西洋菜( Nasturtium officinale R. Br.)通过糖皮质激素受体依赖和 NF-κB 通路有效减轻巴豆油诱导的皮肤炎症,且在小鼠体内无毒性作用。

Nasturtium officinale R. Br. effectively reduces the skin inflammation induced by croton oil via glucocorticoid receptor-dependent and NF-κB pathways without causing toxicological effects in mice.

机构信息

Laboratory Neurotoxicity and Psychopharmacology, Graduate Program in Biological Sciences: Toxicological Biochemistry, Center of Natural and Exact Sciences, Federal University of Santa Maria, Santa Maria, RS, Brazil.

Graduate Program in Genetics and Biochemistry, Institute of Genetics and Biochemistry, Federal University of Uberlandia, Uberlandia, MG, Brazil.

出版信息

J Ethnopharmacol. 2019 Jan 30;229:190-204. doi: 10.1016/j.jep.2018.10.011. Epub 2018 Oct 17.

Abstract

ETHNOPHARMACOLOGICAL RELEVANCE

Inflammatory skin diseases treatments currently used cause adverse effects. Nasturtium officinale (watercress) is used popularly as an anti-inflammatory. However, until now, no study proved its effectiveness as a topical treatment to inflammatory skin diseases. The topical anti-inflammatory activity of N. officinale crude extract leaves (NoE) on an irritant contact dermatitis (ICD) model croton oil-induced in mice was investigated.

MATERIALS AND METHODS

ICD models were induced by a single (1 mg/ear; acute) or repeated (0.4 mg/ear; chronic; 9 days total) croton oil application. NoE and dexamethasone solutions' (diluted in acetone; 20 μL/ear) or NoE gel, dexamethasone gel and base gel (15 mg/ear) were topically applied immediately after croton oil application. The NoE topical anti-inflammatory effect was evaluated for inflammatory parameters (ear edema, inflammatory cells infiltration, and inflammatory cytokines levels). NoE topical anti-inflammatory mechanism (NF-κB pathway and effect glucocorticoid-like) were assessed by western blot and ear edema analyses, respectively. UHPLC-MS/MS chromatography, gels accelerated stability and preliminary study of adverse effects was also performed.

RESULTS

UHPLC-MS/MS of the NoE revealed the presence of coumaric acid, rutin, and ferulic acid. NoE gels stability study showed no relevant changes at low temperature. NoE, dexamethasone, NoE gel and dexamethasone gel inhibited the ear edema croton oil-induced by 82 ± 6% (1 mg/ear), 99 ± 1% (0.1 mg/ear), 81 ± 8% (3%) and 70 ± 6% (0.5%) for the acute model, and 49 ± 7% (1 mg/ear), 80 ± 4% (0.1 mg/ear), 41 ± 8% (3%) and 46 ± 14% (0.5%) for the chronic model, respectively. The same treatments also reduced the inflammatory cells infiltration by 62 ± 3% (1 mg/ear), 97 ± 2% (0.1 mg/ear), 60 ± 3% (3%) and 66 ± 6% (0.5%) for the acute model, respectively, and 25 ± 8% (1 mg/ear) to NoE and 83 ± 13% to dexamethasone to the chronic model. NoE and NoE gel reduced the pro-inflammatory cytokines levels (acute ICD model) by 62 ± 5% and 71 ± 3% (MIP-2) and 32 ± 3% and 44 ± 4% (IL-1β), while dexamethasone solution's and gel reduced by 79 ± 7% and 44 ± 4% to MIP-2 and 98 ± 2% and 83 ± 9% to IL-1β, respectively. NoE' and dexamethasone' solutions inhibited the reduction of IkB-α protein expression induced by croton oil by 100% and 80 ± 14%, respectively. Besides, the mifepristone (glucocorticoid receptor antagonist) pre-treatment prevented the topical anti-edematogenic effect of NoE' and dexamethasone' solutions by 61 ± 5% to NoE and 78 ± 16% to dexamethasone. The repeated topical application of NoE did not cause adverse effects.

CONCLUSION

Our results suggest the N. officinale use in the cutaneous inflammatory process treatment and demonstrate the NoE potential to develop a promising topical anti-inflammatory agent to treat inflammatory disorders.

摘要

民族药理学相关性

目前用于治疗炎症性皮肤病的药物会引起不良反应。豆瓣菜(西洋菜)被广泛用作抗炎药。然而,到目前为止,还没有研究证明其作为局部治疗炎症性皮肤病的有效性。本研究旨在研究豆瓣菜粗提物叶(NoE)对致炎接触性皮炎(ICD)模型中鼠耳的局部抗炎活性。

材料与方法

通过单次(1mg/耳;急性)或重复(0.4mg/耳;慢性;共 9 天)涂抹巴豆油诱导 ICD 模型。NoE 和地塞米松溶液(溶于丙酮;20μL/耳)或 NoE 凝胶、地塞米松凝胶和基质凝胶(15mg/耳)在涂抹巴豆油后立即局部应用。通过耳肿胀、炎症细胞浸润和炎症细胞因子水平评估 NoE 的局部抗炎作用。通过 Western blot 和耳肿胀分析分别评估 NoE 的局部抗炎机制(NF-κB 通路和类皮质激素作用)。还进行了 UHPLC-MS/MS 色谱分析、凝胶加速稳定性和不良反应初步研究。

结果

NoE 的 UHPLC-MS/MS 分析显示存在香豆酸、芦丁和阿魏酸。NoE 凝胶的稳定性研究表明,在低温下无明显变化。NoE、地塞米松、NoE 凝胶和地塞米松凝胶分别抑制了 82±6%(1mg/耳)、99±1%(0.1mg/耳)、81±8%(3%)和 70±6%(0.5%)的急性模型、49±7%(1mg/耳)、80±4%(0.1mg/耳)、41±8%(3%)和 46±14%(0.5%)的慢性模型的耳肿胀。同样的治疗方法还减少了 62±3%(1mg/耳)、97±2%(0.1mg/耳)、60±3%(3%)和 66±6%(0.5%)的急性模型和 25±8%(1mg/耳)至 NoE 和 83±13%至地塞米松的慢性模型的炎症细胞浸润。NoE 和 NoE 凝胶降低了促炎细胞因子水平(急性 ICD 模型)62±5%和 71±3%(MIP-2)和 32±3%和 44±4%(IL-1β),而地塞米松溶液和凝胶降低了 79±7%和 44±4%至 MIP-2 和 98±2%和 83±9%至 IL-1β。NoE 和地塞米松溶液分别抑制了巴豆油诱导的 IkB-α 蛋白表达减少 100%和 80±14%。此外,米非司酮(糖皮质激素受体拮抗剂)预处理阻止了 NoE 和地塞米松溶液的局部抗水肿作用,分别为 NoE 61±5%和地塞米松 78±16%。重复局部应用 NoE 不会引起不良反应。

结论

我们的结果表明豆瓣菜可用于治疗皮肤炎症过程,并证明 NoE 有潜力开发出一种有前途的局部抗炎药物,用于治疗炎症性疾病。

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