Antiprotozoal activity and DNA binding of N-substituted N-phenylbenzamide and 1,3-diphenylurea bisguanidines

Martinez, Carlos; Lagartera, Laura; Kaiser, Marcel; Dardonville, Christophe

doi:10.1016/j.ejmech.2014.04.083

Cited by 13 publications

(19 citation statements)

References 31 publications

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“…3,4,7 In previous studies, we have discovered diphenyl dicationic compounds 1-5 (Chart 1) that showed excellent in vivo activity against African trypanosomes (T. b. rhodesiense) in mouse models of sleeping sickness. [9][10][11][12] The binding interaction of 5 with the minor groove of the all-AT DNA sequence dĲAAAATTTT) 2 and with the selfcomplimentary nucleotide dĲCTTAATTCGAATTAAG) 2 was demonstrated by X-ray crystallography. 13,14 Nagle et al showed that arylamide derivatives 1 and 2 bound strongly and selectively to AT oligonucleotides with a slight preference (2-to 3-fold) for dsDNA CGAATTCG vs. CATATATAT sequences.…”

Section: Introductionmentioning

confidence: 99%

Bisimidazoline arylamides binding to the DNA minor groove: N1-hydroxylation enhances binding affinity and selectivity to AATT sites

et al. 2015

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Section: Introductionmentioning

confidence: 99%

Bisimidazoline arylamides binding to the DNA minor groove: N1-hydroxylation enhances binding affinity and selectivity to AATT sites

et al. 2015

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“…Regarding the mode of action of the antitrypanosomal lead compounds I to V, earlier studies have shown that this class of dicationic compounds binds to the DNA minor groove at AT-rich sequences (55)(56)(57)(58). In trypanosomes, the kinetoplast DNA (kDNA) has a high content of AT-rich regions that could be a site of selective action of this kind of compound (59).…”

Section: Discussionmentioning

confidence: 99%

A New Nonpolar N -Hydroxy Imidazoline Lead Compound with Improved Activity in a Murine Model of Late-Stage Trypanosoma brucei brucei Infection Is Not Cross-Resistant with Diamidines

Martinez

Miller

Ganeshamoorthy

et al. 2015

Antimicrob Agents Chemother

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Treatment of late-stage sleeping sickness requires drugs that can cross the blood-brain barrier (BBB) to reach the parasites located in the brain. We report here the synthesis and evaluation of four new N-hydroxy and 12 new N-alkoxy derivatives of bisimidazoline leads as potential agents for the treatment of late-stage sleeping sickness. These compounds, which have reduced basicity compared to the parent leads (i.e., are less ionized at physiological pH), were evaluated in vitro against Trypanosoma brucei rhodesiense and in vivo in murine models of first-and second-stage sleeping sickness. Resistance profile, physicochemical parameters, in vitro BBB permeability, and microsomal stability also were determined. The N-hydroxy imidazoline analogues were the most effective in vivo, with 4-((1-hydroxy-4,5-dihydro-1H-imidazol-2-yl)amino)-N-(4-((1-hydroxy-4,5-dihydro-1H-imidazol-2-yl)amino)phenyl)benzamide (14d) showing 100% cures in the first-stage disease, while 15d, 16d, and 17d appeared to slightly improve survival. In addition, 14d showed weak activity in the chronic model of central nervous system infection in mice. No evidence of reduction of this compound with hepatic microsomes and mitochondria was found in vitro, suggesting that N-hydroxy imidazolines are metabolically stable and have intrinsic activity against T. brucei. In contrast to its unsubstituted parent compound, the uptake of 14d in T. brucei was independent of known drug transporters (i.e., T. brucei AT1/P2 and HAPT), indicating a lower predisposition to cross-resistance with other diamidines and arsenical drugs. Hence, the N-hydroxy bisimidazolines (14d in particular) represent a new class of promising antitrypanosomal agents.

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“…For the antiprotozoal and antimicrobial properties of phenylbenzamides, see: Ríos Martínez et al (2014); Ş ener et al (2000). For active metabolites of benzoxazoles, see: Mobinikhaledi et al (2006).…”

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confidence: 99%

“…The crystal structure determination of the title compound (I), is part of a study on phenylbenzamides carried out in our research group, and they are synthesized from the reaction of picryl benzoates with 2-hydroxy-aniline. These compounds have received extensive attention because of their antiprotozoal (Ríos Martínez et al, 2014) and anti-microbialactivity (Şener et al, 2000), and as active metabolites of benzoxazoles (Mobinikhaledi et al, 2006). They have also been studied as inhibitors of tyrosine kinases (Capdeville et al, 2002) and inducers of apoptosis in the tumor development process (Olsson et al, 2002).…”

Section: S1 Commentmentioning

confidence: 99%

Crystal structure of 4-bromo-N-(2-hydroxyphenyl)benzamide

2014

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In the title compound, C13H10BrNO2, the mean plane of the non-H atoms of the central amide C—N—C(=O)—C fragment (r.m.s. deviation = 0.004 Å) forms a dihedral angle of 73.97 (12)° with the hydroxy-substituted benzene ring and 25.42 (19)° with the bromo-substituted benzene ring. The two aromatic rings are inclined to one another by 80.7 (2)°. In the crystal, molecules are linked by O—H⋯O and N—H⋯O hydrogen bonds, forming chains along [010]. The chains are linked by weak C—H⋯O hydrogen bonds, forming sheets parallel to (100), and enclosing R 3 3(17) and R 3 2(9) ring motifs.

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Antiprotozoal activity and DNA binding of N-substituted N-phenylbenzamide and 1,3-diphenylurea bisguanidines

Abstract: The compounds were tested against T. b. rhodesiense and P. falciparum.N-alkylated compounds 7b and 7c were 100% curative in the STIB900 mouse model of HAT.DNA binding affinity was measured by SPR with AATT, (AT) 4 and (CG) 4 hairpin duplexes.7b and 7c bind selectively to AT-rich DNA.

Cited by 13 publications

References 31 publications

Bisimidazoline arylamides binding to the DNA minor groove: N1-hydroxylation enhances binding affinity and selectivity to AATT sites

Bisimidazoline arylamides binding to the DNA minor groove: N1-hydroxylation enhances binding affinity and selectivity to AATT sites

A New Nonpolar N -Hydroxy Imidazoline Lead Compound with Improved Activity in a Murine Model of Late-Stage Trypanosoma brucei brucei Infection Is Not Cross-Resistant with Diamidines

Crystal structure of 4-bromo-N-(2-hydroxyphenyl)benzamide

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