Tropism-shifted AAV-PHP.eB-mediated bFGF gene 
therapy promotes varied neurorestoration after 
ischemic stroke in mice

doi:10.4103/NRR.NRR-D-23-01802

Neural Regeneration Research ›› 2026, Vol. 21 ›› Issue (2): 704-714.doi: 10.4103/NRR.NRR-D-23-01802

Tropism-shifted AAV-PHP.eB-mediated bFGF gene therapy promotes varied neurorestoration after ischemic stroke in mice

Rubing Shi1 , Jing Ye1 , Ze Liu1 , Cheng Wang1 , Shengju Wu1 , Hui Shen1 , Qian Suo1 , Wanlu Li1 , Xiaosong He2 , Zhijun Zhang1 , Yaohui Tang1 , Guo-Yuan Yang1, *, Yongting Wang1, *

1 Med-X Research Institute and School of Biomedical Engineering, Shanghai Jiao Tong University, Shanghai, China; 2 Department of Emergency, the Second Affiliated Hospital, Department of Human Anatomy, School of Basic Science, Guangzhou Medical University, Guangzhou, Guangdong Province, China

Online:2026-02-15 Published:2025-05-24
Contact: Yongting Wang, PhD, yongting.wang@gmail.com; Guo-Yuan Yang, MD, PhD, gyyang@sjtu.edu.cn.
Supported by:
This study was supported by the National Natural Science Foundation of China, Nos. 81870921 (to YW), 81974179 (to ZZ), 82271320 (to ZZ), 82071284 (to YT); National Key R&D Program of China, No. 2022YFA1603600 (to ZZ), 2019YFA0112000 (to YT); Scientific Research and Innovation Program of Shanghai Education Commission, No. 2019-01-07-00-02-E00064 (to GYY); Scientific and Technological Innovation Act Program of Shanghai Science and Technology Commission, No. 20JC1411900 (to GYY).

Abstract

Abstract: AAV-PHP.eB is an artificial adeno-associated virus (AAV) that crosses the blood–brain barrier and targets neurons more efficiently than other AAVs when administered systematically. While AAV-PHP.eB has been used in various disease models, its cellular tropism in cerebrovascular diseases remains unclear. In the present study, we aimed to elucidate the tropism of AAV-PHP.eB for different cell types in the brain in a mouse model of ischemic stroke and evaluate its effectiveness in mediating basic fibroblast growth factor (bFGF) gene therapy. Mice were injected intravenously with AAV-PHP.eB either 14 days prior to (prestroke) or 1 day following (post-stroke) transient middle cerebral artery occlusion. Notably, we observed a shift in tropism from neurons to endothelial cells with post-stroke administration of AAV-PHP.eB-mNeonGreen (mNG). This endothelial cell tropism correlated strongly with expression of the endothelial membrane receptor lymphocyte antigen 6 family member A (Ly6A). Furthermore, AAV-PHP.eB-mediated overexpression of bFGF markedly improved neurobehavioral outcomes and promoted long-term neurogenesis and angiogenesis post–ischemic stroke. Our findings underscore the significance of considering potential tropism shifts when utilizing AAV-PHP.eB-mediated gene therapy in neurological diseases and suggest a promising new strategy for bFGF gene therapy in stroke treatment.

Key words: AAV-PHP.eB, angiogenesis, basic fibroblast growth factor, gene therapy, ischemic stroke, Ly6A, neurogenesis, neurological function, transient middle cerebral artery occlusion, tropism

Rubing Shi, Jing Ye, Ze Liu, Cheng Wang, Shengju Wu, Hui Shen, Qian Suo, Wanlu Li, Xiaosong He, Zhijun Zhang, Yaohui Tang, Guo-Yuan Yang, Yongting Wang. Tropism-shifted AAV-PHP.eB-mediated bFGF gene therapy promotes varied neurorestoration after ischemic stroke in mice[J]. Neural Regeneration Research, 2026, 21(2): 704-714.

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Tropism-shifted AAV-PHP.eB-mediated bFGF gene therapy promotes varied neurorestoration after ischemic stroke in mice

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