Acetylcholinesterase inhibition and antimicrobial activity of hydroxyl amides synthesized from natural products derivatives

BOAVENTURA, MARIA AMÉLIA D.; XAVIER, LAURA F.W.; VIEIRA, HENRIETE S.; TAKAHASHI, JACQUELINE A.; NASCIMENTO JUNIOR, WILTON J.D.; ARAUJO, TAMIRES P.; COELHO, AMANDA C.S.

doi:10.1590/0001-3765201820170451

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Chemical Sciences • An. Acad. Bras. Ciênc. 90 (2 suppl 1) • Aug 2018 • https://doi.org/10.1590/0001-3765201820170451 copy

Acetylcholinesterase inhibition and antimicrobial activity of hydroxyl amides synthesized from natural products derivatives

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Thirteen natural products derivatives of hydroxyl amide class, three described for the first time, were synthesized by reaction of three indole acids and 3,4,5-trimethoxybenzoic acid with six different amino alcohols in the presence of triphenylphosphine and N-bromosuccinimide. The derivatives were tested against the Gram (+) bacteria Staphylococcus aureus and Bacillus cereus, Gram (-) Pseudomonas aeruginosa and Escherichia coli, besides the yeast Candida albicans. One of the compounds (7) was selectively active against C. albicans (91.3 ± 0.49% inhibition) showing a great potential as a new drug lead, since it was more active than the positive control, miconazole (88.7 ± 2.41% inhibition). Regarding bacterial inhibition, compounds demonstrated mild activity, but inhibition of compounds 9, 10 and 13 towards E. coli is of interest since it is difficult to find drugs selectively active against Gram (-) bacteria. Most of the compounds were very active in the acetylcholinesterase inhibition assay. Compound 7 was again the most active (93.2 ± 4.47%), being more potent than the control galantamine (90.3 ± 0.45%). The most active gallic acid derivatives, compounds 3, 7 and 8 have in common, besides gallic acid skeleton, a (CH₂)₂OH group, which may be one of the structural requirements for AChE inhibition.

Key words:
acetylcholinesterase inhibition; antimicrobial activity; indole acid derivatives; 3,4,5-trimethoxybenzoic acid derivatives

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[1] Correspondence to: Maria Amélia D. Boaventura E-mail: boaventuram3@gmail.com

Compound	C. albicans	E. coli	P. aeruginosa	S. aureus	B. cereus
3	20.3 ± 2.42	19.7 ± 2.68	17.3 ± 1.19	25.6 ± 0.31	0.0
4	20.7 ± 2.45	24.4 ± 3.80	16.4 ± 1.68	23.1 ± 0.86	0.0
5	23.9 ± 0.48	10.4 ± 1.90	6.9 ± 1.89	13.8 ± 5.84	9.7 ± 0.59
6	25.3 ± 0.56	24.2 ± 1.42	27.7 ± 3.61	24.4 ± 2.26	19.8 ± 0.09
7	91.3 ± 0.49	22.1 ± 0.35	17.8 ± 1.32	26.3 ± 1.01	18.1 ± 0.81
8	29.7 ± 1.20	17.1 ± 3.19	8.3 ± 0.79	15.1 ± 0.88	12.1 ± 0.89
9	61.0 ± 2.30	44.0 ± 1.55	35.6 ± 2.20	40.3 ± 0.66	18.1 ± 4.05
10	63.0 ± 2.18	49.8 ± 1.03	31.0 ± 1.69	36.2 ± 1.63	26.9 ± 0.72
11	31.3 ± 2.95	39.2 ± 3.89	25.6 ± 1.39	38.0 ± 1.09	18.1 ± 5.04
12	21.7 ± 1.15	35.4 ± 2.66	19.9 ± 2.76	43.0 ± 0.62	21.7 ± 0.90
13	21.9 ± 3.33	47.0 ± 3.11	34.1 ± 2.25	47.6 ± 1.79	23.3 ± 1.44
14	24.5 ± 1.27	33.9 ± 2.81	25.8 ± 1.68	33.8 ± 1.22	12.5 ± 1.71
15	56.6 ± 2.84	31.9 ± 2.07	18.7 ± 0.44	35.6 ± 0.39	22.7 ± 2.34
Miconazole	88.7 ± 2.41	-	-	-	-
Ampiciline	-	96.3 ± 0.43	96.5 ± 0.40	97.9 ± 0.12	96.8 ± 0.27

Sample	% Inhibition (mean ± sd)
3	86.7 ± 1.55
4	80.8 ± 1.94
5	80.8 ± 1.94
6	87.5 ± 0.80
7	93.2 ± 4.47
8	83.6 ± 5.94
9	37.9 ± 4.25
10	20.5 ± 3.59
11	56.5 ± 3.83
12	67.5 ± 2.90
13	37.6 ± 3.94
14	59.3 ± 4.82
15	71.4 ± 5.41
Galantamine	90.3 ± 0.45
Eserine	89.8 ± 0.67