving values of IC50 46.76 µM/mL and 55.77 µM/mL respectively [12].  Kasare et al. presented studies involving protein denaturation inhibition bioassay of bovine serum albumin to examine if protein is protected from denaturation. Both tested ligands ( Figure 5) acquire remarkable anti-inflammatory activity in comparison to diclofenac sodium, achieving values of IC 50 46.76 µM/mL and 55.77 µM/mL respectively [12].  Kasare et al. presented studies involving protein denaturation inhibition bioassay of bovine serum albumin to examine if protein is protected from denaturation. Both tested ligands ( Figure 5) acquire remarkable anti-inflammatory activity in comparison to diclofenac sodium, achieving values of IC50 46.76 µM/mL and 55.77 µM/mL respectively [12].  Hassan et al. presented results of anti-inflammatory activity of various novel quinoline hybrids. Three of compounds ( Figure 6) possessing oxime moiety presented excellent general anti-inflammatory activity in in vivo studies, using paw edema in rats induced by carrageenan injection, compared to indomethacin. Observed percentage of edema inhibition were 100%, 101% and 111% respectively [13].

The Antimicrobial Activity
Cytotoxicity is one property of oximes; thus, oximes are therapeutic agents for bacterial, fungal and viral infections. Nocardicin A (Figure 7) is the first β-lactam antibiotic isolated from Nocardia uniformis [15]. The presence of the oxime moiety in this antibiotic makes it less stable to β-lactamases [16]. Modification of already existing antibiotics into oximes is a subject that has appeared in research over the years. Good examples of such modifications are those in cephalosporin antibiotics. Improvement of water solubility of oximes can be achieved by a modification of oxime moiety by attaining their ether and ester derivatives. Ceftobiprole medocaril (Figure 8b) is a fifth-generation cephalosporin antibiotic [17]. Prodrug of ceftobiprole with satisfactory water solubility is shown in (Figure 8a). It is a β-lactam antibacterial agent from one of the cepham series of cephalosporins. Its With the same method Abd-Ellah and coworkers tested 1,3,4-oxadiazole/oxime derivatives as a result on of the hybrids obtained 96.67% reduction in edema [14].

The Antimicrobial Activity
Cytotoxicity is one property of oximes; thus, oximes are therapeutic agents for bacterial, fungal and viral infections. Nocardicin A (Figure 7) is the first β-lactam antibiotic isolated from Nocardia uniformis [15]. The presence of the oxime moiety in this antibiotic makes it less stable to β-lactamases [16]. compared to indomethacin. Observed percentage of edema inhibition were 100%, 101% and 111% respectively [13]. With the same method Abd-Ellah and coworkers tested 1,3,4-oxadiazole/oxime derivatives as a result on of the hybrids obtained 96.67% reduction in edema [14].

The Antimicrobial Activity
Cytotoxicity is one property of oximes; thus, oximes are therapeutic agents for bacterial, fungal and viral infections. Nocardicin A (Figure 7) is the first β-lactam antibiotic isolated from Nocardia uniformis [15]. The presence of the oxime moiety in this antibiotic makes it less stable to β-lactamases [16]. Modification of already existing antibiotics into oximes is a subject that has appeared in research over the years. Good examples of such modifications are those in cephalosporin antibiotics. Improvement of water solubility of oximes can be achieved by a modification of oxime moiety by attaining their ether and ester derivatives. Ceftobiprole medocaril (Figure 8b) is a fifth-generation cephalosporin antibiotic [17]. Prodrug of ceftobiprole with satisfactory water solubility is shown in (Figure 8a). It is a β-lactam antibacterial agent from one of the cepham series of cephalosporins. Its antibacterial activity is connected with the ability to bind to penicillin-binding proteins (PBPs) [18].  Improvement of water solubility of oximes can be achieved by a modification of oxime moiety by attaining their ether and ester derivatives. Ceftobiprole medocaril ( Figure 8b) is a fifth-generation cephalosporin antibiotic [17]. Prodrug of ceftobiprole with satisfactory water solubility is shown in (Figure 8a). It is a β-lactam antibacterial agent from one of the cepham series of cephalosporins. Its antibacterial activity is connected with the ability to bind to penicillin-binding proteins (PBPs) [18]. Paulsen and colleagues synthetized (+)-N-6-hydroxyagelasine D, the enantiomer of a wellknown secondary metabolite from marine sponges-(−)-ageloxime D, [19]. The authors revealed that the previously proposed structures of (-)-ageloxime D extracted from a natural product [20] are in fact not an oxime, as the spectral data did not match. However, (-)-ageloxime can be obtained by a basic hydrolysis of agelasine D. (−)-Ageloxime D inhibits biofilm formation from Gram-positive bacteria Staphylococcus epidermis [19] but is unable to inhibit the growth of planktonic bacteria (MIC > 45 µM) [20]. Proposed (+)-N-6-hydroxyagelasine D bromide also possesses the ability to reduce biofilm formation of Staphylococcus epidermidis by 90% at 63 µM [19].
Many antimicrobial active compounds are modified to resemble oximes to increase their activity. The compound 5,7-dimethoxyflavone carbonyl was modified into an oxime, and this modification amplified its antifungal functions [21]. In their research, Min et al. synthesized new oxime esters that had antifungal activity. In addition, they also considered the E, Z stereoisomer substrates of 3-caren-5-one oxime (Figure 9a,b), which were separated for the first time. Both stereoisomers had relative inhibition rates above 50% against Physalospora piricola [22]. Paulsen and colleagues synthetized (+)-N-6-hydroxyagelasine D, the enantiomer of a well-known secondary metabolite from marine sponges-(−)-ageloxime D, [19]. The authors revealed that the previously proposed structures of (-)-ageloxime D extracted from a natural product [20] are in fact not an oxime, as the spectral data did not match. However, (-)-ageloxime can be obtained by a basic hydrolysis of agelasine D. (−)-Ageloxime D inhibits biofilm formation from Gram-positive bacteria Staphylococcus epidermis [19] but is unable to inhibit the growth of planktonic bacteria (MIC > 45 µM) [20]. Proposed (+)-N-6-hydroxyagelasine D bromide also possesses the ability to reduce biofilm formation of Staphylococcus epidermidis by 90% at 63 µM [19].
Many antimicrobial active compounds are modified to resemble oximes to increase their activity. The compound 5,7-dimethoxyflavone carbonyl was modified into an oxime, and this modification amplified its antifungal functions [21]. In their research, Min et al. synthesized new oxime esters that had antifungal activity. In addition, they also considered the E, Z stereoisomer substrates of 3-caren-5-one oxime (Figure 9a,b), which were separated for the first time. Both stereoisomers had relative inhibition rates above 50% against Physalospora piricola [22]. Synthetic naringenin, a flavonoid that naturally occurs in grapefruits, was modified to contain oximes by Kozłowska et al. Four derivatives have indicated to have antibacterial activity. The minimal inhibitory concentration (MIC) against Staphylococcus aureus was below 100 µg/mL. Two oximes ( Figure 10) showed MIC values against Staphylococcus aureus and Bacillus subtilis below 12.5 µg/mL [23]. In comparison to naringenin itself, which had no antimicrobial activity, the results obtained were satisfactory [24]. Synthetic naringenin, a flavonoid that naturally occurs in grapefruits, was modified to contain oximes by Kozłowska et al. Four derivatives have indicated to have antibacterial activity. The minimal inhibitory concentration (MIC) against Staphylococcus aureus was below 100 µg/mL. Two oximes ( Figure 10) showed MIC values against Staphylococcus aureus and Bacillus subtilis below 12.5 µg/mL [23]. In comparison to naringenin itself, which had no antimicrobial activity, the results obtained were satisfactory [24]. Additionally, Xu observed that in chalcone derivatives oxime moiety enhances antimicrobial activity [25]. The presence of oxime moiety in compound ( Figure 11b) resulted with a MIC value of ≤128 µg/mL [26] whereas compound ( Figure 11a) had a MIC value of 150 µg/mL [27] against B. subtilis. Similar difference was observed for both of compounds against A. niger obtained MIC values was 300 µg/mL [27] and ≤256 µg/mL (oxime) [26]. Additionally, Xu observed that in chalcone derivatives oxime moiety enhances antimicrobial activity [25]. The presence of oxime moiety in compound ( Figure 11b) resulted with a MIC value of ≤128 µg/mL [26] whereas compound ( Figure 11a) had a MIC value of 150 µg/mL [27] against B. subtilis. Similar difference was observed for both of compounds against A. niger obtained MIC values was 300 µg/mL [27] and ≤256 µg/mL (oxime) [26]. Additionally, Xu observed that in chalcone derivatives oxime moiety enhances antimicrobial activity [25]. The presence of oxime moiety in compound ( Figure 11b) resulted with a MIC value of ≤128 µg/mL [26] whereas compound ( Figure 11a) had a MIC value of 150 µg/mL [27] against B. subtilis. Similar difference was observed for both of compounds against A. niger obtained MIC values was 300 µg/mL [27] and ≤256 µg/mL (oxime) [26].    Additionally, Xu observed that in chalcone derivatives oxime moiety enhances antimicrobial activity [25]. The presence of oxime moiety in compound ( Figure 11b) resulted with a MIC value of ≤128 µg/mL [26] whereas compound ( Figure 11a) had a MIC value of 150 µg/mL [27] against B. subtilis. Similar difference was observed for both of compounds against A. niger obtained MIC values was 300 µg/mL [27] and ≤256 µg/mL (oxime) [26].    In vivo studies on mice have proven that indirubin-3 -oxime does not have a positive effect on survival and does not promote weight loss, despite that the reduction of expression and secretion of cytokine and chemokine is observed [30].
Chan et al. tested antiviral activity of indirubin-3′-oxime ( Figure 14) by the assessment of the infectious virus titers in epithelial cells and human macrophages. Viral replication was inhibited by about 10-fold in H5N1 virus-infected macrophages and ATIs by oxime compared to untreated cells. In the H1N1 treatment of virus-infected macrophages at 24 h post-infection, as well as in infected ATIs at 48 h post-infection similar results were observed. Additionally, viral matrix 1 protein expression in H5N1 virus-infected macrophages was effectively suppressed. In vivo studies on mice have proven that indirubin-3′-oxime does not have a positive effect on survival and does not promote weight loss, despite that the reduction of expression and secretion of cytokine and chemokine is observed [30].

The Antioxidant Activity
In addition to having anti-inflammatory activity, naringenin also revealed antioxidant properties. The modification of this compound into an oxime increased its antioxidant activity. The oxime is considered a radioprotector or an anticancer agent [31]. Another example of an oxime with a high antioxidant activity is an isoxanthohumol oxime ( Figure 15). This compound has a 200 times higher activity than isoxanthohumol, which is comparable to ascorbic acid [32]. Kaur et al. evaluated the content of Anethum graveolens L. essential oil and its relationship to its antioxidant activity. Five parameters were tested. The carvone oxime has indicated to have good radical scavenging activity. For the 2,2-diphenyl-1-picrylhydrazyl (DPPH) free radical the IC50 reached 0.31 mg/mL, for the hydroxyl radical the IC50 was 0.23 mg/mL and for the nitric oxide (NO) radical the IC50 was 0.31 mg/mL. The ferric reducing antioxidant power (FRAP) mean value was 196.88 mg/mL. The mean superoxide radical scavenging activity was 44.57 with an IC50 value of 0.31

The Antioxidant Activity
In addition to having anti-inflammatory activity, naringenin also revealed antioxidant properties. The modification of this compound into an oxime increased its antioxidant activity. The oxime is considered a radioprotector or an anticancer agent [31]. Another example of an oxime with a high antioxidant activity is an isoxanthohumol oxime ( Figure 15). This compound has a 200 times higher activity than isoxanthohumol, which is comparable to ascorbic acid [32].
Chan et al. tested antiviral activity of indirubin-3′-oxime ( Figure 14) by the assessment of the infectious virus titers in epithelial cells and human macrophages. Viral replication was inhibited by about 10-fold in H5N1 virus-infected macrophages and ATIs by oxime compared to untreated cells. In the H1N1 treatment of virus-infected macrophages at 24 h post-infection, as well as in infected ATIs at 48 h post-infection similar results were observed. Additionally, viral matrix 1 protein expression in H5N1 virus-infected macrophages was effectively suppressed. In vivo studies on mice have proven that indirubin-3′-oxime does not have a positive effect on survival and does not promote weight loss, despite that the reduction of expression and secretion of cytokine and chemokine is observed [30].

The Antioxidant Activity
In addition to having anti-inflammatory activity, naringenin also revealed antioxidant properties. The modification of this compound into an oxime increased its antioxidant activity. The oxime is considered a radioprotector or an anticancer agent [31]. Another example of an oxime with a high antioxidant activity is an isoxanthohumol oxime ( Figure 15). This compound has a 200 times higher activity than isoxanthohumol, which is comparable to ascorbic acid [32]. Kaur et al. evaluated the content of Anethum graveolens L. essential oil and its relationship to its antioxidant activity. Five parameters were tested. The carvone oxime has indicated to have good radical scavenging activity. For the 2,2-diphenyl-1-picrylhydrazyl (DPPH) free radical the IC50 reached 0.31 mg/mL, for the hydroxyl radical the IC50 was 0.23 mg/mL and for the nitric oxide (NO) radical the IC50 was 0.31 mg/mL. The ferric reducing antioxidant power (FRAP) mean value was 196.88 mg/mL. The mean superoxide radical scavenging activity was 44.57 with an IC50 value of 0.31 Kaur et al. evaluated the content of Anethum graveolens L. essential oil and its relationship to its antioxidant activity. Five parameters were tested. The carvone oxime has indicated to have good radical scavenging activity. For the 2,2-diphenyl-1-picrylhydrazyl (DPPH) free radical the IC 50 reached 0.31 mg/mL, for the hydroxyl radical the IC 50 was 0.23 mg/mL and for the nitric oxide (NO) radical the IC 50 was 0.31 mg/mL. The ferric reducing antioxidant power (FRAP) mean value was 196.88 mg/mL. The mean superoxide radical scavenging activity was 44.57 with an IC 50 value of 0.31 mg/mL [33]. Bandeira et al. proved that organotellurium oximes have promising radical scavenging activity. Against the DPPH radical both compounds presented in Figure 16 had IC 50 values of 5.12 ± 0.71 mg/mL and 7.79 ± 0.33 mg/mL, respectively. Both oximes have also been examined for their ability to reduce the 1-n-propyl-tetrazole complex with Fe 3+ (PTZ-Fe 3+ ) complex in 2,2 -azino-bis(3-ethylbenzothiazoline-6-sulfonic acid) (ABTS) radicals and FRAP. The results showed an antioxidant activity similar to that demonstrated by trolox. The first oxime had a capacity of approximately 8 mM TE/g (ABTS) and 11 mM TE/g (FRAP). The second oxime had a capacity of approximately 7 mM TE/g (ABTS) and 14 mM TE/g (FRAP), which were similar to the control quercetin [34].

The Anticancer Activity
Pregnenolone is an endogenic steroid and a precursor in the biosynthesis of steroid hormones. Pregnenolone was modified to a benzylidene oxime and two other. The derivatives were tested for against cancerous cells: colon (HT-29, HCT-15), central nervous system (SF-295), lungs (HOP-62, A-549) and breast (MCF-7). All of the derivatives showed promising anticancer properties [37]. The

The Anticancer Activity
Pregnenolone is an endogenic steroid and a precursor in the biosynthesis of steroid hormones. Pregnenolone was modified to a benzylidene oxime and two other. The derivatives were tested for against cancerous cells: colon (HT-29, HCT-15), central nervous system (SF-295), lungs (HOP-62, A-549) and breast (MCF-7). All of the derivatives showed promising anticancer properties [37]. The oxime presented in Figure 19 has a specific function as an inhibitor of kinases during the cell cycle and it also suppresses tumor growth. It was tested in liver cells (Hep G2) [38]. Symmetry 2020, 12, x FOR PEER REVIEW 10 of 17 oxime presented in Figure 19 has a specific function as an inhibitor of kinases during the cell cycle and it also suppresses tumor growth. It was tested in liver cells (Hep G2) [38]. Figure 19. Indirubin 3′oxime.
Other oximes that display anticancer activity are alkannin and shikonin derivatives. These modified compounds ( Figure 20) show no activity in healthy cells, but they are active in K562 leukemia cells [39].   (Figure 21a) inhibited the BRAF V600E gene mutation with an IC50 value of 0.9 µM. One of the oxime analogs (Figure 21c) presented excellent inhibitory activity to EGFR TK (IC50 of 0.07 µM). Moreover, all three compounds have been indicated to have dual roles as anticancer agents and MDR (multidrug resistance) reversal agents [40]. Additionally, Kozłowska et al. evaluated the cytotoxicity of naringenin derivatives in the human colon adenocarcinoma HT-29 cell line. The incorporation of the oxime group into one of the compounds allowed this compound to become a highly potent antiproliferative agent from a nonactive substrate. The oxime (Figure 10b) had an IC50 = 4.59 ± 0.56 µg/mL. Further, three other oximes revealed decreased IC50 value compared to the positive control, Other oximes that display anticancer activity are alkannin and shikonin derivatives. These modified compounds (Figure 20) show no activity in healthy cells, but they are active in K562 leukemia cells [39].
Symmetry 2020, 12, x FOR PEER REVIEW 10 of 17 oxime presented in Figure 19 has a specific function as an inhibitor of kinases during the cell cycle and it also suppresses tumor growth. It was tested in liver cells (Hep G2) [38]. Figure 19. Indirubin 3′oxime.
Other oximes that display anticancer activity are alkannin and shikonin derivatives. These modified compounds (Figure 20) show no activity in healthy cells, but they are active in K562 leukemia cells [39].    Figure 19 has a specific function as an inhibitor of kinases during the cell cycle and it also suppresses tumor growth. It was tested in liver cells (Hep G2) [38]. Figure 19. Indirubin 3′oxime.
Other oximes that display anticancer activity are alkannin and shikonin derivatives. These modified compounds (Figure 20) show no activity in healthy cells, but they are active in K562 leukemia cells [39].  Significant antiproliferative activity was presented by one of the oxime compounds (Figure 21c) against the PANC-1, A-549, PaCa-2 and PC-3 cell lines, achieving IC50 value of 0.02 µM. Another compound (Figure 21a) inhibited the BRAF V600E gene mutation with an IC50 value of 0.9 µM. One of the oxime analogs (Figure 21c) presented excellent inhibitory activity to EGFR TK (IC50 of 0.07 µM). Moreover, all three compounds have been indicated to have dual roles as anticancer agents and MDR (multidrug resistance) reversal agents [40]. Additionally, Kozłowska et al. evaluated the cytotoxicity of naringenin derivatives in the human colon adenocarcinoma HT-29 cell line. The incorporation of the oxime group into one of the compounds allowed this compound to become a highly potent antiproliferative agent from a nonactive substrate. The oxime (Figure 10b) had an IC50 = 4.59 ± 0.56 µg/mL. Further, three other oximes revealed decreased IC50 value compared to the positive control, Moreover, all three compounds have been indicated to have dual roles as anticancer agents and MDR (multidrug resistance) reversal agents [40]. Additionally, Kozłowska et al. evaluated the cytotoxicity of naringenin derivatives in the human colon adenocarcinoma HT-29 cell line. The incorporation of the oxime group into one of the compounds allowed this compound to become a highly potent antiproliferative agent from a nonactive substrate. The oxime (Figure 10b) had an IC 50 = 4.59 ± 0.56 µg/mL. Further, three other oximes revealed decreased IC 50 value compared to the positive control, cisplatin and were a bit weaker than the cytostatic antibiotic, doxorubicin [23]. Zha et al. synthesized α,β-unsaturated carbonyl-based oximes containing ligustrazine moiety. Those compounds strongly inhibited growth of five cancer cell types, A-549, PC-3, MCF-7, PaCa-2 and HT-29. The best activity, as an inhibitor of tubulin polymerization, BRAF V600E , focal adhesion kinase (FAK) and EGFR-TK, was displayed by the oxime shown in Figure 22 [41].
Symmetry 2020, 12, x FOR PEER REVIEW 11 of 17 cisplatin and were a bit weaker than the cytostatic antibiotic, doxorubicin [23]. Zha et al. synthesized α,β-unsaturated carbonyl-based oximes containing ligustrazine moiety. Those compounds strongly inhibited growth of five cancer cell types, A-549, PC-3, MCF-7, PaCa-2 and HT-29. The best activity, as an inhibitor of tubulin polymerization, BRAF V600E , focal adhesion kinase (FAK) and EGFR-TK, was displayed by the oxime shown in Figure 22 [41]. Often, oximes are more polar than their baseline molecules [42]. Griseofulvin oxime derivatives proved to have improved anticancer activity than the baseline molecule. Presence of the oxime moiety at the 4′ position improved the potency 2-fold to 12 µM [43].

A counteractive Agent to Organophosphorus Compound Poisoning
Poisoning from organophosphorus (OP) compounds is a very large therapeutic problem, especially from pesticides and substances that pose serious danger to the nervous system. Treating of OP-poisoning depends on the type of nerve agent, which can distinguish the G-type and V-type according to volatility [44]. Additionally it is proven that the location of the oxime moiety is the most important for the capacity of reversing different OP inhibitors effect [45]. There are two therapeutic agents used in OP poisoning: pralidoxime and obidoxime (Figure 23a,b), which are applied as reactivators of OP-inhibited acetylcholinesterase (AChE) in the presence of reversible antagonists of a muscarinic receptor, such as, for example, atropine [44]. Recently, pralidoxime was tested in vivo for its tissue and blood distribution profiles in nonintoxicated rats. The considerable uptake was observed in the kidney and quite lower rates were observed in the liver, lung and heart, with lesser amounts in the brain and blood [46]. Another three promising oxime drugs are asoxime dichloride, trimedoxime dibromide and methoximedichloride, which were synthesized in the previous century [44]. Wilhelm et al. tested reactivators on OP-poisoned guinea pigs. Methoximedichloride is efficacious against broad spectrum of OP (soman, tabun, cyclosarin, sarin and VX, and the chlorpyrifos oxon, pesticides paraoxon and phorate oxon) in case of 24-h survivability in equimolar dose (146 µmol/kg). Asoxime dichloride was also active but on the second tier, trimedoxime dibromide as the toxic compound was tested in a dose of 35 µmol/kg and offered survival protection between the second and third tier [47]. Costa et al. proposed two new oximes (Figure 23c,d) to reactivate human AChE and butyrylcholinesterase (BChE) that has been inhibited by organophosphate compounds, mainly the inhibitory activity of three OPs: chlorpyrifos, diazinon and malathion [48]. Unfortunately, oximes are mostly useless against soman poisoning [49]. Often, oximes are more polar than their baseline molecules [42]. Griseofulvin oxime derivatives proved to have improved anticancer activity than the baseline molecule. Presence of the oxime moiety at the 4 position improved the potency 2-fold to 12 µM [43].

A Counteractive Agent to Organophosphorus Compound Poisoning
Poisoning from organophosphorus (OP) compounds is a very large therapeutic problem, especially from pesticides and substances that pose serious danger to the nervous system. Treating of OP-poisoning depends on the type of nerve agent, which can distinguish the G-type and V-type according to volatility [44]. Additionally it is proven that the location of the oxime moiety is the most important for the capacity of reversing different OP inhibitors effect [45]. There are two therapeutic agents used in OP poisoning: pralidoxime and obidoxime (Figure 23a,b), which are applied as reactivators of OP-inhibited acetylcholinesterase (AChE) in the presence of reversible antagonists of a muscarinic receptor, such as, for example, atropine [44]. Recently, pralidoxime was tested in vivo for its tissue and blood distribution profiles in nonintoxicated rats. The considerable uptake was observed in the kidney and quite lower rates were observed in the liver, lung and heart, with lesser amounts in the brain and blood [46]. Another three promising oxime drugs are asoxime dichloride, trimedoxime dibromide and methoximedichloride, which were synthesized in the previous century [44]. Wilhelm et al. tested reactivators on OP-poisoned guinea pigs. Methoximedichloride is efficacious against broad spectrum of OP (soman, tabun, cyclosarin, sarin and VX, and the chlorpyrifos oxon, pesticides paraoxon and phorate oxon) in case of 24-h survivability in equimolar dose (146 µmol/kg). Asoxime dichloride was also active but on the second tier, trimedoxime dibromide as the toxic compound was tested in a dose of 35 µmol/kg and offered survival protection between the second and third tier [47]. Costa et al. proposed two new oximes (Figure 23c,d) to reactivate human AChE and butyrylcholinesterase (BChE) that has been inhibited by organophosphate compounds, mainly the inhibitory activity of three OPs: chlorpyrifos, diazinon and malathion [48]. Unfortunately, oximes are mostly useless against soman poisoning [49]. The oxime presented in Figure 23c reached a percent (%) reactivation ± SEM at a concentration of 1 µM of 10 ± 0.016, and in Figure 23d showed a value of 7 ± 0.009 against chlorpyrifos. The oxime presented in Figure 23b had a percent (%) reactivation ± SEM at a concentration of 1 µM of 20 ± 0.010, and shown in Figure 23b oxime 2 showed a value of 12 ± 0.025 against the second OP. The oxime presented in Figure 23d had percent (%) reactivation ± SEM at a concentration of 1 µM of 5 ± 0.012, and the oxime shown in Figure 23d showed a value of 12 ± 0.019 against the third OP. The oximes shown in Figure 23c,d had similar activity to pralidoxime: oxime (Figure 23c) had the same percent reactivation against diazinon poisoning as obidoxime [48]. Žunec et al. presented their in vivo research on new therapeutic agents against paraoxon poisoning. Two oximes presented in Figure 24, stood out for their low acute toxicities and excellent antidotal effects. Oximes have been applied in male mice in the amount of 5% of their lethal dose (LD50) and combined with atropine, resulting in a protection index (PI) of 74.1 and 100, respectively. Moreover, the use of these combinations increased the survival of all animals up to 63.0 of the LD50 of paraoxon. Both oximes might be good antidotes for OP poisoning. Moreover, both monoximes are the least toxic among all tested. The LD50 of oxime presented in Figure 24a was 672.8 mg/kg [50]. Kuca et al. presented their research results on trisquarternary bisoxime as a potential drug against OP poisoning. Unfortunately, it cannot be considered an AChE reactivator because the rate of reactivation of AChE was worse than for standard reactivators. The oxime shown in Figure 25 has indicated to reactivate AChE after inhibition by sarin and agent VX with a percent reactivation above 20% at high concentrations (10-3 M). Moreover, this compound will not penetrate the blood-brain barrier due to three positive charges. However, the high hydrophilicity and relatively large size of the studied bisoxime reactivator makes it an interesting candidate for BChE pseudocatalytic reactivation [51]. The oxime presented in Figure 23c reached a percent (%) reactivation ± SEM at a concentration of 1 µM of 10 ± 0.016, and in Figure 23d showed a value of 7 ± 0.009 against chlorpyrifos. The oxime presented in Figure 23b had a percent (%) reactivation ± SEM at a concentration of 1 µM of 20 ± 0.010, and shown in Figure 23b oxime 2 showed a value of 12 ± 0.025 against the second OP. The oxime presented in Figure 23d had percent (%) reactivation ± SEM at a concentration of 1 µM of 5 ± 0.012, and the oxime shown in Figure 23d showed a value of 12 ± 0.019 against the third OP. The oximes shown in Figure 23c,d had similar activity to pralidoxime: oxime (Figure 23c) had the same percent reactivation against diazinon poisoning as obidoxime [48]. Žunec et al. presented their in vivo research on new therapeutic agents against paraoxon poisoning. Two oximes presented in Figure 24, stood out for their low acute toxicities and excellent antidotal effects. The oxime presented in Figure 23c reached a percent (%) reactivation ± SEM at a concentration of 1 µM of 10 ± 0.016, and in Figure 23d showed a value of 7 ± 0.009 against chlorpyrifos. The oxime presented in Figure 23b had a percent (%) reactivation ± SEM at a concentration of 1 µM of 20 ± 0.010, and shown in Figure 23b oxime 2 showed a value of 12 ± 0.025 against the second OP. The oxime presented in Figure 23d had percent (%) reactivation ± SEM at a concentration of 1 µM of 5 ± 0.012, and the oxime shown in Figure 23d showed a value of 12 ± 0.019 against the third OP. The oximes shown in Figure 23c,d had similar activity to pralidoxime: oxime (Figure 23c) had the same percent reactivation against diazinon poisoning as obidoxime [48]. Žunec et al. presented their in vivo research on new therapeutic agents against paraoxon poisoning. Two oximes presented in Figure 24, stood out for their low acute toxicities and excellent antidotal effects. Oximes have been applied in male mice in the amount of 5% of their lethal dose (LD50) and combined with atropine, resulting in a protection index (PI) of 74.1 and 100, respectively. Moreover, the use of these combinations increased the survival of all animals up to 63.0 of the LD50 of paraoxon. Both oximes might be good antidotes for OP poisoning. Moreover, both monoximes are the least toxic among all tested. The LD50 of oxime presented in Figure 24a was 672.8 mg/kg [50]. Kuca et al. presented their research results on trisquarternary bisoxime as a potential drug against OP poisoning. Unfortunately, it cannot be considered an AChE reactivator because the rate of reactivation of AChE was worse than for standard reactivators. The oxime shown in Figure 25 has indicated to reactivate AChE after inhibition by sarin and agent VX with a percent reactivation above 20% at high concentrations (10-3 M). Moreover, this compound will not penetrate the blood-brain barrier due to three positive charges. However, the high hydrophilicity and relatively large size of the studied bisoxime reactivator makes it an interesting candidate for BChE pseudocatalytic reactivation [51]. Oximes have been applied in male mice in the amount of 5% of their lethal dose (LD 50 ) and combined with atropine, resulting in a protection index (PI) of 74.1 and 100, respectively. Moreover, the use of these combinations increased the survival of all animals up to 63.0 of the LD 50 of paraoxon. Both oximes might be good antidotes for OP poisoning. Moreover, both monoximes are the least toxic among all tested. The LD 50 of oxime presented in Figure 24a was 672.8 mg/kg [50]. Kuca et al. presented their research results on trisquarternary bisoxime as a potential drug against OP poisoning. Unfortunately, it cannot be considered an AChE reactivator because the rate of reactivation of AChE was worse than for standard reactivators. The oxime shown in Figure 25 has indicated to reactivate AChE after inhibition by sarin and agent VX with a percent reactivation above 20% at high concentrations (10-3 M). Moreover, this compound will not penetrate the blood-brain barrier due to three positive charges. However, the high hydrophilicity and relatively large size of the studied bisoxime reactivator makes it an interesting candidate for BChE pseudocatalytic reactivation [51]. Another approach was presented by Santoni and colleagues. They synthesized a tetrahydroacridine linked to the non-quaternary oxime reactivator presented in Figure 26 and a chlorinated derivative. Both molecules proved to have excellent nerve agent antidote efficacy (kr2 reactivation), better than the well-known drug obidoxime against three OPs: agent VX, sarin and paraoxon [52].  (Figure 27a,b) that proved to have notable potential in cyclosarin poisoning especially in reversing hBChE blockage. Moreover, both oximes have been predicted to cross the blood-brain barrier at satisfactory levels. [53]. An active compound able to reverse OP poisoning was presented by Kovarik et al. The best results in the in vivo study were obtained against agent VX and paraoxon. The compound shown in Figure 28 proved to have the greatest antidotal potential with a PI above 10 and ensured mouse survival against 10× the LD50. Moreover, this oxime proved to have a better PI against tabun poisoning than the other commonly known drug, trimedoxime bromide. No significant cytotoxicity was observed [54]. Another approach was presented by Santoni and colleagues. They synthesized a tetrahydroacridine linked to the non-quaternary oxime reactivator presented in Figure 26 and a chlorinated derivative. Both molecules proved to have excellent nerve agent antidote efficacy (kr2 reactivation), better than the well-known drug obidoxime against three OPs: agent VX, sarin and paraoxon [52]. Another approach was presented by Santoni and colleagues. They synthesized a tetrahydroacridine linked to the non-quaternary oxime reactivator presented in Figure 26 and a chlorinated derivative. Both molecules proved to have excellent nerve agent antidote efficacy (kr2 reactivation), better than the well-known drug obidoxime against three OPs: agent VX, sarin and paraoxon [52].  (Figure 27a,b) that proved to have notable potential in cyclosarin poisoning especially in reversing hBChE blockage. Moreover, both oximes have been predicted to cross the blood-brain barrier at satisfactory levels. [53]. An active compound able to reverse OP poisoning was presented by Kovarik et al. The best results in the in vivo study were obtained against agent VX and paraoxon. The compound shown in Figure 28 proved to have the greatest antidotal potential with a PI above 10 and ensured mouse survival against 10× the LD50. Moreover, this oxime proved to have a better PI against tabun poisoning than the other commonly known drug, trimedoxime bromide. No significant cytotoxicity was observed [54].  (Figure 27a,b) that proved to have notable potential in cyclosarin poisoning especially in reversing hBChE blockage. Moreover, both oximes have been predicted to cross the blood-brain barrier at satisfactory levels. [53]. Another approach was presented by Santoni and colleagues. They synthesized a tetrahydroacridine linked to the non-quaternary oxime reactivator presented in Figure 26 and a chlorinated derivative. Both molecules proved to have excellent nerve agent antidote efficacy (kr2 reactivation), better than the well-known drug obidoxime against three OPs: agent VX, sarin and paraoxon [52].  (Figure 27a,b) that proved to have notable potential in cyclosarin poisoning especially in reversing hBChE blockage. Moreover, both oximes have been predicted to cross the blood-brain barrier at satisfactory levels. [53]. An active compound able to reverse OP poisoning was presented by Kovarik et al. The best results in the in vivo study were obtained against agent VX and paraoxon. The compound shown in Figure 28 proved to have the greatest antidotal potential with a PI above 10 and ensured mouse survival against 10× the LD50. Moreover, this oxime proved to have a better PI against tabun poisoning than the other commonly known drug, trimedoxime bromide. No significant cytotoxicity was observed [54]. An active compound able to reverse OP poisoning was presented by Kovarik et al. The best results in the in vivo study were obtained against agent VX and paraoxon. The compound shown in Figure 28 proved to have the greatest antidotal potential with a PI above 10 and ensured mouse survival against 10× the LD 50 . Moreover, this oxime proved to have a better PI against tabun poisoning than the other commonly known drug, trimedoxime bromide. No significant cytotoxicity was observed [54].

Conclusions
In conclusion, oximes were indicated to have a therapeutic potential. Some have already been used as drugs for OP poisoning and antibiotics. Many newly synthesized oximes have shown promising properties, such as antimicrobial, anti-inflammatory, antioxidant, anticancer and against OP poisoning. Consequently, further studies on oximes and their biological activities should be undertaken to determine more active agents that might be considered as effective drugs.