Department of Pharmaceutical Sciences, School of Pharmacy and Pharmaceutical Sciences, The State University of New York at Buffalo, USA.
Biologic Therapeutics, Antibody Discovery and Protein Engineering, R&D, AstraZeneca, Cambridge, UK.
J Pharm Sci. 2024 Jan;113(1):131-140. doi: 10.1016/j.xphs.2023.08.023. Epub 2023 Sep 1.
Recombinant adeno-associated viruses(rAAVs) are an attractive tool to ensure long-term expression monoclonal antibody(mAb) in the central nervous system(CNS). It is still unclear whether systemic injection or local CNS administration of AAV9 is more beneficial for the exposure of the expressed mAb in the brain. Hence, we compared the biodistribution and transgene expression following AAV9-Trastuzumab administration through different routes.
In-house generated AAV9-Trastuzumab vectors were administered at 5E+11 Vgs/rat through intravenous(IV), intracerebroventricular(ICV), intra-cisterna magna(ICM) and intrastriatal(IST) routes. Vector and trastuzumab blood/plasma concentrations were assessed at different time points up to the terminal time point of 21 days. Different brain regions in addition to the spinal cord, cerebrospinal fluid(CSF) and interstitial fluid(ISF), were also analyzed at the terminal time point. Our results show that vector biodistribution and Trastuzumab expression in the brain could the ranked as follows: IST>ICM>ICV>IV. Rapid clearance of vector was observed after administration via the ICM and ICV routes. The ICV route produced similar expression levels across different brain regions, while the ICM route had better expression in the hindbrain and spinal cord region. The IST route had higher expression in the forebrain region compared to the hindbrain region. A sharp decline in trastuzumab plasma concentration was observed across all routes of administration due to anti-trastuzumab antibody response.
In this study we have characterized vector biodistribution and transgene mAb expression after AAV9 vector administration through different routes in rats. IST and ICM represent the best administration routes to deliver antibody genes to the brain.
重组腺相关病毒(rAAV)是确保单克隆抗体(mAb)在中枢神经系统(CNS)中长期表达的一种有吸引力的工具。目前尚不清楚全身注射或局部 CNS 给予 AAV9 哪种方式更有利于 mAb 在大脑中的表达。因此,我们比较了通过不同途径给予 AAV9-曲妥珠单抗后其在体内的分布和转基因表达。
本研究中使用的 AAV9-曲妥珠单抗载体通过静脉(IV)、脑室内(ICV)、脑池内(ICM)和纹状体内(IST)途径,以 5E+11 Vgs/大鼠的剂量给药。在不同时间点评估载体和曲妥珠单抗的血/血浆浓度,直至 21 天的终末时间点。除了脊髓、脑脊液(CSF)和间质液(ISF)之外,还在终末时间点分析了不同的脑区。结果显示,载体在脑中的分布和曲妥珠单抗的表达可按如下顺序排列:IST>ICM>ICV>IV。通过 ICM 和 ICV 途径给药后,载体迅速清除。ICV 途径在不同脑区产生相似的表达水平,而 ICM 途径在后脑和脊髓区域具有更好的表达。与后脑区域相比,IST 途径在前脑区域具有更高的表达。由于抗曲妥珠单抗抗体的反应,所有给药途径的曲妥珠单抗血浆浓度均迅速下降。
本研究通过不同途径在大鼠中对 AAV9 载体给药后的载体分布和转基因 mAb 表达进行了特征描述。IST 和 ICM 是将抗体基因递送至大脑的最佳给药途径。
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