1. Low incidence of hepatocellular carcinoma in mice and cats treated with systemic adeno-associated viral vectors
- Author
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Zelin Chen, Charles P. Venditti, John M. Cullen, Ping Wang, Stephanie Smith, Rita Ferla, Tyra G. Wolfsberg, Anh-Dao Nguyen, Alberto Auricchio, Randy J. Chandler, Shawn M. Burgess, Mark E. Haskins, Margherita Dell’Anno, Charles H. Vite, Patricia O'Donnell, Marialuisa Alliegro, Edoardo Nusco, Ferla, R., Alliegro, M., Dell'Anno, M., Nusco, E., Cullen, J. M., Smith, S. N., Wolfsberg, T. G., O'Donnell, P., Wang, P., Nguyen, A. -D., Chandler, R. J., Chen, Z., Burgess, S. M., Vite, C. H., Haskins, M. E., Venditti, C. P., and Auricchio, A.
- Subjects
0301 basic medicine ,lcsh:QH426-470 ,insertional mutagenesi ,Genetic enhancement ,viruses ,Mucopolysaccharidosis type VI ,MPS VI ,medicine.disease_cause ,liver ,Viral vector ,03 medical and health sciences ,0302 clinical medicine ,Genetics ,Medicine ,cancer ,Vector (molecular biology) ,lcsh:QH573-671 ,lysosomal storage diseases ,Molecular Biology ,mouse ,business.industry ,lcsh:Cytology ,Cancer ,HCCS ,medicine.disease ,gene therapy ,lcsh:Genetics ,030104 developmental biology ,lysosomal storage disease ,age ,030220 oncology & carcinogenesis ,Hepatocellular carcinoma ,Cancer research ,insertional mutagenesis ,Molecular Medicine ,Original Article ,AAV8 ,business ,Carcinogenesis - Abstract
Adeno-associated viral (AAV) vectors have emerged as the preferred platform for in vivo gene transfer because of their combined efficacy and safety. However, insertional mutagenesis with the subsequent development of hepatocellular carcinomas (HCCs) has been recurrently noted in newborn mice treated with high doses of AAV, and more recently, the association of wild-type AAV integrations in a subset of human HCCs has been documented. Here, we address, in a comprehensive, prospective study, the long-term risk of tumorigenicity in young adult mice following delivery of single-stranded AAVs targeting liver. HCC incidence in mice treated with therapeutic and reporter AAVs was low, in contrast to what has been previously documented in mice treated as newborns with higher doses of AAV. Specifically, HCCs developed in 6 out 76 of AAV-treated mice, and a pathogenic integration of AAV was found in only one tumor. Also, no evidence of liver tumorigenesis was found in juvenile AAV-treated mucopolysaccharidosis type VI (MPS VI) cats followed as long as 8 years after vector administration. Together, our results support the low risk of tumorigenesis associated with AAV-mediated gene transfer targeting juvenile/young adult livers, although constant monitoring of subjects enrolled in AAV clinical trial is advisable., Graphical Abstract, Systemic delivery of high doses of adeno-associated viral (AAV) vectors causes insertional mutagenesis and hepatocellular carcinomas in newborn mice. The study shows that this risk is lower in young adult mice and juvenile cats using AAV doses similar to those used in many clinical applications.
- Published
- 2020