The Biodistribution of Replication-Defective Simian Adenovirus 1 Vector in a Mouse Model
Juan Chen, Xiaojuan Guo, Xiaohui Zou, Min Wang, Chunlei Yang, Wenzhe Hou, Matvey V. Sprindzuk, Zhuozhuang Lu

TL;DR
This study examines how different administration routes affect the biodistribution and transgene expression of a simian adenovirus vector in mice.
Contribution
The study identifies optimal administration routes for a novel simian adenovirus vector in vaccine development.
Findings
Intravenous administration targets liver and spleen macrophages and hepatocytes.
Intranasal administration allows repeated use with moderate respiratory tract expression.
Intramuscular injection shows sustained expression but requires a switch to HAdV-5 for recovery after repeated use.
Abstract
The administration route affects the biodistribution of a gene transfer vector and the expression of a transgene. A simian adenovirus 1 vector carrying firefly luciferase and GFP reporter genes (SAdV1-GFluc) were constructed, and its biodistribution was investigated in a mouse model by bioluminescence imaging and virus DNA tracking with real-time PCR. Luciferase activity and virus DNA were mainly found in the liver and spleen after the intravenous administration of SAdV1-GFluc. The results of flow cytometry illustrated that macrophages in the liver and spleen as well as hepatocytes were the target cells. Repeated inoculation was noneffective because of the stimulated serum neutralizing antibodies (NAbs) against SAdV-1. A transient, local expression of low-level luciferase was detected after intragastric administration, and the administration could be repeated without compromising the…
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Taxonomy
TopicsVirus-based gene therapy research · Viral Infectious Diseases and Gene Expression in Insects · CAR-T cell therapy research
