蒿芩滴鼻剂安全性评价研究

doi:10.19803/j.1672-8629.20260238

中国药物警戒 ›› 2026, Vol. 23 ›› Issue (6): 656-662.
DOI: 10.19803/j.1672-8629.20260238

蒿芩滴鼻剂安全性评价研究

何韬¹, 王新堂^1Δ, 颜玉文², 刘燕¹, 程江南¹, 顾政一¹, 毛艳^1,*

¹新疆维吾尔自治区药物研究院,新疆维吾尔药重点实验室,新疆乌鲁木齐 830010;
²苏州华测生物技术有限公司,江苏苏州 215300

收稿日期:2026-03-25 出版日期:2026-06-15 发布日期:2026-06-18
通讯作者: ^*毛艳,女,硕士,研究员·硕导,中药新药研发与质量控制。E-mail: maoyan7529@163.com
作者简介:何韬,男,硕士,助理研究员,中药新药研究与开发。^Δ为并列第一作者。
基金资助:
新疆维吾尔自治区重大科技专项项目（2021A03002-1）; 新疆维吾尔自治区自然科学基金资助项目（2021D01E25）; “天山英才”医药卫生高层次人才培养计划项目（TSYC202401B034）

Safety Assessment of Haoqin Nasal Drops

HE Tao¹, WANG Xintang^1Δ, YAN Yuwen², LIU Yan¹, CHENG Jiangnan¹, GU Zhengyi¹, MAO Yan^1,*

¹Xinjiang Institute of Materia Medica, Key Laboratory of Xinijang Uygur Medicine, Urumqi Xinjiang 830010, China;
²CTI Biotechnology (Suzhou) Co., Ltd, Suzhou Jiangsu 215300, China

Received:2026-03-25 Online:2026-06-15 Published:2026-06-18

摘要/Abstract

摘要： 目的观察蒿芩滴鼻剂大鼠单次给药和13周重复给药可能出现的毒性反应,为其临床试验及临床安全用药提供参考。方法单次给药毒性试验中,大鼠给予最大给药体积（0.4 mL·kg^-1）、最大给药剂量（1 440 mg生药·kg^-1）的蒿芩滴鼻剂,观察14 d内的一般状态、体重及摄食量、毒性症状及死亡情况,并对主要组织脏器进行组织病理学检查;重复给药毒性试验中,蒿芩滴鼻剂低、中、高剂量组大鼠分别给予67.5、135.0、270.0 mg生药·kg^-1 13周,每天观察大鼠一般状态,每周称量体重,分别于给药13周及停药后4周,检测指标包括血液学指标、凝血指标、血液生化指标、尿液指标、脏器系数及组织病理学检查。结果单次给药毒性试验中,大鼠的一般状态、体重及摄食量等指标均无异常;13周重复给药毒性试验中,与溶媒对照组比,给药期结束,部分给药组的个别指标如红细胞和平均红细胞血红蛋白浓度、网织红细胞、血红蛋白、红细胞比积和尿素等具有统计学差异,但属正常范围波动。高剂量组1例雄性肝脏肝细胞空泡变、1例雌性动物骨髓造血干细胞轻微减少,结合血液生化等指标的检测结果,考虑为大鼠的自发性病变。结论蒿芩滴鼻剂单次给药的最大耐受量（MTD）为1 440 mg生药·kg^-1（约为400倍临床拟用剂量）,13周重复给药的无毒反应剂量（NOAEL）为270 mg生药·kg^-1（约为75倍临床拟用剂量）,表明该药在拟临床使用剂量范围及疗程内未见明显的毒性反应,在治疗剂量范围内安全性较高,可为该药进一步开展临床试验提供参考。

关键词: 蒿芩滴鼻剂, 单次给药, 重复给药, 最大耐受量, 无毒反应剂量, 安全性评价, 大鼠

Abstract: Objective To assess the safety of Haoqin nasal drops and provide a reference for safe clinical medications for allergic rhinitis (AR). Methods In single-dose toxicity test, SD rats were administered with the maximum tolerated dose (0.4 mL·kg^-1) of Haoqin nasal drops, which was equivalent to 1440 mg crude drug/kg. The overall state, body weight, food intake, toxic symptoms, and mortality of these rats were observed over a period of 14 days, followed by histopathological examination of major tissues and organs. In the repeated dose toxicity test, SD rats were divided into high-dose(270.0 mg·kg^-1), medium-dose (135.0 mg·kg^-1), low-dose(67.5 mg·kg^-1) groups and a control group, with 30 rats in each. The rats were administered with this drug for 13 weeks, followed by 4 weeks of recovery. The overall state of these rats was observed daily while their body weight was measured weekly. Such indexes were recorded as parameters of hematology, coagulation and blood biochemistry, urine indexes, organ coefficients and results of histopathological examination. Results In the single-dose toxicity test, the overall state, body weight, food intake and other indicators of rats were normal. In the repeated-dose toxicity test, some of the indicators of the medication group, such as red blood cell count and the average hemoglobin concentration of red blood cells, reticulocytes, hemoglobin, hematocrit and urea at the end of the dosing period, were statistically different from those of the control group, but within the normal range of fluctuation. In the high-dose group, there was one case of male hepatocyte vacuolation and one case of a slight decrease in female bone marrow hematopoietic stem cells. The two cases were considered a spontaneous disease in rats based on blood biochemical indicators. Conclusion The MTD of Haoqin nasal drops is 1440 mg crude drug/kg (equivalent to 400 times the intended clinical dose) for a single administration, and the NOAEL for the 13-week repeated doses is 270 mg crude drug/kg (equivalent to 75 times the intended clinical dose). Haoqin nasal drops show no significant toxicity and prove quite safe at therapeutic dosages.

Key words: Haoqin Nasal Drops, Single Administration, Repeated Administration, MTD, NOAEL, Safety Assessment, Rats

中图分类号:

R282
R994.11

何韬, 王新堂, 颜玉文, 刘燕, 程江南, 顾政一, 毛艳. 蒿芩滴鼻剂安全性评价研究[J]. 中国药物警戒, 2026, 23(6): 656-662.

HE Tao, WANG Xintang, YAN Yuwen, LIU Yan, CHENG Jiangnan, GU Zhengyi, MAO Yan. Safety Assessment of Haoqin Nasal Drops[J]. Chinese Journal of Pharmacovigilance, 2026, 23(6): 656-662.

导出引用管理器 EndNote|Ris|BibTeX

链接本文: https://zgywjj.magtechjournal.com/CN/10.19803/j.1672-8629.20260238

https://zgywjj.magtechjournal.com/CN/Y2026/V23/I6/656

参考文献

[1] CZECH EJ, OVERHOLSER A, SCHULTZ P.Allergic Rhinitis[J]. Med Clin North Am, 2024, 108(4): 609-628.
[2] PONDA P, CARR T, RANK MA, et al.Nonallergic Rhinitis, Allergic Rhinitis, and Immunotherapy: Advances in the Last Decade[J]. J Allergy Clin Immunol Pract, 2023, 11(1): 35-42.
[3] CZECH EJ, OVERHOLSER A, SCHULTZ P.Allergic Rhinitis[J]. Prim Care, 2023, 50(2): 159-178.
[4] VOELKER R.What Is Allergic Rhinitis?[J]. JAMA: Journal of the American Medical Association, 2024, 332(19): 1682.
[5] ADINA·ABDULAINI, MAO Y, ZHANG SR. Predictive Analysis of Quality Markers of Artemisia rupestris L. from Xinjiang[J]. Pharmacology and Clinics of Chinese Materia Medica(中药药理与临床), 2025, 41(8): 106-114.
[6] CHENG JN, DING M, CAI XC, et al.Study on the “Spectrum-Effect” Relationship of Anti-Hepatitis B Virus Effect in vitro of Different Polarity Extracts of Artemisia rupestris L. from Xinjiang[J]. Central South Pharmacy(中南药学), 2025, 23(12): 3528-3533.
[7] DONG XH, GU ZY, HUANG H, et al.Experimental Study on the Efficacy of Gaoqin Nasal Drops in Rats with Allergic Rhinitis[J]. Journal of Xinjiang Medical University(新疆医科大学学报), 2013, 36(3): 320-324.
[8] GULIBAIREMU·YUSUYIN, TANG CF, MUHETAER·ABDUREHEMU, et al. Effects of Compound Yizhihao Nasal Drops on Inflammatory and Immune Factors in Mice with Allergic Rhinitis[J]. Journal of Xinjiang Medical University(新疆医科大学学报), 2020, 43(7): 951-956.
[9] HE T, MAO Y, GU ZY.Exploration on the Mechanism of Qinhao Nasal Drops in the Treatment of Allergic Rhinitis Based on Network Pharmacology and Molecular Docking[J]. Chinese Journal of Information on Traditional Chinese Medicine(中国中医药信息杂志), 2021, 28(7): 21-26.
[10] NMPA. Good Laboratory Practice for Nonclinical Drug Studies (Order No. 34 of the China Food and Drug Administration)[EB/OL]. (2017-07-27)[2026-05-01]. https://www.nmpa.gov.cn/yaopin/ypfgwj/ypfgbmgzh/20170802160401550.html.
[11] CDE, NMPA. Technical Guidelines for Single Dose Toxicity Study of Drugs[EB/OL]. (2014-05-13)[2026-05-01]. https://www.cde.org.cn/zdyz/domesticinfopage?zdyzIdCODE=0c935796de664b377759b4dcb6a2634c.
[12] NMPA. Technical Guidelines for Sample Research in Toxicological Studies of New Traditional Chinese Medicines (Trial)[EB/OL]. (2022-01-04)[2026-05-01]. http://www.nmpa.gov.cn/directory/web/nmpa/yaopin/ypggtg/20220107174107185.html.
[13] CDE, NMPA. Technical Guidelines for Toxicity Studies of Drug Repeated Administration[EB/OL]. (2014-05-13)[2026-05-01]. https://www.cde.org.cn/zdyz/domesticinfopage?zdyzIdCODE=eb1121e208d156f8fb0384d1e77edb8f.
[14] ZHANG HT, LI YL, LI L, et al.Toxicity Study of Single and Repeated Administration of Guishao Zichuan Formula[J]. Chinese Journal of Pharmacovigilance(中国药物警戒), 2025, 22(5): 547-553, 569.
[15] WANG YF, LIU H, SHUHELA・ZHUMABIEKE, et al. Safety Evaluation Study of Bushi Bitong Pills[J]. Chinese Journal of Pharmacovigilance(中国药物警戒), 2026, 23(4): 432-437.
[16] DING HX, TANG XM.FDA Pharmacology and Toxicology Guidelines(FDA药物毒理学与毒理学指南)[M]. Beijing: China Medical Science and Technology Press, 2018.

蒿芩滴鼻剂安全性评价研究

Safety Assessment of Haoqin Nasal Drops

PDF (PC)

可视化

摘要/Abstract

引用本文

使用本文

参考文献

相关文章 15

编辑推荐

Metrics

[1]	王子未, 李艳君, 黄力, 刘呈祥, 肖响, 杨德爽, 王金平, 乔佳君, 白雪, 李琳. 鹿茸对心肌梗死模型大鼠心肌细胞凋亡及Bcl-2/Bax/Caspase蛋白表达的影响[J]. 中国药物警戒, 2026, 23(6): 613-620.
[2]	李艳君, 刘呈祥, 汤波, 柳翼, 张久亮, 姜国臣, 白雪. 补土汤激活AKT/Bcl-2信号轴抑制心肌细胞凋亡改善大鼠心力衰竭机制研究[J]. 中国药物警戒, 2026, 23(6): 621-629.
[3]	庄杰, 綦梦洁, 杨世婕, 翟晨斐, 牛剑钊, 许风国, 刘倩. 高效液相色谱法测定乙醇对阿司匹林肠溶片体外释放行为的影响[J]. 中国药物警戒, 2026, 23(6): 636-642.
[4]	秦昭恒, 李珍地, 李亚娟, 尹纪业. 清疫胶囊对大鼠非临床安全性评价[J]. 中国药物警戒, 2026, 23(6): 649-655.
[5]	张媛, 郭龙静, 杨泽岸, 贺庆, 王宏宇, 吴彦霖, 纳涛. 垂体后叶中活性成分测定方法的替代研究[J]. 中国药物警戒, 2026, 23(5): 533-538.
[6]	陈熙泰, 马增春, 张娴勰, 戚凌, 李芳, 陈丽苹, 拓艳玲, 李舒曼, 高亮. 高原睡眠障碍动物模型的构建与评价研究进展[J]. 中国药物警戒, 2026, 23(4): 368-374.
[7]	戚凌, 张娴勰, 陈熙泰, 黄天科, 李芳, 陈丽苹, 拓艳玲, 马增春. 高原日间功能障碍痰浊蒙窍证动物模型的构建与评价[J]. 中国药物警戒, 2026, 23(4): 375-382.
[8]	于蔚洁, 刘雨欣, 林瑞超, 李向日, 赵崇军. 基于斑马鱼模型的重楼不同制备样本肝毒性比较和评价[J]. 中国药物警戒, 2026, 23(4): 390-397.
[9]	郑海云, 王瑞芬, 熊婕, 赵飞, 王斌, 余文. 基于UPLC-Q Exactive Orbitrap HRMS的归脾安眠汤体内外化学成分分析[J]. 中国药物警戒, 2026, 23(4): 414-419.
[10]	王云飞, 刘欢, 舒合拉·朱马别克, 帕依曼·亥米提, 于宁. 补肾痹通丸安全性评价研究[J]. 中国药物警戒, 2026, 23(4): 432-437.
[11]	罗强, 邓彬, 熊慧瑜, 王春婷, 黄彦, 刘佐仁. 儿童用药安全性评价指标体系构建探索[J]. 中国药物警戒, 2026, 23(3): 285-289.
[12]	李娜, 姚魁武. 通心舒胶囊对心肌梗死大鼠心脏炎症微环境及心肌细胞凋亡的影响[J]. 中国药物警戒, 2026, 23(2): 141-146.
[13]	杜建才, 姚方方, 刘若训, 赵云, 李国超, 仇德洋, 李斌, 姚景春. 新利司他杂质A大鼠90 d重复灌胃给药毒性研究[J]. 中国药物警戒, 2026, 23(2): 147-154.
[14]	任中杰, 魏明慧, 尹东杰, 郭颖, 鲁子瑜, 于洋, 郭玉婷, 张欣, 刘芳冰, 张佳茹, 王敏杰, 薛明明. 基于组织非靶向代谢组学探究四味土木香散治疗高血压性心肌肥厚的作用机制[J]. 中国药物警戒, 2026, 23(1): 42-49.
[15]	吴美晶, 徐向楠, 刘晓庆, 于雪, 钟赣生, 修琳琳. 海藻-甘草配伍对甲状腺肿大大鼠JNK1/Bcl-2/Beclin1通路表达的影响[J]. 中国药物警戒, 2026, 23(1): 55-62.