Protective Mechanism ofAcacia salignaButanol Extract and Its Nano-Formulations against Ulcerative Colitis in Rats as Revealed via Biochemical and Metabolomic Assays

被引:38
作者
Abdallah, Heba M. I. [1 ]
Ammar, Naglaa M. [2 ]
Abdelhameed, Mohamed F. [1 ]
Gendy, Abd El-Nasser G. El [3 ]
Ragab, Tamer I. M. [4 ]
Abd-ElGawad, Ahmed M. [5 ,6 ]
Farag, Mohamed A. [7 ,8 ]
Alwahibi, Mona S. [9 ]
Elshamy, Abdelsamed I. [10 ,11 ]
机构
[1] Natl Res Ctr, Dept Pharmacol, Div Med Res, Giza 12622, Egypt
[2] Natl Res Ctr, Therapeut Chem Dept, Giza 12622, Egypt
[3] Natl Res Ctr, Med & Aromat Plants Res Dept, Giza 12622, Egypt
[4] Natl Res Ctr, Chem Nat & Microbial Prod Dept, Giza 12622, Egypt
[5] King Saud Univ, Plant Prod Dept, Coll Food & Agr Sci, POB 2460, Riyadh 11451, Saudi Arabia
[6] Mansoura Univ, Dept Bot, Fac Sci, Mansoura 35516, Egypt
[7] Cairo Univ, Dept Pharmacognosy, Coll Pharm, Kasr el Aini St, Cairo 11562, Egypt
[8] Amer Univ Cairo, Dept Chem, Sch Sci & Engn, New Cairo 11835, Egypt
[9] King Saud Univ, Dept Bot & Microbiol, Coll Sci, Riyadh 11451, Saudi Arabia
[10] Natl Res Ctr, Dept Nat Cpds Chem, Giza 12622, Egypt
[11] Tokushima Bunri Univ, Fac Pharmaceut Sci, Yamashiro Cho, Tokushima 7708514, Japan
来源
BIOLOGY-BASEL | 2020年 / 9卷 / 08期
关键词
Acacia saligna; ulcerative colitis; nano-extract; inflammation; metabolomics; NANOCRYSTALLINE SILVER CREAM; INFLAMMATORY-BOWEL-DISEASE; ACID-INDUCED COLITIS; ANTIINFLAMMATORY PROPERTIES; MODEL; ANTIOXIDANT; L; ACTIVATION; INHIBITION; EXPRESSION;
D O I
10.3390/biology9080195
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
Ulcerative colitis (UC) is a relapsing inflammatory disease of unknown etiology. The increased risk of cancer in UC patients warrants for the development of novel drug treatments. Herein, this work concerns with the investigation of the protective effects ofAcacia salignabutanol extract (ASBE) and its nanoformulations on UC in a rat model and its underlying mechanism. Colitis was induced by slow intrarectal infusion of 2 mL of 4% (v/v in 0.9% saline) acetic acid. Colon samples were evaluated macroscopically, microscopically, and assayed for pro-inflammatory cytokine levels. To monitor associated metabolic changes in acetic acid-induced UC model, serum samples were analyzed for primary metabolites using GC-MS followed by multivariate data analyses. Treatment with ASBE attenuated acetic acid-induced UC as revealed by reduction of colon weight, ulcer area, and ulcer index. ASBE treatment also reduced Cyclooxygenase-2 (COX-2), Prostaglandin E2 (PGE2) & Interleukin-1 beta(IL-1 beta) levels in the inflamed colon. The nano-formulation of ASBE showed better protection than the crude extract against ulcer indices, increased PGE2 production, and histopathological alterations such as intestinal mucosal lesions and inflammatory infiltration. Distinct metabolite changes were recorded in colitis rats including a decrease in oleamide and arachidonic acid along with increased levels of lactic acid, fructose, and pyroglutamic acid. Treatment with nano extract restored metabolite levels to normal and suggests that cytokine levels were regulated by nano extract in UC. Conclusion: ASBE nano extract mitigated against acetic acid-induced colitis in rats, and the underlying mechanism could be attributed to the modulatory effects of ASBE on the inflammatory cascades. The applicability of metabolomics developed in this rat model seems to be crucial for evaluating the anti-inflammatory mechanisms of new therapeutics for acute colitis.
引用
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页码:1 / 21
页数:21
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