Results in Chemistry of Natural Organic Compounds. Synthesis of New Anticancer Vinca Alkaloids and Flavone Alkaloids

: The antitumor indole–indoline alkaloids of the evergreen Catharanthus roseus —namely vinblastine and vincristine—are widely used in chemotherapy of cancer. Many efforts were made to synthesize more efficient derivatives with less side-effect. The 14,15-cyclopropane derivative of vinblastine was synthesized successfully by a five-step procedure starting from vindoline. Vincristine, vinorelbine and several derivatives condensed with a cyclopropane ring were synthesized. Various hybrid molecules were prepared by the coupling reaction of vindoline and methyl ester of tryptophan, which were conjugated by carrier peptides of octaarginine. Studying the halogenation reactions of vindoline and catharanthine some fluorine derivatives were obtained which showed promising antitumor activity on various tumor types. The synthesis of the Aspidospermane alkaloid bannucine and 5 (cid:48) -epibannucine were carried out using N -acyliminium intermediates. The same intermediate was also applied in the first synthesis of sessiline. The research group have synthesized of flavonoid alkaloids: dracocephins A and B. Further three flavonoid alkaloids, namely 8-(2”-pyrrolidinon-5 (cid:48)(cid:48) -yl)quercetin, 6-(2 (cid:48)(cid:48) -pyrrolidinon-5 (cid:48)(cid:48) -yl)-( − )-and 8-(2 (cid:48)(cid:48) -pyrrolidinon-5 (cid:48)(cid:48) -yl)-( − )-epicatechin were prepared by acid-catalyzed regioselective Mannich reaction starting from the corresponding flavonoid precursor. Vindoline was also coupled to synthetic pharmacophores, such as triphenylphosphine and various N -heterocycles. Some of these hybrid molecules showed significant antitumor activity. Furthermore, 7-OH and 7-NH modified flavonoid derivatives were synthesized by a regioselective alkylation followed by Smiles rearrangement and hydrolysis.

to Madagascar. These compounds are antitumor agents and are used in anticancer therapy. During cell division they act as inhibitors of tubulin polymerization thus blocking the formation of mitotic spindle. In the cancer cells they also inhibit the DNS repairing mechanism and the synthesis of RNS, inhibiting the DNS-dependent RNS polymerase. In anticancer therapy, these types of compounds are used especially against leukemia and lymphoma.
Chemistry 2020, 2, x 2 formyl group (Figure 1) instead of a methyl group as is in the vinblastine (3). These compounds can be classified as Vinca alkaloids, which were isolated first in the 1950s from the periwinkle Catharanthus roseus being native to Madagascar. These compounds are antitumor agents and are used in anticancer therapy. During cell division they act as inhibitors of tubulin polymerization thus blocking the formation of mitotic spindle. In the cancer cells they also inhibit the DNS repairing mechanism and the synthesis of RNS, inhibiting the DNS-dependent RNS polymerase. In anticancer therapy, these types of compounds are used especially against leukemia and lymphoma. In the literature, there are many publication in connection of chemical and biologic feature of vinblastine (3) and vincristine (4) as well as synthesis of their new derivatives having important biologic activity [1][2][3]. Moreover, in the course of our research work, the purpose was not only the synthesis of new vinblastine (3) and vincristine (4) derivatives, but also the extensive investigation of the chemistry of their monomers vindoline (1) and catharanthine (2). In 2015, a detailed review was published presenting the most important results obtained by our research group in this area [4].
Flavonoids are secondary plant metabolites containing numerous low-molecular-weight members [5,6]. Their general structure consists of a 15-carbon skeleton with a heterocyclic (pyran) ring (C) between two phenyl rings (A and B) ( Figure 2). Flavonoids have a broad-spectrum of biologic activity including anti-inflammatory [7,8], antiviral [8][9][10], antioxidant [11,12] and antitumor [5,8] effects. Flavonoids have been found to be able to dock into ATP binding sites using the adenosine like part at position 4 and 5 [13].  In the literature, there are many publication in connection of chemical and biologic feature of vinblastine (3) and vincristine (4) as well as synthesis of their new derivatives having important biologic activity [1][2][3]. Moreover, in the course of our research work, the purpose was not only the synthesis of new vinblastine (3) and vincristine (4) derivatives, but also the extensive investigation of the chemistry of their monomers vindoline (1) and catharanthine (2). In 2015, a detailed review was published presenting the most important results obtained by our research group in this area [4].

Derivatives Condensed the Three-Membered Rings
Flavonoids are secondary plant metabolites containing numerous low-molecular-weight members [5,6]. Their general structure consists of a 15-carbon skeleton with a heterocyclic (pyran) ring (C) between two phenyl rings (A and B) ( Figure 2). Flavonoids have a broad-spectrum of biologic activity including anti-inflammatory [7,8], antiviral [8][9][10], antioxidant [11,12] and antitumor [5,8] effects. Flavonoids have been found to be able to dock into ATP binding sites using the adenosine like part at position 4 and 5 [13]. terature, there are many publication in connection of chemical and biolog 3) and vincristine (4) as well as synthesis of their new derivatives havin ity [1][2][3]. Moreover, in the course of our research work, the purpose was ew vinblastine (3) and vincristine (4) derivatives, but also the extensive inv of their monomers vindoline (1) and catharanthine (2). In 2015, a detailed esenting the most important results obtained by our research group in this ids are secondary plant metabolites containing numerous low-molec ]. Their general structure consists of a 15-carbon skeleton with a heterocy een two phenyl rings (A and B) ( Figure 2). Flavonoids have a broad-spectrum ding anti-inflammatory [7,8], antiviral [8][9][10], antioxidant [11,12] and ant noids have been found to be able to dock into ATP binding sites using th osition 4 and 5 [13].

Derivatives Condensed the Three-Membered Rings
It was observed recently that the saturation of the carbon-carbon double bond in position 14,15 of vinblastine (3) by catalytic hydrogenation decreased the biologic effect almost with two orders of magnitude [14]. Considering the drastic change in the biologic activity of this rather large molecule was caused by a minor structural modification; it can be concluded that this C=C double bond has an important role in the biologic effect. Since that, these compounds can be seen appropriate for cyclopropanation, the question is coming up, how the biologic activities change in the case of replacing this double bond with cyclopropane ring having a similar electron structure. This was the reason to propose the synthesis of new vinblastine derivatives condensed with cyclopropane ring in position 14,15. Cyclopropane skeletons can be found in several molecules-as well as in natural organic compounds in a condensed form or as substituents [15]. Nevertheless, the cyclopropane ring has specific properties thanks to its unique structure. Based on the NMR spectra of the different cyclopropane derivatives, it can be concluded that the C-H bond in the cyclopropane ring has larger s-character than in other hydrocarbons. This is the reason, however, that the C-C bonds have larger p-character. It was calculated that the s-character of these C-C bonds is not more than 17%, so that it corresponds to the special sp 5 hybrid state. This is supported by the C-C coupling constants measured in the 13 C-NMR spectra of cyclopropane derivatives [16].
The 1 H-NMR shifts of some cyclopropane derivatives are also interesting [17,18]. It can be observed that the chemical shift is slightly increased in the case of the possibility of conjugation, however, development of an aromatic character causes an enormous increase in the chemical shift, e.g., the value of cyclopentadiene-spiro-cyclopropane changes almost fourfold compared to the saturated cyclopentane-spirocyclopropane. Thus, one of cyclopropane ring can give two electrons to form the aromatic delocalized electron sextet.
X-ray crystallographic investigations confirmed that the C-C bonds in cyclopropane are shorter than usual in the normally saturated analogs and show slight diffraction because of the large strain of the cyclopropane ring [19]. Therefore, the classical valence theories in the case of cyclopropane can be hardly used. Moreover, how it changes the biologic activity?
Many methods can be offered for the preparation of cyclopropane derivatives. Of these, the classic Simmons-Smith reaction exceeds, in which the carbene unit is given by diethyl zinc [20].
At first, the direct cyclopropanation of vinblastine (3) was tried. However, it failed using known procedures. Then the monomer vindoline (1) was treated with diethylzinc and diiodomethane, protecting the position 10 of vindoline (1) with a bromine substituent for avoiding the dimerization reaction taking place through the diiodomethane. Hence, thus, we succeeded in the synthesis of the desired 14,15-cyclopropanovinblastine (10) in an indirect way by a 5-step synthesis [4,[21][22][23].
Dimer alkaloids condensed with a cyclopropane ring synthesized by us were investigated by the National Institute of Health (NIH, Bethesda, MD, USA) on 60 different cell lines of 9 different tumor types.
The cytostatic activity of compounds 14,15-cyclopropanovinblastine (10) and 14,15-cyclopropanovincristine (11)slightlydiffersfromvinblastine(3)andvincristine(4)usedintherapyasanticancermedicines; thecyclopropane analogs are more effective inhibitors for the cell proliferation, respectively and destroy the tumorous cells with more efficiency. The 14,15-cyclopropanovinblastine (10) shows excellent anticancer activity in the case of leukemia, non-small cell lung cancer, colon cancer, melanoma and breast cancer, the vincristine derivative (11) is outstanding against colon cancer, melanoma, ovarian cancer and prostate cancer. From the vinorelbine derivatives, the 14,15-cyclopropanovinorelbine (12) has the most significant effect in the case of non-small cell lung cancer, colon cancer, central nervous system cancers, melanoma and breast cancer.

Vinca Hybrid Molecules Containing Amino Acid Esters
In the last few years, there was great interest in the hybrid molecules. Among anticancer compounds, some hybrid molecules were built by coupling an antiproliferative structural part with another pharmacophore. From our compounds at first vindoline (1) was coupled with amino acid esters [26].
10-bromovindoline (6) was treated with hydrazine resulting in 15a hydrazide derivative and the latter was coupled with (l)-and (d)-tryptophan methyl ester, respectively, by means of azide coupling method known in peptide chemistry ( Figure 5). Different derivatives of vindoline (1) were used: 14,15-dihydro-, 14,15-cyclopropanovindoline, moreover, the derivatives not containing a bromo substituent at position 10 were also synthesized. The cytostatic activity of the prepared compounds (17a-l) was investigated on HL-60 leukemia cells. It was established, that the most effective molecule was compound 17f, which has hydrogen atom at C-10 and is coupled with (l)-tryptophan methyl ester at position 16. Derivatives of vinblastine (3) coupled also with (l)-tryptophan methyl ester, conjugated with N-terminal of octaarginine carrier peptide after hydrolysis of the ester to the corresponding carboxylic acid showed substantially larger activity [27].

Vinca Hybrid Molecules Containing Steroid Vectors
The conjugation of Vinca alkaloids with (l)-and (d)-tryptophan methyl ester proved that the cytotoxic effect of vindoline (1) can be promoted by coupling this monomer with suitable pharmacophores. As a continuation of our work we aimed to synthesize vindoline (1) steroid hybrids presuming that the lipophilic steroid vector can facilitate Vinca alkaloids to pass through the cell membranes and reach higher bioavailability. Accordingly, 5α-dihydrotestosterone and 19-nortestosterone were connected to vindoline (1) in positions 10 and 17 through succinate linkers. From the successfully synthesized four new hybrid derivatives, the most efficient one was compound 18, where 19-nortestosterone was coupled with vindoline (1) in position 17 ( Figure 6) [28]. According to the in vitro biologic evaluations of NIH (USA), compound 18 displayed increased cell growth inhibition than vindoline (1), furthermore, it showed a higher antitumor effect on several cell lines even than vinblastine (3) sulfate used in therapy.

Vinca Hybrid Molecules Containing Synthetic Pharmacophores
After the encouraging results derived from the conjugation of natural pharmacophores (amino acid esters and steroids) and Vinca alkaloids, our next research project was to combine vindoline (1) with well-known synthetic pharmacophores for example triphenylphosphine and certain N-heterocycles such as morpholine, piperazine and N-methylpiperazine. These moieties are widely used pharmacophores in modern drug discovery and proved to be efficient structural units of several drugs on market [29,30]. Our main purpose was still the same: producing new vindoline hybrid molecules which could have potential anticancer activity. First, vindoline (1) was O-acylated with 4-bromobutyric acid, after hydrolysis in position 17. After this step, the linker-containing vindoline derivative (19) was successfully coupled with the mentioned synthetic pharmacophores to give the expected hybrid molecules (20)(21)(22)(23) (Figure 7) [31][32][33].

Vinca Hybrid Molecules Containing Steroid Vectors
The conjugation of Vinca alkaloids with (L)-and (D)-tryptophan methyl ester proved that the cytotoxic effect of vindoline (1) can be promoted by coupling this monomer with suitable pharmacophores. As a continuation of our work we aimed to synthesize vindoline (1) steroid hybrids presuming that the lipophilic steroid vector can facilitate Vinca alkaloids to pass through the cell membranes and reach higher bioavailability. Accordingly, 5α-dihydrotestosterone and 19nortestosterone were connected to vindoline (1) in positions 10 and 17 through succinate linkers. From the successfully synthesized four new hybrid derivatives, the most efficient one was compound 18, where 19-nortestosterone was coupled with vindoline (1) in position 17 ( Figure 6) [28]. According to the in vitro biologic evaluations of NIH (USA), compound 18 displayed increased cell growth inhibition than vindoline (1), furthermore, it showed a higher antitumor effect on several cell lines even than vinblastine (3) sulfate used in therapy.

Vinca Hybrid Molecules Containing Steroid Vectors
The conjugation of Vinca alkaloids with (L)-and (D)-tryptophan methyl ester proved that the cytotoxic effect of vindoline (1) can be promoted by coupling this monomer with suitable pharmacophores. As a continuation of our work we aimed to synthesize vindoline (1) steroid hybrids presuming that the lipophilic steroid vector can facilitate Vinca alkaloids to pass through the cell membranes and reach higher bioavailability. Accordingly, 5α-dihydrotestosterone and 19nortestosterone were connected to vindoline (1) in positions 10 and 17 through succinate linkers. From the successfully synthesized four new hybrid derivatives, the most efficient one was compound 18, where 19-nortestosterone was coupled with vindoline (1) in position 17 ( Figure 6) [28]. According to the in vitro biologic evaluations of NIH (USA), compound 18 displayed increased cell growth inhibition than vindoline (1), furthermore, it showed a higher antitumor effect on several cell lines even than vinblastine (3) sulfate used in therapy.  used pharmacophores in modern drug discovery and proved to be efficient structural units of several drugs on market [29,30]. Our main purpose was still the same: producing new vindoline hybrid molecules which could have potential anticancer activity. First, vindoline (1) was O-acylated with 4bromobutyric acid, after hydrolysis in position 17. After this step, the linker-containing vindoline derivative (19) was successfully coupled with the mentioned synthetic pharmacophores to give the expected hybrid molecules (20)(21)(22)(23) (Figure 7) [31][32][33].  The new compounds (20-23) were tested on 60 different human tumor cell lines in vitro (NIH, Bethesda, MD, USA). The results showed that the linker, the morpholine, and the N-methylpiperazine moieties could not improve the anticancer activity of vindoline (1). However, the 20 phosphonium-salt and the 22-vindoline dimer (containing piperazine) represented outstanding cytotoxic activities. These derivatives (20,22) were more potent than vinblastine (3) sulfate itself on several cell lines. The anticancer investigation (NIH, USA) of these compounds (19)(20)(21)(22)(23) confirmed our hypothesis suggesting vindoline (1) can become an effective anticancer drug by conjugating it with suitable pharmacophores.

Halogenation Reactions of VINCA Alkaloids
The mechanism of the cyclopropanation reaction of vinblastine (3) presented in chapter 2.1. was investigated and established the reason for forming the N-methyl quaternary salt of vinblastine instead of cyclopropanation in the course of Simmons-Smith reaction [34].
Halogenation reactions of monomer indole alkaloids vindoline (1) and catharanthine (2) were studied in detail, first of all the introduction of fluorine atom was investigated (Figure 8). In both cases the reactions resulted in unexpected products. Thus, in the case of vindoline (1) the fluoro containing quinone derivative (24) was formed and, in the case of catharanthine (2) a fluoro substituted indolenine (25) could be isolated [35].
Halogenation reactions of monomer indole alkaloids vindoline (1) and catharanthine (2) were studied in detail, first of all the introduction of fluorine atom was investigated (Figure 8). In both cases the reactions resulted in unexpected products. Thus, in the case of vindoline (1) the fluoro containing quinone derivative (24) was formed and, in the case of catharanthine (2) a fluoro substituted indolenine (25) could be isolated [35].

Vindoline and Flavone Derivatives Containing 2-Pyrrolidone Ring
Our other important research area was the chemistry of Aspidospermane alkaloids. A detailed review was published in 2008 by us presenting the synthesis and derivatives of these types of alkaloids [36]. Then the first synthesis of bannucine (26) and 5′-epibannucine (27) was elaborated [37]. This alkaloid was first isolated in 1986 from the leaves of Catharanthus roseus by Atta-Ur-Rahman and coworkers [38]. Bannucine (26) is a derivative of vindoline (1) having a 2-pyrrolidone ring in position 10. The key step of the procedure appears the reaction between the natural (−)-vindoline (1) and a cyclic N-acyliminium intermediate. As a result of the reaction not only the bannucine (26), but also its 5′-epimeric isomer (27) was formed in an approximate ratio of 2:3 ( Figure 9). The isomers were separated, and their structure was identified also by X-ray crystallography. The pure epimers were investigated on 57 cell lines of different types of cancer, however, important anticancer activity was not found [36]. The first synthesis of sessiline (30) was achieved by applying the experiences gained in the field of acylaminocarbinols [39]. The alkaloid sessiline (30) was isolated from the fruits of Acanthopanas sessiliflorus in 2002 [40]. The molecule consists of two 5-membered heterocycles coupling through an acylaminocarbinol ether-type bond ( Figure 10). Sessiline (30) was prepared by reaction of 5hydroxypyrrolidin-2-one (28) with 5-hydroxymethyl-furfural (29) at 60 °C with 54% yield [39].

Vindoline and Flavone Derivatives Containing 2-Pyrrolidone Ring
Our other important research area was the chemistry of Aspidospermane alkaloids. A detailed review was published in 2008 by us presenting the synthesis and derivatives of these types of alkaloids [36]. Then the first synthesis of bannucine (26) and 5 -epibannucine (27) was elaborated [37]. This alkaloid was first isolated in 1986 from the leaves of Catharanthus roseus by Atta-Ur-Rahman and coworkers [38]. Bannucine (26) is a derivative of vindoline (1) having a 2-pyrrolidone ring in position 10. The key step of the procedure appears the reaction between the natural (−)-vindoline (1) and a cyclic N-acyliminium intermediate. As a result of the reaction not only the bannucine (26), but also its 5 -epimeric isomer (27) was formed in an approximate ratio of 2:3 ( Figure 9). The isomers were separated, and their structure was identified also by X-ray crystallography. The pure epimers were investigated on 57 cell lines of different types of cancer, however, important anticancer activity was not found [36].
instead of cyclopropanation in the course of Simmons-Smith reaction [34].
Halogenation reactions of monomer indole alkaloids vindoline (1) and catharanthine (2) were studied in detail, first of all the introduction of fluorine atom was investigated (Figure 8). In both cases the reactions resulted in unexpected products. Thus, in the case of vindoline (1) the fluoro containing quinone derivative (24) was formed and, in the case of catharanthine (2) a fluoro substituted indolenine (25) could be isolated [35].

Vindoline and Flavone Derivatives Containing 2-Pyrrolidone Ring
Our other important research area was the chemistry of Aspidospermane alkaloids. A detailed review was published in 2008 by us presenting the synthesis and derivatives of these types of alkaloids [36]. Then the first synthesis of bannucine (26) and 5′-epibannucine (27) was elaborated [37]. This alkaloid was first isolated in 1986 from the leaves of Catharanthus roseus by Atta-Ur-Rahman and coworkers [38]. Bannucine (26) is a derivative of vindoline (1) having a 2-pyrrolidone ring in position 10. The key step of the procedure appears the reaction between the natural (−)-vindoline (1) and a cyclic N-acyliminium intermediate. As a result of the reaction not only the bannucine (26), but also its 5′-epimeric isomer (27) was formed in an approximate ratio of 2:3 ( Figure 9). The isomers were separated, and their structure was identified also by X-ray crystallography. The pure epimers were investigated on 57 cell lines of different types of cancer, however, important anticancer activity was not found [36]. The first synthesis of sessiline (30) was achieved by applying the experiences gained in the field of acylaminocarbinols [39]. The alkaloid sessiline (30) was isolated from the fruits of Acanthopanas sessiliflorus in 2002 [40]. The molecule consists of two 5-membered heterocycles coupling through an acylaminocarbinol ether-type bond ( Figure 10). Sessiline (30) was prepared by reaction of 5hydroxypyrrolidin-2-one (28) with 5-hydroxymethyl-furfural (29) at 60 °C with 54% yield [39]. The first synthesis of sessiline (30) was achieved by applying the experiences gained in the field of acylaminocarbinols [39]. The alkaloid sessiline (30) was isolated from the fruits of Acanthopanas sessiliflorus in 2002 [40]. The molecule consists of two 5-membered heterocycles coupling through an acylaminocarbinol ether-type bond ( Figure 10). Sessiline (30) was prepared by reaction of 5-hydroxypyrrolidin-2-one (28) with 5-hydroxymethyl-furfural (29) at 60 • C with 54% yield [39]. Previously in our department, serious research was followed on the flavonoid chemistry. On the base of these results, the synthesis of flavones coupled with a heterocyclic ring was investigated. dracocephin A (32) and its regioisomer B (33) as a mixture of four stereoisomers were isolated in China from Dracocephalum rupestre in 2008 by Ren and coworkers [41]. A mixture of dracocephin A Previously in our department, serious research was followed on the flavonoid chemistry. On the base of these results, the synthesis of flavones coupled with a heterocyclic ring was investigated. dracocephin A (32) and its regioisomer B (33) as a mixture of four stereoisomers were isolated in China from Dracocephalum rupestre in 2008 by Ren and coworkers [41]. A mixture of dracocephin A (32) and B (33) in a ratio of 43:57 was prepared in a one-step reaction from (±)-naringenin (31) and separated by analytical chiral HPLC, the absolute configuration was identified by HPLC-ECD measurements and by using TDDFT-ECD (Time-dependent density functional theory electronic circular dichroism) calculations ( Figure 11). The physicochemical parameters and biologic activities of the compounds were also studied. Previously in our department, serious research was followed on the flavonoid chemistry. On the base of these results, the synthesis of flavones coupled with a heterocyclic ring was investigated. dracocephin A (32) and its regioisomer B (33) as a mixture of four stereoisomers were isolated in China from Dracocephalum rupestre in 2008 by Ren and coworkers [41]. A mixture of dracocephin A (32) and B (33) in a ratio of 43:57 was prepared in a one-step reaction from (±)-naringenin (31) and separated by analytical chiral HPLC, the absolute configuration was identified by HPLC-ECD measurements and by using TDDFT-ECD (Time-dependent density functional theory electronic circular dichroism) calculations ( Figure 11). The physicochemical parameters and biologic activities of the compounds were also studied. Further flavone alkaloids were also synthesized: 8-(2′′-pyrrolidinon-5′′-il)-quercetin (35) and (−)epicatechin (37) with the same substituent in position eight (38) and in position six (39), respectively [42,43]. Starting from quercetin (34) compound 35 and its C-6 (36) isomer were obtained in a ratio of 94:6 ( Figure 12). By a similar procedure, epicatechin (37) yielded a mixture of 38 and 39 in a 87:13 ratio ( Figure 13). These derivatives were prepared by acid-catalyzed regioselective Mannich reaction in which the in situ generated N-acyliminium ion started an electrophile attack to the aromatic A ring of the corresponding flavonoid precursors. Further flavone alkaloids were also synthesized: 8-(2 -pyrrolidinon-5 -il)-quercetin (35) and (−)-epicatechin (37) with the same substituent in position eight (38) and in position six (39), respectively [42,43]. Starting from quercetin (34) compound 35 and its C-6 (36) isomer were obtained in a ratio of 94:6 ( Figure 12). By a similar procedure, epicatechin (37) yielded a mixture of 38 and 39 in a 87:13 ratio ( Figure 13). These derivatives were prepared by acid-catalyzed regioselective Mannich reaction in which the in situ generated N-acyliminium ion started an electrophile attack to the aromatic A ring of the corresponding flavonoid precursors.

7-OH and 7-NH Modified Flavonoid Derivatives
Chrysin (40)-also known as 5,7-dihydroxyflavone-can be found among others in Passiflora caerulea [44,45], honey and propolis. Like several flavonoids, it has a number of biologic effects, of which it is important to mention its anticancer activity both as a chemopreventive and as a chemotherapeutic agent [46]. The driving force of our work was that several 7-O-modified derivatives had been found to be effective against different malignant tumor cells [47,48]. Therefore, we synthesized several new aryloxy acetamide derivatives (45)(46)(47)(48) (Figure 13). These products were rearranged to a biphenyl amine structure via Smiles rearrangement and hydrolysis to obtain a new series of 7-aminoflavone derivatives (49-52) ( Figure 14) [49].

7-OH and 7-NH Modified Flavonoid Derivatives
Chrysin (40)-also known as 5,7-dihydroxyflavone-can be found among others in Passiflora caerulea [44,45], honey and propolis. Like several flavonoids, it has a number of biologic effects, of which it is important to mention its anticancer activity both as a chemopreventive and as a chemotherapeutic agent [46]. The driving force of our work was that several 7-O-modified derivatives had been found to be effective against different malignant tumor cells [47,48]. Therefore, we synthesized several new aryloxy acetamide derivatives (45-48) ( Figure 13). These products were rearranged to a biphenyl amine structure via Smiles rearrangement and hydrolysis to obtain a new series of 7-aminoflavone derivatives (49-52) ( Figure 14) [49]. The products (45-52) were tested on 60 different human tumor cell lines in vitro (NIH, MD, USA) and three of the hydrolyzed Smiles products (50-52) showed prominent antitumor effect on several cell lines [49]. The products (45-52) were tested on 60 different human tumor cell lines in vitro (NIH, MD, USA) and three of the hydrolyzed Smiles products (50-52) showed prominent antitumor effect on several cell lines [49]. Funding: This research received no external funding.

Conflicts of Interest:
The authors declare no conflict of interest.