基因治疗药物AAV5-脂蛋白脂酶变异体在小鼠体内的毒性研究

doi:10.19803/j.1672-8629.20220338

中国药物警戒 ›› 2023, Vol. 20 ›› Issue (1): 19-26.
DOI: 10.19803/j.1672-8629.20220338

• 基因治疗产品安全性评价专栏 • 上一篇下一篇

基因治疗药物AAV5-脂蛋白脂酶变异体在小鼠体内的毒性研究

侯田田¹, 马思思^2∆, 吴小兵², 霍桂桃¹, 潘东升¹, 王超¹, 夏艳², 刘艺², 周晓冰^1#, 刘国庆^2,*, 耿兴超¹

¹中国食品药品检定研究院国家药物安全评价监测中心,药物非临床安全评价研究北京市重点实验室,北京100176;
²北京锦篮基因科技有限公司,北京100176

收稿日期:2022-06-22 发布日期:2023-01-19
通讯作者: ^*刘国庆,男,博士,教授·博导,脂代谢紊乱和动脉粥样硬化研究。E-mail: liuguoqing@bj-genecradle.com
^#为共同通信作者。
作者简介:侯田田,女,硕士,助理研究员,药物临床前安全性评价。
^△为并列第一作者。
基金资助:
国家重点研发计划（2021YFA1101602）

Toxicity of gene therapy drug AAV5-LPLS447X in mice

HOU Tiantian¹, MA Sisi^2∆, WU Xiaobing², HUO Guitao¹, PAN Dongsheng¹, WANG Chao¹, XIA Yan², LIU Yi², ZHOU Xiaobing^1#, LIU Guoqing^2,*, GENG Xingchao¹

¹National Center for Safety Evaluation of Drugs, National Institutes for Food and Drug Control, Beijing Key Laboratory for Safety Evaluation of Drugs, Beijing 100176, China;
²Genecradle Therapeutics Inc, Beijing 100176, China

Received:2022-06-22 Published:2023-01-19

摘要/Abstract

摘要： 目的评估基因治疗药物AAV5-脂蛋白脂酶变异体（GC304）在小鼠体内的毒性。方法 ①急性毒性研究中,40只C57BL/6N小鼠随机分为2组,分别为溶媒组和受试物组,单次尾静脉注射后,进行连续15 d临床症状观察、体重和摄食量测定,于第15天剖检。②长期毒性研究中,440只小鼠随机分为4组,分别设置溶媒组,受试物低剂量组（1×10¹³vg·kg^-1）、中剂量组（5×10¹³ vg·kg^-1）和高剂量组（1.5×10¹⁴vg·kg^-1）,单次尾静脉注射后,对动物体重、摄食量、血液学、血清生化、免疫毒性及免疫原性等毒性指标进行测定。给药后4周和6个月时解剖,动物进行组织病理学检查,并在2、4周,3、6个月采用qPCR的方法检测GC304在动物各个脏器的分布和表达情况。结果 ①急性毒性研究中,动物临床症状、体重、摄食量未见异常,未见与GC304相关的大体病理学改变。②长期毒性研究中,动物临床症状、体重、摄食量、细胞因子和T淋巴细胞亚群未见与GC304相关的明显异常。GC304能够降低血浆中甘油三酯以及与抗药抗体相关的白蛋白/球蛋白比值下降,能够诱导抗AAV5结合抗体和中和抗体的产生,并持续至给药后6个月。给予GC304后,未检测到抗脂蛋白脂肪酶（LPL）抗体。组织病理学结果显示,小鼠给药后4周,注射部位出现与药物相关的炎性细胞浸润,至给药后6个月可见恢复。与药物相关的改变为脾脏生发中心活跃伴易染体巨噬细胞增多、腹股沟淋巴结生发中心活跃伴易染体巨噬细胞增多。qPCR检测结果显示,GC304在小鼠外周血及脏器广泛分布和表达,但在肝脏中分布和表达显著高于其他脏器。结论 C57BL/6N小鼠单次静脉给予GC304后,主要在肝脏中表达和分布,并且动物耐受性良好,未见明显毒性反应,为该药物进入临床试验提供参考。

关键词: 基因治疗, AAV5-脂蛋白脂酶变异体, 毒性研究, 小鼠

Abstract: Objective To assess the toxicity of gene therapy drug AAV5-LPLS447X (GC304) in mice. Methods ①Acute toxicity study:40 C57BL/6N mice were randomly divided into 2 groups: the vehicle group and the test substance group. After a single tail vein injection, clinical symptoms, body weight and food intake were measured for 15 consecutive days, and necropsy was performed on the 15^th day.② Long-term toxicity study: 440 mice were randomly divided into 4 groups: the vehicle group, low-dose group(1×10¹³vg·kg^-1), middle-dose group(5×10¹³ vg·kg^-1) and high-dose group(1.5×10¹⁴vg·kg^-1). After a single tail vein injection, such indicators of toxicity as body weight, food intake, hematology, serum biochemistry, immunotoxicity and immunogenicity were measured. The mice were dissected at 4 weeks and 6 months after administration before being examined histopathologically. The distribution and expression of GC304 in various organs of the animals were detected by qPCR at 2 weeks, 4 weeks, 3 months, and 6 months. Results ①In the acute toxicity study: the clinical symptoms, body weight and food intake of the animals were normal, and no gross pathological changes related to GC304 were found.② In the long-term toxicity study: no obvious abnormalities related to GC304 were found in clinical symptoms, body weight, food intake, cytokines or T lymphocyte subsets. GC304 reduced plasma triglycerides and the albumin/globulin ratio associated with anti-drug antibodies, and induced the production of anti-AAV5-binding antibodies and neutralizing antibodies, which persisted up to 6 months after administration. After administration of GC304, no anti-LPL antibodies were detected. Histopathological results showed that drug-related inflammatory cell infiltration occurred at the injection site 4 weeks after administration in mice, and recovery was seen 6 months after administration. Drug-related changes were an active germinal center in the spleen with increased predisposition macrophages, and an active germinal center in the inguinal lymph nodes with increased predisposed macrophages. The results of qPCR showed that GC304 was widely distributed and expressed in the peripheral blood and organs of mice, especially in the liver. Conclusion After a single intravenous administration in C57BL/6N mice, GC304 is mainly expressed and distributed in the liver, and the animals are well tolerated without obvious toxic reactions, which provides reference for clinical trials of the drug.

Key words: gene therapy, GC304, toxicity study, mice

中图分类号:

R965.3

侯田田, 马思思, 吴小兵, 霍桂桃, 潘东升, 王超, 夏艳, 刘艺, 周晓冰, 刘国庆, 耿兴超. 基因治疗药物AAV5-脂蛋白脂酶变异体在小鼠体内的毒性研究[J]. 中国药物警戒, 2023, 20(1): 19-26.

HOU Tiantian, MA Sisi, WU Xiaobing, HUO Guitao, PAN Dongsheng, WANG Chao, XIA Yan, LIU Yi, ZHOU Xiaobing, LIU Guoqing, GENG Xingchao. Toxicity of gene therapy drug AAV5-LPLS447X in mice[J]. Chinese Journal of Pharmacovigilance, 2023, 20(1): 19-26.

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基因治疗药物AAV5-脂蛋白脂酶变异体在小鼠体内的毒性研究

Toxicity of gene therapy drug AAV5-LPLS447X in mice

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