Abstract

Human bocavirus 1 (HBoV1), an autonomous parvovirus, is a helper virus supporting replication of wild-type adeno-associated virus 2 (AAV2). In this study, we compared the helper functions from HBoV1 with those from adenovirus (Ad) for the production of recombinant AAV (rAAV) vector in HEK293 cells. We demonstrated that triple plasmids transfection of (1) a cloned HBoV1 helper minigenome (pBocaHelper) that expresses HBoV1 genes NP1, NS2, and BocaSR, (2) pAAV transfer plasmid, and (3) pAAVRepCap supports rAAV production in HEK293 cells. Despite a production yield of 1–2 log lower than that using pAdHelper (expressing Ad genes E2A, E4, and VA), rAAV vector produced using pBocaHelper transduced cells as efficiently as that produced using pAdHelper. The low vector production is largely due to the inefficient expression of the AAV Rep52 and capsid proteins, as well as reduced rAAV genome replication. When the AAV capsid proteins and Rep52 were ectopically expressed under strong promoters, the enhanced protein expression significantly improved the rAAV production using pBocaHelper, approaching a level of 50%–70% of that produced using pAdHelper. Through further dissection of the helper functions from pAdHelper in a five-plasmid transfection system, we found that the addition of the Ad E2A gene to the above HBoV1 helper system significantly increased rAAV DNA replication, which increased the rAAV vector production to a level of 3–7 times higher than that using pAdHelper. We finally combined HBoV1 NP1 and NS2 genes with Ad helper genes to create a novel dual helper plasmid (pABHelper) for rAAV vector production in the conventional three-plasmid transfection system. The pABHelper facilitated rAAV production at a yield ∼2 times higher than that using the pAdHelper.

Highlights

  • Adeno-associated viruses (AAVs) are members of the genus Dependoparvovirus of the family Parvoviridae.[1]

  • human bocavirus 1 (HBoV1) Helper Facilitates recombinant AAV (rAAV) Vector Production We have previously found that HBoV1 helped WT associated virus 2 (AAV2) replication during co-infection in polarized human airway epithelia and that NP1, NS2, and BocaSR genes were identified as the HBoV1 helper genes for full replication of AAV2 in HEK293 cells.[30]

  • To test the helper function of pBocaHelper in supporting rAAV production by transfection, HEK293 cells were co-transfected with pBocaHelper, a rAAV2 transgene plasmid that hosts mCherry and luciferase expression cassettes flanked by two AAV2 inverted terminal repeats (ITRs), and an AAV helper plasmid pAAVRep2Cap[2] or pAAVRep2Cap[5]

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Summary

Introduction

Adeno-associated viruses (AAVs) are members of the genus Dependoparvovirus of the family Parvoviridae.[1]. Direct capsid evolution and rational capsid design have greatly increased the diversity of AAV capsids with improved specificity, efficiency, and escape of neutralizing antibodies.[7,8] Despite the cross-package of rAAV2 genome by AAV serotypes or variants, it can be packaged cross-genus efficiently, for example, with the capsid of human bocavirus 1 (HBoV1),[9] which extends the toolbox of AAV capsid variants further

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