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盐酸小檗碱载黏液穿透性海藻酸钠-壳聚糖纳米粒口服递送至溃疡性结肠炎炎症部位。

Mucus-Penetrating Alginate-Chitosan Nanoparticles Loaded with Berberine Hydrochloride for Oral Delivery to the Inflammation Site of Ulcerative Colitis.

机构信息

Anhui Province Key Laboratory of Pharmaceutical Technology and Application, Key Laboratory of Xin'an Medicine Ministry of Education, Anhui Province Key Laboratory of Chinese Medicinal Formula, Anhui University of Chinese Medicine, Hefei, 230038, Anhui, China.

School of Pharmacy, China Pharmaceutical University, Nanjing, 210009, Jiangsu, China.

出版信息

AAPS PharmSciTech. 2022 Jun 27;23(6):179. doi: 10.1208/s12249-022-02327-4.

DOI:10.1208/s12249-022-02327-4
PMID:35761150
Abstract

The rectal enemas of berberine hydrochloride (BH) have emerged as one of the most effective strategies in the clinical treatment of ulcerative colitis (UC). However, oral dosages of BH exhibit a poor anti-inflammatory effect of UC, which may attribute to premature absorption of BH by the upper gastrointestinal tract. Moreover, the thick colonic mucus layer obstructs the penetration of the drug, resulting in low bioavailability to the inflammatory site of the colon. The aim of this study was to develop the mucus-penetrating sodium alginate-chitosan nanoparticles (SA-CS NPs) for oral delivery of BH to the site of colonic ulcer lesions. BH-loaded SA-CS NPs were developed through the ionic gelation method and analyzed for physicochemical characteristics, release performance, penetrability, site retention, and therapeutic efficacy. The results showed that the NPs have a particle size of 257 nm with a negative charge, presenting desired pH-dependent release behavior. The permeation studies elucidated that negatively charged SA-CS NPs had 2.9 times higher mucus penetration ability than positively charged CS NPs. An ex vivo retention study indicated the high retention of BH-SA-CS NPs at the colon site for more than 16 h. In vivo therapeutic effectiveness demonstrated that the prepared NPs could not only alleviate colonic injury by decreasing the disease activity index and colon mucosa damage index, but also improve the immunologic function by decreasing the spleen index. In conclusion, the BH-SA-CS NPs could enhance the mucus permeability and deliver drugs to the colonic inflammation site, providing new insights into improving the therapeutic effect of UC.

摘要

盐酸小檗碱(BH)直肠给药已成为溃疡性结肠炎(UC)临床治疗中最有效的策略之一。然而,BH 的口服剂量对 UC 的抗炎效果不佳,这可能归因于 BH 在上消化道的过早吸收。此外,厚厚的结肠黏液层阻碍了药物的渗透,导致药物对结肠炎症部位的生物利用度较低。本研究旨在开发穿透黏液的海藻酸钠-壳聚糖纳米粒子(SA-CS NPs),用于 BH 口服递送至结肠溃疡病变部位。通过离子凝胶法制备 BH 负载的 SA-CS NPs,并对其理化特性、释放性能、穿透性、部位保留和治疗效果进行分析。结果表明, NPs 的粒径为 257nm,带负电荷,呈现出理想的 pH 依赖性释放行为。渗透研究表明,带负电荷的 SA-CS NPs 的黏液穿透能力比带正电荷的 CS NPs 高 2.9 倍。离体保留研究表明,BH-SA-CS NPs 在结肠部位的保留时间超过 16 小时。体内治疗效果表明,所制备的 NPs 不仅可以通过降低疾病活动指数和结肠黏膜损伤指数来减轻结肠损伤,还可以通过降低脾脏指数来改善免疫功能。综上所述,BH-SA-CS NPs 可以增强黏液的渗透性,并将药物递送至结肠炎症部位,为提高 UC 的治疗效果提供了新的思路。

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