Effect of <i>Withania somnifera</i> on gentamicin induced renal lesions in rats

Govindappa, Prem Kumar; Gautam, Vidhi; Tripathi, Syamantak Mani; Sahni, Yash Pal; Raghavendra, Hallur Lakshmana Shetty

doi:10.1016/j.bjp.2018.12.005

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Original articles • Rev. bras. farmacogn. 29 (2) • Mar-Apr 2019 • https://doi.org/10.1016/j.bjp.2018.12.005 copy

Effect of Withania somnifera on gentamicin induced renal lesions in rats

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Gentamicin induced renal complications are well known in humans and animals. Medicinal properties of Withania somnifera (L.) Dunal, Solanaceae, are recognized to improve renal functions. However, the pharmacological function of W. somnifera is not completely understood. We sought to unravel medicinal therapeutic function of W. somnifera on gentamicin-induced nephrotoxicity in wistar rats. Twenty-four adult male wistar rats evenly divided into four groups to evaluate in vivo nephroprotective and nephrocurative function of W. somnifera in gentamicin induced nephrotoxic rats. Experimental design as follows: Group I, saline control for 21 days; Group II, gentamicin nephrotoxic control for eight days; Group III, alcoholic extract of W. somnifera for 13 days + simultaneous administration of gentamicin and W. somnifera, from day 14 to 21 (nephroprotective) and Group IV, gentamicin for 8 days + alcoholic extract of W. somnifera from day 9 to 21 (nephrocurative). End of experiment, respective serum and kidney tissue samples used to analyze renal function. Withania somnifera as a nephroprotective and nephrocurative molecule significantly restore the renal function on gentamicin-induced nephrotoxicity. This phenomenon is accompanied with significantly reduced blood urea nitrogen, creatine, alkaline phosphatase, gamma-glutamyl transferase, albumin, total protein, calcium, potassium and kidney malondialdehyde concentrations. Additionally, W. somnifera significantly increased antioxidant activities of glutathione and superoxide dismutase to protect renal tissue damage from gentamicin in wistar rats. Over all, W. somnifera treated nephroprotective animal shows improved recovery compared to nephrocuartive. The nephroprotective or nephrocurative effect of W. somnifera could be due to inherent antioxidant and free-radical-scavenging principle(s). In the near future, biologically active compounds of W. somnifera (withanolides) could appear as a novel therapeutic molecule for renal disorders.

Keywords:
Gentamicin; Antioxidant; Nephrotoxicity; Nephroprotective and nephrocurative

Peak	Number retention time	Active ingredient	Area	Area%
1	16.753	Withanoside IV	703 633	14.042
2	20.606	Withanoside V	715 829	14.285
3	21.140	Withaferin A	2 414 057	48.176
4	21.960	Withastramonolide	472 909	9.438
5	22.150	N/A	131 542	2.625
6	22.786	Withanolide A	472 719	9.434
7	25.965	Withanolide B	100 238	2.000
		Total	5 010 927	100.000

Group	Cr (mg dl^-1)	BUN (mg dl^-1)	Total Prot. (g dl^-1)	ALB (g dl^-1)	GGT (IU l^-1)	ALP (IU l^-1)	ALT (IU l^-1)	AST (IU l^-1)
Control	0.32 ± 0.01	34.09 ± 1.09	7.12 ± 0.08	3.05 ± 0.06	2.52 ± 0.10	140.2 ± 2.11	46.29 ± 1.30	56.59 ± 1.60
GM	0.90 ± 0.04^a	78.17 ± 2.45^a	9.91 ± 0.59^a	3.74 ± 0.09^a	5.40 ± 0.23^a	256.51 ± 5.21^a	75.84 ± 3.70^a	83.01 ± 1.47^a
NP	0.37 ± 0.01^b	37.42 ± 0.35^b	7.46 ± 0.05^b	3.14 ± 0.05^b	3.09 ± 0.03^b	141.32 ± 1.45^b	47.61 ± 1.32^b	58.77 ± 1.32^b
NC	0.40 ± 0.02^b	39.92 ± 0.81^b	7.85 ± 0.11^b	3.16 ± 0.03^b	3.23 ± 0.10^b	143.54 ± 1.30^b	50.87 ± 1.00^b	59.76 ± 0.94^b

Group	Sodium (mEq l^-1)	Potassium (mEq l^-1)	Calcium (mg dl^-1)
Control	138.53 ± 1.74	6.20 ± 0.74	7.91 ± 0.10
GM	142.52 ± 2.68	4.55 ± 1.01^a	5.14 ± 0.07^a
NP	140.50 ± 1.48	6.33 ± 0.78^b	7.21 ± 0.10^b
NC	140.75 ± 1.84	5.68 ± 0.87^b	7.16 ± 0.20^b

Group	LPO (nM MDA g^-1 of tissue)	GSH (µM GSH g^-1 of tissue)	SOD (U g^-1 of tissue)
Control	71.85 ± 1.08	71.74 ± 3.73	876.83 ± 0.32
GM	126.71 ± 1.45^a	37.38 ± 4.06^a	574.87 ± 0.36^a
NP	73.83 ± 1.56^b	60.77 ± 3.66^b	843.34 ± 0.68^b
NC	80.59 ± 0.51^b	58.79 ± 4.67^b	806.98 ± 0.71^b

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[1] * Corresponding author. E-mail:pgovindappa@pennstatehealth.psu.edu (P.K. Govindappa).