The deleterious effect of xylene-induced ear edema in rats: Protective role of dexketoprofen trometamol transdermal invasomes via inhibiting the oxidative stress/NF-ΚB/COX-2 pathway

被引:9
|
作者
Soliman, Sara M. [1 ]
Teaima, Mahmoud Hassan [2 ]
Rashwan, Kareem Omar [1 ]
Ali, Bassam Mohamed [3 ]
Jasti, Bhaskara R. [4 ]
El-Nabarawi, Mohamed A. [2 ]
El-Halim, Shady M. Abd [1 ]
机构
[1] October 6 Univ, Fac Pharm, Dept Pharmaceut & Ind Pharm, 6th of October City 12585, Giza, Egypt
[2] Cairo Univ, Fac Pharm, Dept Pharmaceut & Ind Pharm, Cairo 11562, Egypt
[3] October 6 Univ, Fac Pharm, Dept Biochem, 6th of October City 12585, Giza, Egypt
[4] Univ Pacific, Thomas J Long Sch Pharm & Hlth Sci, Dept Pharmaceut & Med Chem, Stockton, CA USA
关键词
Dexketoprofen trometamol; Invasomes; Transdermal; Xylene-induced ear edema; COX-2; NF-?B p65; Oxidative stress; DRUG-DELIVERY SYSTEMS; IN-VITRO; EX-VIVO; ANTIINFLAMMATORY ACTIVITIES; FENTICONAZOLE NITRATE; LOADED INVASOMES; OPTIMIZATION; TERPESOMES; NANOPARTICLES; FORMULATION;
D O I
10.1016/j.ijpharm.2022.122525
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Pain and inflammation could have a negative impact on a patient's quality of life and performance, causing them to sleep less. Dexketoprofen trometamol (DKT) is a water-soluble, nonselective NSAIDs. Because DKT is quickly eliminated in the urine after oral delivery, its efficacy is limited and must be taken repeatedly throughout the day. The main ambition of this work is to develop and characterize the potential of invasomes to enhance the transdermal transport of DKT to achieve efficient anti-inflammatory and pain management. The optimum formulation (C1) showed the least %RE (53.29 +/- 2.68 %), the highest %EE (86.51 +/- 1.05 %), and spherical nanosized vesicles (211.9 +/- 0.57 nm) with (PDI) of 0.353 +/- 0.01 and (ZP) of-19.15 +/- 2.45 mV. DKT flux and deposition in stratum corneum, epidermal, and dermal skin layers were significantly augmented by 2.6 and 3.51 folds, respectively, from the optimum invasomal gel formulation (C1-G) compared to DKT conventional gel (DKT-G). The anti-inflammatory activity of C1-G was evaluated using a model of xylene-induced ear edema in rats. Xylene exposure upregulated the ear expression of COX-2 level and MPO activity. Xylene also significantly increased the ear NF-kappa B p65, TNF-alpha, IL-I beta, and MDA levels. Furthermore, xylene induced oxidative stress, as evidenced by a significant decrease in ear GSH and serum TAC levels. These impacts were drastically improved by applying C1-G compared to rats that received DKT-G and plain invasomal gel formulation (plain C1-G). The histopathological findings imparted substantiation to the biochemical and molecular investigations. Thereby, C1 -G could be a promising transdermal drug delivery system to improve the anti-inflammatory and pain manage-ment of DKT.
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页数:13
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