| Literature DB >> 30772143 |
Caitlin M Guenther1, Mitchell J Brun2, Antonette D Bennett3, Michelle L Ho1, Weitong Chen2, Banghe Zhu4, Michael Lam1, Momona Yamagami1, Sunkuk Kwon4, Nilakshee Bhattacharya5, Duncan Sousa5, Annicka C Evans1, Julie Voss4, Eva M Sevick-Muraca4, Mavis Agbandje-McKenna3, Junghae Suh6.
Abstract
Adeno-associated virus (AAV) has emerged as a promising gene delivery vector because of its non-pathogenicity, simple structure and genome, and low immunogenicity compared to other viruses. However, its adoption as a safe and effective delivery vector for certain diseases relies on altering its tropism to deliver transgenes to desired cell populations. To this end, we have developed a protease-activatable AAV vector, named provector, that responds to elevated extracellular protease activity commonly found in diseased tissue microenvironments. The AAV9-based provector is initially inactive, but then it can be switched on by matrix metalloproteinases (MMP)-2 and -9. Cryo-electron microscopy and image reconstruction reveal that the provector capsid is structurally similar to that of AAV9, with a flexible peptide insertion at the top of the 3-fold protrusions. In an in vivo model of myocardial infarction (MI), the provector is able to deliver transgenes site specifically to high-MMP-activity regions of the damaged heart, with concomitant decreased delivery to many off-target organs, including the liver. The AAV provector may be useful in the future for enhanced delivery of transgenes to sites of cardiac damage.Entities:
Keywords: AAV; activatable; adeno-associated virus; cardiac gene therapy; gene delivery; gene therapy; inflammation targeting; matrix metalloproteinase; myocardial infarction; provector; stimulus responsive; viral vector
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Year: 2019 PMID: 30772143 PMCID: PMC6404099 DOI: 10.1016/j.ymthe.2019.01.015
Source DB: PubMed Journal: Mol Ther ISSN: 1525-0016 Impact factor: 11.454