Novel Chimeric Gene Therapy Vectors Based on Adeno-Associated Virus and Four Different Mammalian Bocaviruses

被引:40
作者
Fakhiri, Julia [1 ,2 ]
Schneider, Marc A. [3 ,4 ]
Puschhof, Jens [5 ,6 ]
Stanifer, Megan [1 ,7 ]
Schildgen, Verena [8 ]
Holderbach, Stefan [1 ,2 ]
Voss, Yannik [1 ,2 ]
El Andari, Jihad [1 ,2 ]
Schildgen, Oliver [8 ]
Boulant, Steeve [1 ,7 ]
Meister, Michael [3 ,4 ]
Clevers, Hans [5 ,6 ,9 ,10 ]
Yan, Ziying [11 ]
Qiu, Jianming [12 ]
Grimm, Dirk [1 ,2 ,13 ]
机构
[1] Heidelberg Univ Hosp, Dept Infect Dis Virol, BioQuant BQ0030,Neuenheimer Feld 267, D-69120 Heidelberg, Germany
[2] Heidelberg Univ, BioQuant Ctr, Heidelberg, Germany
[3] Heidelberg Univ Hosp, Thoraxklin, Translat Res Unit, Heidelberg, Germany
[4] Translat Lung Res Ctr Heidelberg TLRC, German Ctr Lung Res DZL, Heidelberg, Germany
[5] Royal Netherlands Acad Arts & Sci KNAW, Hubrecht Inst, Utrecht, Netherlands
[6] Royal Netherlands Acad Arts & Sci KNAW, Oncode Inst, Utrecht, Netherlands
[7] German Canc Res Ctr, Res Grp Cellular Polar Viral Infect, Heidelberg, Germany
[8] Hosp Private Univ Witten Herdecke, Kliniken Stadt Koln GGmbH, Inst Pathol, Cologne, Germany
[9] UMC Utrecht, Utrecht, Netherlands
[10] Princess Maxima Ctr, Utrecht, Netherlands
[11] Univ Iowa, Dept Anat & Cell Biol, Ctr Gene Therapy, Iowa City, IA USA
[12] Univ Kansas, Med Ctr, Dept Microbiol Mol Genet & Immunol, Kansas City, KS 66103 USA
[13] German Ctr Infect Res DZIF, Partner Site Heidelberg, Heidelberg, Germany
基金
欧盟地平线“2020”;
关键词
HIGH-EFFICIENCY TRANSDUCTION; HUMAN PARVOVIRUS B19; PACKAGING CAPACITY; IN-VITRO; IMMUNE-RESPONSES; VIRAL VECTORS; AAV2; VECTORS; INFECTION; HUMAN-CELLS; EXPRESSION;
D O I
10.1016/j.omtm.2019.01.003
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
Parvoviruses are highly attractive templates for the engineering of safe, efficient, and specific gene therapy vectors, as best exemplified by adeno-associated virus (AAV). Another candidate that currently garners increasing attention is human bocavirus 1 (HBoV1). Notably, HBoV1 capsids can cross-package recombinant (r) AAV2 genomes, yielding rAAV2/HBoV1 chimeras that specifically transduce polarized human airway epithelia (pHAEs). Here, we largely expanded the repertoire of rAAV/BoV chimeras, by assembling packaging plasmids encoding the capsid genes of four additional primate bocaviruses, HBoV2-4 and GBoV (Gorilla BoV). Capsid protein expression and efficient rAAV cross-packaging were validated by immunoblotting and qPCR, respectively. Interestingly, not only HBoV1 but also HBoV4 and GBoV transduced pHAEs as well as primary human lung organoids. Flow cytometry analysis of pHAEs revealed distinct cellular specificities between the BoV isolates, with HBoV1 targeting ciliated, club, and KRT5+ basal cells, whereas HBoV4 showed a preference for KRT5+ basal cells. Surprisingly, primary human hepatocytes, skeletal muscle cells, and T cells were also highly amenable to rAAV/BoV transduction. Finally, we adapted our pipeline for AAV capsid gene shuffling to all five BoV isolates. Collectively, our chimeric rAAV/BoV vectors and bocaviral capsid library represent valuable new resources to dissect BoV biology and to breed unique gene therapy vectors.
引用
收藏
页码:202 / 222
页数:21
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