Synthesis of some novel enzyme inhibitors and antibacterial agents derived from 5-(1-(4-tosyl)piperidin-4-yl)-1,3,4-oxadiazol-2-thiol

Sattar, Almas; Aziz-ur-Rehman,; Abbasi, Muhammad Athar; Siddiqui, Sabahat Zahra; Rasool, Shahid; Ahmad, Irshad

doi:10.1590/S1984-82502016000100009

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Brazilian Journal of Pharmaceutical Sciences

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Articles • Braz. J. Pharm. Sci. 52 (01) • Mar 2016 • https://doi.org/10.1590/S1984-82502016000100009 copy

Synthesis of some novel enzyme inhibitors and antibacterial agents derived from 5-(1-(4-tosyl)piperidin-4-yl)-1,3,4-oxadiazol-2-thiol

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Keeping in mind the pharmacological importance of the 1,3,4-oxadiazole moiety, a series of new S-substituted derivatives, 5a-h, of 5-(1-(4-tosyl)piperidin-4-yl)-1,3,4-oxadiazol-2-thiol (3) were synthesized. The reaction of p-toluenesulfonyl chloride (a) and ethyl isonipecotate (b) produced ethyl 1-(4-tosyl)piperidin-4-carboxylate (1) which was further transformed into 1-(4-tosyl)piperidin-4-carbohydrazide (2) by hydrazine hydrate in methanol. Compound 2 was refluxed with CS₂ in the presence of KOH to synthesize 5-(1-(4-tosyl)piperidin-4-yl)-1,3,4-oxadiazol-2-thiol (3). The desired compounds, 5a-h, were synthesized by stirring 3 with aralkyl halides, 4a-h, in DMF using NaH as an activator. The structures of synthesized compounds were elucidated by ¹H-NMR, IR and EI-MS spectral studies. These compounds were further evaluated for enzyme inhibitory activity against lipoxygenase and alpha-glucosidase, along with antibacterial activity against Gram-negative and Gram-positive bacteria.

Uniterms:
1,3,4-Oxadiazole/antibacterial activity. 1,3,4-Oxadiazole/enzyme inhibitory activity. Isonipecotate. Sulfonamide.

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: Aziz-ur-Rehman. Department of Chemistry. Government College University. Lahore-54000. Pakistan. E-mail: azizryk@yahoo.com, rehman@gcu.edu.pk

Compound	Lipoxygenase (LOX)		α-Glucosidase
Compound	Inhibition (%) at 0.5 mM	IC₅₀ µM	Inhibition (%) at 0.5 mM	IC₅₀ µM
5a	47.81 ± 0.06	-	65.22 ± 0.31	197.98 ± 0.11
5b	99.12 ± 0.41	78.38 ± 0.12	81.11 ± 0.24	181.92 ± 0.17
5c	11.71 ± 0.14	-	78.14 ± 0.31	195.53 ± 0.19
5d	56.95 ± 0.33	229.72 ± 0.16	11.33 ± 0.25	-
5e	12.25 ± 0.89	-	83.56 ± 0.16	185.58 ± 0.18
5f	47.43 ± 0.56	-	9.27 ± 0.12	-
5g	11.62 ± 0.41	-	61.55 ± 0.13	313.79 ± 0.07
5h	14.37 ± 0.29	-	84.46 ± 0.16	321.43 ± 0.14
Control	93.79 ± 1.27^a	22.41 ± 1.3^a	92.23 ± 0.14^b	38.25 ± 0.12^b

Compounds	% INHIBITION
Compounds	S. typhi (-)	E. coli (-)	P. aeruginosa (-)	S. aureus (+)	B. subtilis (+)
5a	57.94 ± 0.75	61.15 ± 0.35	63.32 ± 0.19	33.43 ± 0.10	74.60 ± 0.93
5b	55.76 ± 0.80	51.50 ± 0.10	53.93 ± 0.89	20.86 ± 0.55	56.50 ± 1.13
5c	-	-	-	-	-
5d	64.05 ± 0.60	70.00 ± 1.00	44.36 ± 0.50	40.28 ± 0.55	52.07 ± 0.33
5e	72.39 ± 0.70	67.10 ± 1.10	47.02 ± 0.56	34.29 ± 0.45	58.80 ± 0.47
5f	79.74 ± 0.60	46.70 ± 0.65	48.35 ± 0.17	29.05 ± 0.81	70.53 ± 0.13
5g	68.55 ± 0.09	63.15 ± 0.85	64.33 ± 0.32	27.38 ± 0.24	72.57 ± 0.81
5h	52.73 ± 0.68	57.30 ± 0.70	49.95 ± 0.66	57.14 ± 0.29	57.87 ± 0.09
Ciprofloxacin	91.05 ± 0.68	92.32 ± 0.42	92.02 ± 053	91.44 ± 0.64	92.50 ± 0.34

Compounds	MIC (µM)
Compounds	S. typhi (-)	E. coli (-)	P. aeruginosa (-)	S. aureus (+)	B. subtilis (+)
5a	16.42 ± 0.10	14.32 ± 0.56	12.87 ± 0.41	-	9.65 ± 0.24
5b	16.98 ± 0.45	19.80 ± 0.12	17.97 ± 0.15	-	16.43 ± 0.52
5c	-	-	-	-	-
5d	11.57 ± 0.71	9.78 ± 0.66	-	-	19.80 ± 0.18
5e	9.15 ± 0.24	10.09 ± 0.05	-	-	16.83 ± 0.91
5f	8.24 ± 0.90	-	-	-	9.10 ± 0.41
5g	9.69 ± 0.16	13.79 ± 0.12	11.87 ± 0.50	-	9.27 ± 0.17
5h	17.43 ± 0.33	15.67 ± 0.34	-	16.78 ± 0.95	16.42 ± 0.12
Ciprofloxacin	7.45 ± 0.58	7.16 ± 0.58	7.29 ± 0.90	7.80 ± 0.19	7.14 ± 0.18