AI Article Synopsis

  • This study investigates how adeno-associated virus (AAV) enters cells and reaches the nucleus, which is crucial for its use in gene therapy.
  • Researchers conducted genome-wide screens in U-2 OS cells with AAV2 to identify genes that affect AAV transduction efficiency.
  • They identified specific genes that either enhance or inhibit AAV transduction, with one gene, GPR108, playing a key role in the viral trafficking process and showing selectivity for certain AAV serotypes.

Article Abstract

Adeno-associated virus (AAV) has been used extensively as a vector for gene therapy. Despite its widespread use, the mechanisms by which AAV enters the cell and is trafficked to the nucleus are poorly understood. In this study, we performed two pooled, genome-wide screens to identify positive and negative factors modulating AAV2 transduction. Genome-wide libraries directed against all human genes with four designs per gene or eight designs per gene were transduced into U-2 OS cells. These pools were transduced with AAV2 encoding EGFP and sorted based on the intensity of EGFP expression. Analysis of enriched and depleted barcodes in the sorted samples identified several genes that putatively decreased AAV2 transduction. A subset of screen hits was validated in flow cytometry and imaging studies. In addition to (), we confirmed the role of two genes, and , in mediating viral transduction in eight different AAV serotypes. Interestingly, displayed serotype selectivity and was not required for AAV5 transduction. Follow-up studies suggested that GPR108 localized primarily to the Golgi, where it may interact with AAV and play a critical role in mediating virus escape or trafficking. Cumulatively, these results expand our understanding of the process of AAV transduction in different cell types and serotypes.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7139131PMC
http://dx.doi.org/10.1016/j.omtm.2020.03.012DOI Listing

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