Wilson's disease (WD) is an autosomal recessive disorder caused by pathogenic variants in the ATP7B gene, resulting in the toxic accumulation of copper (Cu). Impaired Cu homeostasis in WD is characterized by low serum ceruloplasmin, excess hepatic Cu, and elevated urinary Cu. WD often presents with hepatic and/or neurological diseases and is fatal if untreated. Adeno-associated virus (AAV)-mediated gene therapy holds promise for WD, but challenges remain in efficacy and safety. Here, we established an Atp7b R780L knockin (KI) mouse model corresponding to the human ATP7B R778L variant and investigated the therapeutic efficacy and safety of liver-targeted AAV8-mediated ATP7B (AAV8-ÎC4ATP7B) gene therapy in this model. The results demonstrated the Atp7b (KI/KI) mice recapitulated key features of impaired Cu metabolism in WD but had mild liver disease. Ten-week-old Atp7b (KI/KI) mice received a single-dose of AAV8-ÎC4ATP7B and were sacrificed at 8 or 30Â weeks after treatment. Treated Atp7b (KI/KI) mice showed normalization of serum ceruloplasmin, reduced hepatic Cu, decreased urinary Cu, and reversed liver histopathology. Serum transaminases had a transient increase at 8Â weeks after treatment but returned to normal at 30Â weeks after treatment. These data provide evidence for the efficacy and safety of AAV8-ÎC4ATP7B in animals, supporting clinical translation to patients with WD.
Evaluation of efficacy and safety of AAV8-ÎC4ATP7B gene therapy in a mutant mouse model of Wilson's disease.
在威尔逊病突变小鼠模型中评估 AAV8-ΔC4ATP7B 基因疗法的疗效和安全性
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作者:Zeng Chunhua, Lin Yunting, Lu Xinshuo, Chen Shehong, Xia Yan, Zhang Kangdi, Shao Yongxian, Guan Zhihong, Du Rong, Liu Zongcai, Zhao Mingqi, Jiang Xiaoling, Cai Yanna, Li Taolin, Su Xueying, Chen Yaoyong, Dong Xiaoyan, Zhang Wen, Liu Li, Zhou Wenhao
| 期刊: | Molecular Therapy-Methods & Clinical Development | 影响因子: | 4.700 |
| 时间: | 2025 | 起止号: | 2025 Feb 13; 33(1):101435 |
| doi: | 10.1016/j.omtm.2025.101435 | 种属: | Mouse |
| 研究方向: | 其它 | ||
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