Synthesis, antileishmanial activity and QSAR studies of 2-chloro-<b><i>N</i></b> -arylacetamides

Lavorato, Stefânia Neiva; Duarte, Mariana Costa; Andrade, Pedro Henrique Rocha De; Coelho, Eduardo Antonio Ferraz; Alves, Ricardo José

doi:10.1590/s2175-97902017000116067

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Brazilian Journal of Pharmaceutical Sciences

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Article • Braz. J. Pharm. Sci. 53 (1) • 2017 • https://doi.org/10.1590/s2175-97902017000116067 copy

Synthesis, antileishmanial activity and QSAR studies of 2-chloro-N -arylacetamides

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ABSTRACT

We describe herein the synthesis and evaluation of the antileishmanial activity against promastigote forms of Leishmania amazonensis and cytotoxicity to murine macrophages of a series of 2-chloro-N-arylacetamide derivatives. All compounds were active, except one (compound 3). Compound 5 presented the most promising results, showing good antileishmanial activity (CI₅₀=5.39±0.67 µM) and moderate selectivity (SI=6.36), indicating that further development of this class is worthwhile. Preliminary QSAR studies, although not predictive, furnished some insights on the importance of electronic character of aryl substituent to biological activity, as well as an indirect influence of hydrophobicity on activity.

Uniterms:
Leishmaniasis/treatment; Chloroacetamides; Leishmania amazonensisChloroacetamides/QSAR.

Compounds	R	log (1/IC₅₀)^a			ClogP^c	σ_R ^d	MR_R ^e
Compounds	R	Obs.	Calc.^b	∆
1	H	4.94	4.865	0.075	1.75	0	1.03
2	COOCH₂CH₃	5.36	5.178	0.182	2.11	0.45	17.49
3	COOH	-	-	-	-1.66^f	0.45	6.93
4^g	SO₂NH₂	4.84	5.262	-0.422	0.35^f	0.57	12.28
5	COCH₃	5.27	5.213	0.057	1.31	0.50	11.18
6	Cl	4.93	5.025	-0.095	2.35	0.23	6.03
7	Br	4.92	5.025	-0.105	2.52	0.23	8.88
8	NO₂	5.32	5.408	-0.088	1.69	0.78	7.36
9	CH₃	4.72	4.747	-0.027	2.26	-0.17	5.65
10	OCH₃	4.68	4.678	0.002	1.59	-0.27	7.87

	Regression equation	n/p ^a	^_rb	^_r2c	^_pe	Outlier
1	log(1/IC₅₀) = 0.6949(±0.2817)σ_R + 4.8655(±0.1122)	8	0.927	0.859	0.0009	4
2	log(1/IC₅₀) = 0.0059(±0.3455)ClogP + 4.9873(±0.6485)	9	0.015	0.0002	0.9689	-
3	log(1/IC₅₀) = 0.0263(±0.0431)MR_R + 4.7701(±0.4184)	9	0.479	0.230	0.1920	-
4	log(1/IC₅₀) = 0.6521(±0.4272)σ_R + 0.1314(±0.2271)ClogP + 4.5972(±0.4726)	4.5	0.836	0.699	0.0272	-
5	log(1/IC₅₀) = 0.5166(±0.5207)σ_R + 0.0071(±0.0394)MR_R + 4.8037(±0.3338)	4.5	0.782	0.611	0.0587	-
6	log(1/IC₅₀) = 0.0280(±0.0490)MR_R + 0.0516(±0.3446)ClogP + 4.6642(±0.8457)	4.5	0.496	0.246	0.4281	-

Universidade de São Paulo, Faculdade de Ciências Farmacêuticas Av. Prof. Lineu Prestes, n. 580, 05508-000 S. Paulo/SP Brasil, Tel.: (55 11) 3091-3824 - São Paulo - SP - Brazil
E-mail: bjps@usp.br

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[1] *Correspondence: R. J. Alves. Departamento de Produtos Farmacêuticos. Faculdade de Farmácia. Universidade Federal de Minas Gerais. Avenida Antônio Carlos, 6627 - 31.270-901 - Belo Horizonte, MG, Brasil. Tel: +55 31 3409 6955; Fax: + 55 31 3409 6935. E-mail: ricardodylan@farmacia.ufmg.br

Compounds	IC₅₀ ±SD (µM)^a	CC₅₀ ±SD (µM)^b	SI^c
1	11.41±6.05	46.37±4.29	4.06
2	4.74±0.20	18.52±3.89	3.91
3	Inactive	ND^d	ND^d
4	14.42±2.13	22.84±8.70	1.58
5	5.39±0.67	34.28±16.66	6.36
6	11.88±0.80	17.99±1.66	1.51
7	11.91±0.57	17.71±4.89	1.49
8	4.78±1.22	18.50±0.13	3.87
9	18.84±10.86	29.95±4.08	1.59
10	21.01±7.33	25.15±0.21	1.20
AmpB^e	0.1±0.02	0.78±0.21	8.0