用于经鼻给药的厚朴挥发油:经鼻给药:木兰花挥发油的制备、特性及治疗过敏性鼻炎的作用机制》。

Qiuting Guo, Xuan Wang, Yao Wang, Peijie Zhou, Xiaofei Zhang
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引用次数: 0

摘要

背景:过敏性鼻炎(AR)是一种常见的慢性鼻部疾病,通常由过敏原引起。当人体接触过敏原时,免疫系统会做出过度反应,释放出大量组织化学物质,导致鼻塞、分泌物增多以及鼻粘膜炎症反应:在临床实践中,这仍然是一个重要的公共卫生问题。现代药理研究表明,厚朴挥发油(MVO)具有良好的抗炎、抗菌、免疫调节等药理作用。以往的研究和文献报道表明,厚朴挥发油对过敏性鼻炎有良好的治疗效果。然而,由于厚朴的水溶性较差,其生物利用度较低。本研究的目的是开发一种新的微乳剂配方,以提高厚朴的稳定性和生物利用度:结果:研究人员对厚朴挥发油微乳液(MVOME)的液滴尺寸、PDI 和 zeta 电位及其物理特性进行了表征,发现这些值分别为 14.270.03 nm、0.09410.31 和 -0.35850.12 mV,表明微乳液的形成是成功的。在 OVA 诱导的 AR 大鼠中,MVO-ME 能显著降低血清中 TNF-α、IL-1β 和 IL-6 炎症因子的水平。此外,MVO-ME 还能显著抑制 AR 大鼠鼻粘膜中 PPAR-γ 和 P65 蛋白水平的表达。因此,我们推测MVO-ME可能通过激活PPAR信号通路以及抑制NF/κB信号通路的激活,对AR起到治疗作用:结论:MVO-ME具有高溶解度、生物利用度等系统性优势。结论:MVO-ME 具有高溶解度、生物利用度等系统优势,有望成为临床治疗过敏性鼻炎的高效纳米给药系统。
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Volatile Oil of Magnolia biondii Pamp. for Transnasal Administration: Its Preparation, Characterization, and Mechanism of Action in the Treatment of Allergic Rhinitis.

Background: Allergic Rhinitis (AR) is a common chronic nasal condition usually caused by allergens. The immune system overreacts when the body is exposed to allergens, releasing a lot of tissue chemicals that cause congestion, more secretions, and an inflammatory reaction in the nasal mucosa.

Method: In clinical practice, it remains a significant public health issue. Modern pharmacological studies have demonstrated that Magnolia Volatile Oil (MVO) has good anti-inflammatory, antibacterial, immunomodulatory, and other pharmacological effects. Previous research and literature reports have reported that MVO has good therapeutic effects on allergic rhinitis. However, due to the poor water solubility of Magnolia, its bioavailability is low. The purpose of this present work is to develop a new microemulsion formulation to improve the stability and bioavailability of MVO.

Results: The droplet size, PDI, and zeta potential of Magnolia volatile oil microemulsion (MVOME) were characterized along with its physical characteristics, and these values were found to be 14.270.03 nm, 0.09410.31, and -0.35850.12 mV, respectively, demonstrating the successful formation of microemulsion. In OVA-induced AR rats, MVO-ME dramatically reduced the serum levels of TNF-α, IL-1β, and IL-6 inflammatory factors. In addition, MVO-ME significantly inhibited the expression of protein levels of PPAR-γ and P65 in the nasal mucosa of AR rats. In this regard, we hypothesized that MVO-ME may play a therapeutic role in AR by activating the PPAR signaling pathway as well as inhibiting the activation of the NF/κB signaling pathway.

Conclusion: MVO-ME has systematic advantages, such as high solubility, bioavailability, etc. It is expected to be an efficient nano-drug delivery system for the clinical treatment of allergic rhinitis.

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