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Abstract

Both subretinal dosing and intravitreal (IVT) dosing of adeno-associated virus (AAV) in higher species induce mild and transient inflammatory responses that increase with dose. Foreign protein and foreign DNA are known inducers of inflammation, which is also true in the immune-privileged ocular environment. We explored which component(s) of AAV vectors, viral capsid, or viral DNA drive inflammatory responses. Recombinant AAV with three tyrosine to phenylalanine substitutions in the capsid of AAV serotype 2 (rAAV2tYF), and with a generic ubiquitous promoter (cytomegalovirus [CMV]) controlling the expression of humanized green fluorescent protein (hGFP), was processed to enrich for AAV capsids containing genome (full capsids), capsids without genome (empty capsids), and residual material. Nonhuman primate eyes were injected by IVT in both eyes. During in-life, ocular inflammation and development of neutralizing antibodies (NAb) were measured. Following termination, lymph node immunophenotyping was performed, vitreous was processed for cytokine and RNAseq analyses, and ocular sections were assessed for transgene expression (by in situ hybridization) and histopathology. IVT dosing of AAV vectors transiently raised cellular inflammation in the aqueous and induced a more sustained inflammation in the vitreous. Lowering the total capsid dose by removing empty AAV capsids reduced inflammation and improved viral transduction. IVT dosing of AAV induced systemic NAb to AAV irrespective of the vector preparation. Similarly, lymph node immunophenotyping revealed identical profiles irrespective of viral preparation used for dosing. Immune cells in the vitreous were identified based on RNAseq analysis. Three months postdose, cytokine levels were low, indicative of minimal levels of inflammation in agreement with histopathological assessment of the retina.

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References

Wang

, Tai

PWL

, Gao

. Adeno-associated virus vector as a platform for gene therapy delivery. Nat Rev Drug Discov, 2019; 18:358–378.

Ochakovski

, Bartz-Schmidt

, Fischer

. Retinal gene therapy: surgical vector delivery in the translation to clinical trials. Front Neurosci, 2017; 11:174.

Grzybowski

, Told

, Sacu

, et al. 2018 Update on Intravitreal Injections: euretina Expert Consensus Recommendations. Ophthalmologica, 2018; 239:181–193.

Dalkara

, Byrne

, Klimczak

, et al. In vivo-directed evolution of a new adeno-associated virus for therapeutic outer retinal gene delivery from the vitreous. Sci Transl Med, 2013; 5:189ra176.

Day

, Byrne

, Schaffer

, et al. Advances in AAV vector development for gene therapy in the retina. Adv Exp Med Biol, 2014; 801:687–693.

Marsic

, Govindasamy

, Currlin

, et al. Vector design Tour de Force: integrating combinatorial and rational approaches to derive novel adeno-associated virus variants. Mol Ther, 2014; 22:1900–1909.

Marsic

, Zolotukhin

. Altering Tropism of rAAV by Directed Evolution p151. Methods Mol Biol, 2016; 1382:151–173.

Kotterman

, Yin

, Strazzeri

, et al. Antibody neutralization poses a barrier to intravitreal adeno-associated viral vector gene delivery to non-human primates. Gene Ther, 2015; 22:116–126.

Maclachlan

, Lukason

, Collins

, et al. Preclinical safety evaluation of AAV2-sFLT01—a gene therapy for age-related macular degeneration. Mol Ther, 2011; 19:326–334.

10.

, Budzynski

, Sonnentag

, et al. Safety and biodistribution evaluation in CNGB3-deficient mice of rAAV2tYF-PR1.7-hCNGB3, a recombinant AAV vector for treatment of achromatopsia. Hum Gene Ther Clin Dev, 2016; 27:27–36.

11.

, Conlon

, Erger

, et al. Safety and biodistribution evaluation of rAAV2tYF-CB-hRS1, a recombinant adeno-associated virus vector expressing retinoschisin, in RS1-deficient mice. Hum Gene Ther Clin Dev, 2015; 26:177–184.

12.

Marangoni

, Wu

, Wiley

, et al. Preclinical safety evaluation of a recombinant AAV8 vector for X-linked retinoschisis after intravitreal administration in rabbits. Hum Gene Ther Clin Dev, 2014; 25:202–211.

13.

Streilein

. Ocular immune privilege: the eye takes a dim but practical view of immunity and inflammation. J Leukoc Biol, 2003; 74:179–185.

14.

Streilein

, Ohta

, Mo

, et al. Ocular immune privilege and the impact of intraocular inflammation. DNA Cell Biol, 2002; 21:453–459.

15.

Conway

, Rhys

, Zolotukhin

, et al. High-titer recombinant adeno-associated virus production utilizing a recombinant herpes simplex virus type I vector expressing AAV-2 Rep and Cap. Gene Ther, 1999; 6:986–993.

16.

Conway

, Zolotukhin

, Muzyczka

, et al. Recombinant adeno-associated virus type 2 replication and packaging is entirely supported by a herpes simplex virus type 1 amplicon expressing Rep and Cap. J Virol, 1997; 71:8780–8789.

17.

Kang

, Wang

, Harrell

, et al. An efficient rHSV-based complementation system for the production of multiple rAAV vector serotypes. Gene Ther, 2009; 16:229–239.

18.

Thomas

, Wang

, Niamke

, et al. Scalable recombinant adeno-associated virus production using recombinant herpes simplex virus type 1 coinfection of suspension-adapted mammalian cells. Hum Gene Ther, 2009; 20:861–870.

19.

, Scotti

, Liu

, et al. Clearance and characterization of residual HSV DNA in recombinant adeno-associated virus produced by an HSV complementation system. Gene Ther, 2011; 18:135–144.

20.

Chulay

, Ye

, Thomas

, et al. Preclinical evaluation of a recombinant adeno-associated virus vector expressing human alpha-1 antitrypsin made using a recombinant herpes simplex virus production method. Hum Gene Ther, 2011; 22:155–165.

21.

Thomasy

, Eaton

, Timberlake

, et al. Species differences in the geometry of the anterior segment differentially affect anterior chamber cell scoring systems in laboratory animals. J Ocul Pharmacol Ther, 2016; 32:28–37.

22.

Clement

, Grieger

. Manufacturing of recombinant adeno-associated viral vectors for clinical trials. Mol Ther Methods Clin Dev, 2016; 3:16002.

23.

Penaud-Budloo

, Francois

, Clement

, et al. Pharmacology of recombinant adeno-associated virus production. Mol Ther Methods Clin Dev, 2018; 8:166–180.

24.

Gao

, Li

, Zhong

, et al. Empty virions in AAV8 vector preparations reduce transduction efficiency and may cause total viral particle dose-limiting side-effects. Mol Ther Methods Clin Dev, 2014; 1:20139.

25.

Reichel

, Dauletbekov

, Klein

, et al. AAV8 can induce innate and adaptive immune response in the primate eye. Mol Ther, 2017; 25:2648–2660.

26.

Yin

, Greenberg

, Hunter

, et al. Intravitreal injection of AAV2 transduces macaque inner retina. Invest Ophthalmol Vis Sci, 2011; 52:2775–2783.

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Ocular Inflammatory Response to Intravitreal Injection of Adeno-Associated Virus Vector: Relative Contribution of Genome and Capsid

Abstract

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