Your search keyword '"dependovirus"' showing total 10,102 results

351. Use of an adeno‐associated virus serotype Anc80 to provide durable cure of phenylketonuria in a mouse model

Author

Michael Martinez, Nicholas D. Weber, William Cao, Lori G Hillin, Robert A. Kaiser, Anne Douar, Kari L. Allen, Joseph B. Lillegard, Caitlin J. VanLith, Rafael Aldabe, Laia Trigueros-Motos, and Gloria González-Aseguinolaza

Subjects

Male, Phenylalanine hydroxylase, Phenylalanine, Genetic enhancement, Genetic Vectors, DNA, Recombinant, Biology, Gene delivery, Pharmacology, medicine.disease_cause, Virus, Cell Line, Mice, Transduction, Genetic, Phenylketonurias, Genetics, medicine, Animals, Humans, Hair Color, Adeno-associated virus, Genetics (clinical), Phenylalanine Hydroxylase, Genetic Therapy, Dependovirus, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Liver, Inborn error of metabolism, Injections, Intravenous, Systemic administration, biology.protein, Female

Abstract

Phenylketonuria (PKU) is the most common inborn error of metabolism of the liver, and results from mutations of both alleles of the phenylalanine hydroxylase gene (PAH). As such, it is a suitable target for gene therapy via gene delivery with a recombinant adeno-associated virus (AAV) vector. Here we use the synthetic AAV vector Anc80 via systemic administration to deliver a functional copy of a codon-optimized human PAH gene, with or without an intron spacer, to the Pahenu2 mouse model of PKU. Dose-dependent transduction of the liver and expression of PAH mRNA were present with both vectors, resulting in significant and durable reduction of circulating phenylalanine, reaching near control levels in males. Coat color of treated Pahenu2 mice reflected an increase in pigmentation from brown to the black color of control animals, further indicating functional restoration of phenylalanine metabolism and its byproduct melanin. There were no adverse effects associated with administration of AAV up to 5 × 1012 VG/kg, the highest dose tested. Only minor and/or transient variations in some liver enzymes were observed in some of the AAV-dosed animals which were not associated with pathology findings in the liver. Finally, there was no impact on cell turnover or apoptosis as evaluated by Ki-67 and TUNEL staining, further supporting the safety of this approach. This study demonstrates the therapeutic potential of AAV Anc80 to safely and durably cure PKU in a mouse model, supporting development for clinical consideration.

Published

2021

352. Effects and Mechanisms of Synaptotagmin-7 in the Hippocampus on Cognitive Impairment in Aging Mice

Author

Yaru Xie, Kaining Zhi, and Xian-Fang Meng

Subjects

Male, Aging, Conditioning, Classical, Genetic Vectors, Long-Term Potentiation, Spatial Learning, Neuroscience (miscellaneous), Hippocampus, Nerve Tissue Proteins, medicine.disease_cause, Synaptotagmin 1, Mice, Random Allocation, Synaptotagmins, Cellular and Molecular Neuroscience, Genes, Reporter, Morris Water Maze Test, medicine, Animals, Memory impairment, CA1 Region, Hippocampal, Neuroinflammation, Electroshock, Memory Disorders, business.industry, Genes, p16, Galactose, Recognition, Psychology, Long-term potentiation, Transporter, Cognition, Fear, Dependovirus, Genes, p53, Recombinant Proteins, Specific Pathogen-Free Organisms, Mice, Inbred C57BL, Gene Expression Regulation, nervous system, Neurology, Cognition Disorders, business, Neuroscience, Oxidative stress

Abstract

Aging is an irreversible biological process that involves oxidative stress, neuroinflammation, and apoptosis, and eventually leads to cognitive dysfunction. However, the underlying mechanisms are not fully understood. In this study, we investigated the role and potential mechanisms of Synaptotagmin-7, a calcium membrane transporter in cognitive impairment in aging mice. Our results indicated that Synaptotagmin-7 expression significantly decreased in the hippocampus of D-galactose-induced or naturally aging mice when compared with healthy controls, as detected by western blot and quantitative reverse transcriptase-polymerase chain reaction analysis. Synaptotagmin-7 overexpression in the dorsal CA1 of the hippocampus reversed long-term potentiation and improved hippocampus-dependent spatial learning in D-galactose-induced aging mice. Synaptotagmin-7 overexpression also led to fully preserved learning and memory in 6-month-old mice. Mechanistically, we demonstrated that Synaptotagmin-7 improved learning and memory by elevating the level of fEPSP and downregulating the expression of aging-related genes such as p53 and p16. The results of our study provide new insights into the role of Synaptotagmin-7 in improving neuronal function and overcoming memory impairment caused by aging, suggesting that Synaptotagmin-7 overexpression may be an innovative therapeutic strategy for treating cognitive impairment.

Published

2021

353. Detailed Protocol for the Novel and Scalable Viral Vector Upstream Process for AAV Gene Therapy Manufacturing

Author

Ramarao Vepachedu, Trevor Broadt, Peter Pechan, Brian Bowser, Nora Yang, George Mitra, Asaf Alimardanov, Samir Hussein Shaban, Jenna Burns, Nagarathinam Selvaraj, Chao-Kuei Wang, Nirmala Saptharishi, and Diane Golebiowski

Subjects

Protocol (science), Computer science, viruses, Genetic enhancement, Genetic Vectors, HEK 293 cells, Genetic Therapy, Computational biology, Dependovirus, Transfection, Cell Line, law.invention, Viral vector, law, Scalability, Methods, Genetics, Recombinant DNA, Molecular Medicine, Upstream (networking), Vector (molecular biology), Molecular Biology

Abstract

Recombinant adeno-associated viral (rAAV) vector-based gene therapy has been adapted for use in more than 100 clinical trials. This is mainly because of its excellent safety profile, ability to target a wide range of tissues, stable transgene expression, and significant clinical benefit. However, the major challenge is to produce a high-titer, high-potency vector to achieve a better therapeutic effect. Even though the three plasmid-based transient transfection method is currently being used for AAV production in many clinical trials, there are complications associated with scalability and it is not cost-effective. Other methods require either large-scale production of two herpes simplex viruses, rHSV-RepCap and rHSV-GOI (gene of interest), with high titers, or a stable cell line with high titer wild-type adenovirus infection. Both of these options make the process even more complex. To address this issue, we have developed a stable cell line-based production with the use of only one rHSV-RepCap virus. Using this new methodology in small-scale production, we achieved ∼1–6 E + 04 vg/cell of AAV9 in the top producer clones. Large-scale production in 10-CS (10-Cell Stack) of one of the top producing clones resulted in ∼1–2 E + 13 vg/10-CS with 50% of full capsid ratio after purification. This method could potentially be adapted to suspension cells. The major advantage of this novel methodology is that by using the rHSV-RepCap virus, high titer AAV can be produced with any GOI containing a stable adherent or suspension producer cell line. The use of this AAV production platform could be beneficial for the treatment of many diseases.

Published

2021

354. Gene Therapy for Rdh12-Associated Retinal Diseases Helps to Delay Retinal Degeneration and Vision Loss

Author

Hongyu Chen, Jianhong An, Ming Qi, Yuqing Cao, Jiaxin Bian, Qing Pan, and Jun-hui Sun

Subjects

Male, Retinal degeneration, medicine.medical_specialty, Time Factors, genetic structures, mouse model, Genetic enhancement, Vision Disorders, Pharmaceutical Science, Virus, Mice, chemistry.chemical_compound, Ophthalmology, parasitic diseases, Drug Discovery, Electroretinography, medicine, Animals, Original Research, Mice, Knockout, Pharmacology, Drug Design, Development and Therapy, medicine.diagnostic_test, business.industry, Retinal Degeneration, Retinal, Genetic Therapy, Dependovirus, medicine.disease, gene therapy, Phenotype, Rdh12, eye diseases, Mice, Inbred C57BL, Alcohol Oxidoreductases, Disease Models, Animal, retinal diseases, chemistry, Female, business, Erg, Bright light

Abstract

Jiaxin Bian,1,2 Hongyu Chen,1,2 Junhui Sun,1,2 Yuqing Cao,3 Jianhong An,3 Qing Pan,4 Ming Qi1,2,5– 8 1Department of Cell Biology and Medical Genetics, School of Medicine Zhejiang University, Hangzhou, 310000, People’s Republic of China; 2Center for Precision Medicine, Zhejiang-California International NanoSystems Institute, Hangzhou, 310000, People’s Republic of China; 3School of Optometry and Ophthalmology Wenzhou Medical College, Wenzhou, People’s Republic of China; 4Department of Ophthalmology, Zhejiang University Medical School First Affiliated Hospital, Hangzhou, 310000, People’s Republic of China; 5Assisted Reproduction Unit, Department of Obstetrics and Gynecology, Department of Laboratory Medicine, Sir Run Run Shaw Hospital, Zhejiang University School of Medicine, Key Laboratory of Reproductive Dysfunction Management of Zhejiang Province, Hangzhou, 310000, People’s Republic of China; 6DIAN Diagnostics, Hangzhou, 310000, People’s Republic of China; 7Department of Pathology and Laboratory of Medicine, University of Rochester Medical Centre, Rochester, NY, 14609, USA; 8HVP-China, Hangzhou, 310000, People’s Republic of ChinaCorrespondence: Qing PanDepartment of Ophthalmology, Zhejiang University Medical School First Affiliated Hospital, 79 Qingchun Road, Hangzhou, People’s Republic of ChinaTel +86 13515814709Email panqing@hotmail.comMing QiDepartment of Cell Biology and Medical Genetics, School of Medicine Zhejiang University, Research Building A713, Yuhangtang Road 866, Hangzhou, People’s Republic of ChinaTel +86 13666686943Fax +86 57188208274Email mingqi@zju.edu.cn; ming_qi@urmc.Rochester.eduPurpose: The aim of study was to establish Rdh12-associated inherited retinal disease (Rdh12-IRD) mouse model and to identify the best timepoint for gene therapy.Methods: We induced retinal degeneration in Rdh12−/− mice using a bright light. We clarified the establishment of Rdh12-IRD mouse model by analyzing the thickness of retinal layers and electroretinography (ERG). Rdh12-IRD mice received a subretinal injection of adeno-associated virus 2/8-packaged Rdh12 cDNA for treatment. We evaluated the visual function and retinal structure in the treated and untreated eyes to identify the best timepoint for gene therapy.Results: Rdh12-IRD mice showed significant differences in ERG amplitudes and photoreceptor survival compared to Rdh12+/+ mice. Preventive gene therapy not only maintained normal visual function but also prevented photoreceptor loss. Salvage gene therapy could not reverse the retinal degeneration phenotype of Rdh12-IRD mice, but it could slow down the loss of visual function.Conclusion: The light-induced retinal degeneration in our Rdh12−/− mice indicated that a defect in Rdh12 alone was sufficient to cause visual dysfunction and photoreceptor degeneration, which reproduced the phenotypes observed in RDH12-IRD patients. This model is suitable for gene therapy studies. Early treatment of the primary Rdh12 defect helps to delay the later onset of photoreceptor degeneration and maintains visual function in Rdh12-IRD mice.Keywords: Rdh12, retinal diseases, mouse model, gene therapy

Published

2021

355. Gene therapy reforms photoreceptor structure and restores vision in NPHP5-associated Leber congenital amaurosis

Author

Samuel G. Jacobson, Simone Iwabe, Ana Ripolles Garcia, William A. Beltran, Sanford L. Boye, Roman Nikonov, Malgorzata Swider, Gustavo D. Aguirre, Raghavi Sudharsan, Valerie L. Dufour, William W. Hauswirth, and Artur V. Cideciyan

Subjects

Retinal degeneration, genetic structures, Genetic enhancement, Mutant, Genetic Vectors, Leber Congenital Amaurosis, Degeneration (medical), Biology, medicine.disease_cause, Photoreceptor cell, Dogs, Drug Discovery, Electroretinography, Genetics, medicine, Animals, Humans, Molecular Biology, Pharmacology, Mutation, Retina, Childhood blindness, Correction, Genetic Therapy, Dependovirus, medicine.disease, eye diseases, Cell biology, Disease Models, Animal, Ciliopathy, Treatment Outcome, medicine.anatomical_structure, Retinal Cone Photoreceptor Cells, Molecular Medicine, Calmodulin-Binding Proteins, Original Article, sense organs, Retinopathy

Abstract

The inherited childhood blindness caused by mutations in NPHP5, a form of Leber congenital amaurosis, results in abnormal development, dysfunction and degeneration of photoreceptors. A naturally occurring NPHP5 mutation in dogs results in a phenotype that very nearly duplicates the human retinopathy in terms of the photoreceptors involved, spatial distribution of degeneration and the natural history of vision loss. We show that AAV-mediated NPHP5 gene augmentation of mutant canine retinas at the time of active degeneration and peak cell death stably restores photoreceptor structure, function, and vision with either the canine or human NPHP5 transgenes. Mutant cone photoreceptors, which failed to form outer segments during development, reform this structure after treatment. Degenerating rod photoreceptor outer segments are stabilized and develop normal structure. This process begins within 8 weeks following treatment, and remains stable throughout the 6 month post treatment period. In both photoreceptor cell classes, mislocalization of rod and cone opsins is minimized or reversed. Retinal function and functional vision are restored. Efficacy of gene therapy in this large animal ciliopathy model of Leber congenital amaurosis provides a path for translation to human treatment.

Published

2021

356. Astrocyte-to-neuron transportation of enhanced green fluorescent protein in cerebral cortex requires F-actin dependent tunneling nanotubes

Author

Jing Chen and Junyan Cao

Subjects

Cell biology, Science, Green Fluorescent Proteins, Endocytosis, Exosomes, Article, Green fluorescent protein, Mice, Organelle, medicine, Animals, Humans, Gene Knock-In Techniques, Actin, Cerebral Cortex, Neurons, Multidisciplinary, Nanotubes, Chemistry, Dependovirus, Actins, Cortex (botany), medicine.anatomical_structure, Cerebral cortex, Astrocytes, Medicine, Neuron, Astrocyte, Neuroscience

Abstract

Tunneling Nanotube (TNT) , a dynamic cell-cell contact, is dependent on actin polimerization. TNTs are efficient in transporting ions, proteins and organelles intercellularly, which are important mechanisms in physiological and phathological precesses. Reported studies on the existence and function of TNTs among neural cells focus on cultured cell for the convenience in detecting TNTs’ ultrastructure. In this study, the adeno-associated virus (AAV-GFAP-EGFP-p2A-cre) was injected in the cerebral cortex of knock-in mice ROSA26 GNZ. GFAP promoter initiated the expression of Enhanced Green Fluorescent Protein (EGFP) in infected astrocytes. At 10 days post injection (10 DPI), we found that EGFP could transfer from astrocytes in layerⅠ-Ⅲ to neurons in layer Ⅴ. The dissemination of EGFP was not through endocytosis or exosome. And the intercellular transportation of EGFP was F-actin dependent. Therefore, we concluded EGFP transported from astrocytes to neurons in coetex via F-actin dependent TNTs. Although it is hardly to detect the ultrastrucute of TNTs in brain for its transiency and the noisy background, we established an animal model and indirect experimental methods to explore TNTs in vivo.

Published

2021

357. Rapid Highly-Efficient Digestion and Peptide Mapping of Adeno-Associated Viruses

Author

Ken Cook, Alexander Boris Schwann, Craig Dufresne, Alexander R. Ivanov, Estee Naggar Toole, and Somak Ray

Subjects

Chemistry, viruses, Proteolytic enzymes, Dependovirus, Trypsin, Cleavage (embryo), Tandem mass spectrometry, Peptide Mapping, Article, Analytical Chemistry, Capsid, Digestion (alchemy), Biochemistry, medicine, Humans, Capsid Proteins, Digestion, Denaturation (biochemistry), Gene, medicine.drug

Abstract

Adeno-associated viruses (AAVs) comprise an area of rapidly growing interest due to their ability to act as a gene delivery vehicle in novel gene therapy strategies and vaccine development. Peptide mapping is a common technique in the biopharmaceutical industry to confirm the correct sequence, product purity, post-translational modifications (PTMs), and stability. However, conventional peptide mapping is time-consuming and has proven difficult to reproduce with viral capsids because of their high structural stability and the suboptimal localization of trypsin cleavage sites in the AAV protein sequences. In this study, we present an optimized peptide mapping-based workflow that provides thorough characterization within 1 day. This workflow is also highly reproducible due to its simplicity having very few steps and is easy to perform proteolytic digestion utilizing thermally stable pepsin, which is active at 70 °C in acidic conditions. The acidic conditions of the peptic digestions drive viral capsid denaturation and improve cleavage site accessibility. We characterized the efficiency and ease of digestion through peptide mapping of the AAV2 viral capsid protein. Using nanoflow liquid chromatography coupled with tandem mass spectrometry, we achieved 100% sequence coverage of the low-abundance VP1 capsid protein with a digestion process taking only 10 min to prepare and 45 min to complete the digestion.

Published

2021

358. Low-Dose Recombinant Adeno-Associated Virus-Mediated Inhibition of Vascular Endothelial Growth Factor Can Treat Neovascular Pathologies Without Inducing Retinal Vasculitis

Author

Bo Tian, Yongwen Luo, Claudio Punzo, Phillip W. L. Tai, Guangping Gao, Haijiang Lin, Qiang Zheng, Qin Su, Jun Xie, Jihye Ko, Anneliese Malachi, Xiao Ke, and Shun-Yun Cheng

Subjects

Vascular Endothelial Growth Factor A, Intercellular Adhesion Molecule-1, CNV, Angiogenesis Inhibitors, AMD, rAAV, medicine.disease_cause, vasculitis, 03 medical and health sciences, chemistry.chemical_compound, Macular Degeneration, Mice, 0302 clinical medicine, Immune system, DR, wet AMD, Genetics, Medicine, Animals, Humans, Molecular Biology, Adeno-associated virus, Research Articles, 030304 developmental biology, Retinal Vasculitis, 0303 health sciences, business.industry, Cell adhesion molecule, Macular degeneration, Dependovirus, medicine.disease, VEGF, Extravasation, Choroidal Neovascularization, Vascular endothelial growth factor, Choroidal neovascularization, chemistry, anti-VEGF, 030220 oncology & carcinogenesis, Intravitreal Injections, Cancer research, Molecular Medicine, medicine.symptom, business, conbercept

Abstract

The wet form of age-related macular degeneration is characterized by neovascular pathologies that, if untreated, can result in edemas followed by rapid vision loss. Inhibition of vascular endothelial growth factor (VEGF) has been used to successfully treat neovascular pathologies of the eye. Nonetheless, some patients require frequent intravitreal injections of anti-VEGF drugs, increasing the burden and risk of complications from the procedure to affected individuals. Recombinant adeno-associated virus (rAAV)-mediated expression of anti-VEGF proteins is an attractive alternative to reduce risk and burden to patients. However, controversy remains as to the safety of prolonged VEGF inhibition in the eye. Here, we show that two out of four rAAV serotypes tested by intravitreal delivery to express the anti-VEGF drug conbercept lead to a dose-dependent vascular sheathing pathology that is characterized by immune cell infiltrates, reminiscent of vasculitis in humans. We show that this pathology is accompanied by increased expression in vascular cell adhesion molecule 1 (VCAM1) and intercellular adhesion molecule 1 (ICAM1), both of which promote extravasation of immune cells from the vasculature. While formation of the vascular sheathing pathology is prevented in immunodeficient Rag-1 mice that lack B and T cells, increased expression of VACM1 and ICAM1 still occurs, indicating that inhibition of VEGF function leads to expression changes in cell adhesion molecules that promote extravasation of immune cells. Importantly, a 10-fold lower dose of one of the vectors that cause a vascular sheathing pathology is still able to reduce edemas resulting from choroidal neovascularization without causing any vascular sheathing pathology and only a minimal increase in VCAM1 expression. The data suggest that treatments of neovascular eye pathologies with rAAV-mediated expression of anti VEGF drugs can be developed safely. However, viral load needs to be adjusted to the tropisms of the serotype and the expression pattern of the promoter.

Published

2021

359. Dravet Syndrome: Novel Approaches for the Most Common Genetic Epilepsy

Author

Kelly G. Knupp and Lori L. Isom

Subjects

medicine.medical_specialty, Neurology, Exacerbation, Epilepsies, Myoclonic, Review, Disease, Epilepsy, Quality of life (healthcare), Dravet syndrome, medicine, Animals, Humans, Pharmacology (medical), Precision Medicine, Intensive care medicine, Pharmacology, business.industry, Genetic Therapy, Dependovirus, Oligonucleotides, Antisense, medicine.disease, Precision medicine, Clinical trial, Anticonvulsants, Neurology (clinical), business, Sodium Channel Blockers

Abstract

Dravet syndrome (DS) is a severe developmental and epileptic encephalopathy that is mainly associated with variants in SCN1A. While drug-resistant epilepsy is the most notable feature of this syndrome, numerous symptoms are present that have significant impact on patients’ quality of life. In spite of novel, third-generation anti-seizure treatment options becoming available over the last several years, seizure freedom is often not attained and non-seizure symptoms remain. Precision medicine now offers realistic hope for seizure freedom in DS patients, with several approaches demonstrating preclinical success. Therapeutic approaches such as antisense oligonucleotides (ASO) and adeno-associated virus (AAV)-delivered gene modulation have expanded the potential treatment options for DS, with some of these approaches now transitioning to clinical trials. Several of these treatments may risk the exacerbation of gain-of-function variants and may not be reversible, therefore emphasizing the need for functional testing of new pathogenic variants. The current absence of treatments that address the overall disease, in addition to seizures, exposes the urgent need for reliable, valid measures of the entire complement of symptoms as outcome measures to truly know the impact of treatments on DS. Additionally, with so many treatment options on the horizon, there will be a need to understand how to select appropriate patients for each treatment, whether treatments are complementary or adverse to each other, and long-term risks of the treatment. Nevertheless, precision therapeutics hold tremendous potential to provide long-lasting seizure freedom and even complete cures for this devastating disease. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1007/s13311-021-01095-6.

Published

2021

360. Manufacturing Challenges and Rational Formulation Development for AAV Viral Vectors

Author

Ger Brophy, Arvind Srivastava, Krishna M.G. Mallela, and Nandkumar Deorkar

Subjects

Computer science, Genetic Vectors, Gene Transfer Techniques, Pharmaceutical Science, Genetic Therapy, 02 engineering and technology, Dependovirus, Gene delivery, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, Unit operation, Viral vector, 03 medical and health sciences, Safety profile, Transduction (genetics), 0302 clinical medicine, Downstream (manufacturing), Vector (molecular biology), Biochemical engineering, 0210 nano-technology, Light exposure

Abstract

Adeno-associated virus (AAV) has emerged as a leading platform for gene delivery for treating various diseases due to its excellent safety profile and efficient transduction to various target tissues. However, the large-scale production and long-term storage of viral vectors is not efficient resulting in lower yields, moderate purity, and shorter shelf-life compared to recombinant protein therapeutics. This review provides a comprehensive analysis of upstream, downstream and formulation unit operation challenges encountered during AAV vector manufacturing, and discusses how desired product quality attributes can be maintained throughout product shelf-life by understanding the degradation mechanisms and formulation strategies. The mechanisms of various physical and chemical instabilities that the viral vector may encounter during its production and shelf-life because of various stressed conditions such as thermal, shear, freeze-thaw, and light exposure are highlighted. The role of buffer, pH, excipients, and impurities on the stability of viral vectors is also discussed. As such, the aim of this review is to outline the tools and a potential roadmap for improving the quality of AAV-based drug products by stressing the need for a mechanistic understanding of the involved processes.

Published

2021

361. Intravitreal Injection of an Exosome-Associated Adeno-Associated Viral Vector Enhances Retinoschisin 1 Gene Transduction in the Mouse Retina

Author

Weiping Wang, Bingtao Hao, Ruiqi Qiu, Mingzhu Yang, Bo Lei, Ya Li, Jingyang Liu, and Shasha Bian

Subjects

viruses, Genetic enhancement, Genetic Vectors, Biology, Exosomes, medicine.disease_cause, Exosome, Retina, Virus, Viral vector, Mice, 03 medical and health sciences, Transduction (genetics), 0302 clinical medicine, Plasmid, Transduction, Genetic, Genetics, medicine, Animals, Humans, Vector (molecular biology), Molecular Biology, Adeno-associated virus, 030304 developmental biology, 0303 health sciences, Dependovirus, Cell biology, Mice, Inbred C57BL, 030220 oncology & carcinogenesis, Intravitreal Injections, Molecular Medicine

Abstract

To investigate whether exosome-associated adeno-associated virus (AAV) retinoschisin 1 (RS1) vector improved the transduction efficiency of RS1 in the mouse retina. pAAV2-RS1-ZsGreen plasmid was co...

Published

2021

362. Gene therapy for aromatic L-amino acid decarboxylase deficiency by MR-guided direct delivery of AAV2-AADC to midbrain dopaminergic neurons

Author

Neha Seth, Amy Minnema, Miguel Hernandez Pampaloni, Amy Viehoever, Toni S. Pearson, Waldy San Sebastian, Ana Grijalvo-Perez, Shannon Lundy, Erin Smith, Russell R. Lonser, Krystof S. Bankiewicz, Jill Imamura-Ching, J. Bradley Elder, Jeffrey R. Leonard, Youngho Seo, Jill C. Heathcock, Keith Hyland, Gardenia de Oliveira Barbosa, Paul S. Larson, Alex J. Fay, and Nalin Gupta

Subjects

0301 basic medicine, Male, Time Factors, viruses, General Physics and Astronomy, Striatum, 0302 clinical medicine, Mesencephalon, Child, Pediatric, Neurotransmitter Agents, Multidisciplinary, Inborn Errors, Dopaminergic, Gene Transfer Techniques, Gene Therapy, Dependovirus, Magnetic Resonance Imaging, Ventral tegmental area, medicine.anatomical_structure, Aromatic-L-Amino-Acid Decarboxylases, Child, Preschool, Neurological, Metabolome, Female, medicine.drug, medicine.medical_specialty, Science, Clinical Trials and Supportive Activities, Substantia nigra, Gene delivery, Motor Activity, Paediatric research, General Biochemistry, Genetics and Molecular Biology, Article, Midbrain, 03 medical and health sciences, Dopamine, Clinical Research, Internal medicine, medicine, Genetics, Humans, Preschool, Movement disorders, Amino Acid Metabolism, Inborn Errors, Dyskinesias, business.industry, Dopaminergic Neurons, Neurosciences, General Chemistry, Genetic Therapy, Brain Disorders, Amino Acid Metabolism, 030104 developmental biology, Endocrinology, nervous system, Serotonin, business, 030217 neurology & neurosurgery

Abstract

Aromatic L-amino acid decarboxylase (AADC) deficiency is a rare genetic disorder characterized by deficient synthesis of dopamine and serotonin. It presents in early infancy, and causes severe developmental disability and lifelong motor, behavioral, and autonomic symptoms including oculogyric crises (OGC), sleep disorder, and mood disturbance. We investigated the safety and efficacy of delivery of a viral vector expressing AADC (AAV2-hAADC) to the midbrain in children with AADC deficiency (ClinicalTrials.gov Identifier NCT02852213). Seven (7) children, aged 4–9 years underwent convection-enhanced delivery (CED) of AAV2-hAADC to the bilateral substantia nigra (SN) and ventral tegmental area (VTA) (total infusion volume: 80 µL per hemisphere) in 2 dose cohorts: 1.3 × 1011 vg (n = 3), and 4.2 × 1011 vg (n = 4). Primary aims were to demonstrate the safety of the procedure and document biomarker evidence of restoration of brain AADC activity. Secondary aims were to assess clinical improvement in symptoms and motor function. Direct bilateral infusion of AAV2-hAADC was safe, well-tolerated and achieved target coverage of 98% and 70% of the SN and VTA, respectively. Dopamine metabolism was increased in all subjects and FDOPA uptake was enhanced within the midbrain and the striatum. OGC resolved completely in 6 of 7 subjects by Month 3 post-surgery. Twelve (12) months after surgery, 6/7 subjects gained normal head control and 4/7 could sit independently. At 18 months, 2 subjects could walk with 2-hand support. Both the primary and secondary endpoints of the study were met. Midbrain gene delivery in children with AADC deficiency is feasible and safe, and leads to clinical improvements in symptoms and motor function., Aromatic L-amino acid decarboxylase deficiency (AADC) is a rare neurodevelopmental disorder. Here the authors describe a clinical trial of MR-guided delivery of AAV2-AADC for the treatment of AADC.

Published

2021

363. Co-editing PINK1 and DJ-1 Genes Via Adeno-Associated Virus-Delivered CRISPR/Cas9 System in Adult Monkey Brain Elicits Classical Parkinsonian Phenotype

Author

Shihao Wu, Jing Wu, Liqi Xu, Longbao Lv, Xia Ma, Tian-Lin Cheng, Yingzhou Hu, Xiao Li, Zhi-Fang Chen, Zilong Qiu, Hao Li, Wenchao Wang, Ling Li, Yong Yin, Haisong Jiang, and Xintian Hu

Subjects

0301 basic medicine, DJ-1, medicine.medical_specialty, Parkinson's disease, Neurology, Physiology, Transgene, PINK1, Biology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, CRISPR, Adeno-associated virus-delivered CRISPR/Cas9, Pathological, Adeno-associated virus, General Neuroscience, Brain, Haplorhini, General Medicine, Parkinsonian phenotype, Dependovirus, medicine.disease, Phenotype, Monkey, 030104 developmental biology, Parkinson’s disease, Original Article, CRISPR-Cas Systems, Protein Kinases, Neuroscience, 030217 neurology & neurosurgery

Abstract

Whether direct manipulation of Parkinson’s disease (PD) risk genes in the adult monkey brain can elicit a Parkinsonian phenotype remains an unsolved issue. Here, we used an adeno-associated virus serotype 9 (AAV9)-delivered CRISPR/Cas9 system to directly co-edit PINK1 and DJ-1 genes in the substantia nigras (SNs) of two monkey groups: an old group and a middle-aged group. After the operation, the old group exhibited all the classic PD symptoms, including bradykinesia, tremor, and postural instability, accompanied by key pathological hallmarks of PD, such as severe nigral dopaminergic neuron loss (>64%) and evident α-synuclein pathology in the gene-edited SN. In contrast, the phenotype of their middle-aged counterparts, which also showed clear PD symptoms and pathological hallmarks, were less severe. In addition to the higher final total PD scores and more severe pathological changes, the old group were also more susceptible to gene editing by showing a faster process of PD progression. These results suggested that both genetic and aging factors played important roles in the development of PD in the monkeys. Taken together, this system can effectively develop a large number of genetically-edited PD monkeys in a short time (6–10 months), and thus provides a practical transgenic monkey model for future PD studies. Supplementary Information The online version contains supplementary material available at 10.1007/s12264-021-00732-6.

Published

2021

364. Gene Therapy Using Adeno‐Associated Virus Serotype 8 Encoding <scp> TNAP‐D 10 </scp> Improves the Skeletal and Dentoalveolar Phenotypes in <scp> Alpl −/− </scp> Mice

Author

Sonoko Narisawa, Koichi Miyake, Yuka Kinoshita, Fatma F Mohamed, Brian L. Foster, José Luis Millán, and Flávia Amadeu de Oliveira

Subjects

Adult, 0301 basic medicine, medicine.medical_specialty, DENTAL BIOLOGY, Endocrinology, Diabetes and Metabolism, GENETIC ANIMAL MODELS, Hypophosphatasia, 030209 endocrinology & metabolism, Rickets, Serogroup, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, BONE μCT, medicine, Animals, Humans, Orthopedics and Sports Medicine, BONE HISTOMORPHOMETRY, Dental alveolus, business.industry, Osteoid, ALPL, Original Articles, Genetic Therapy, X-Ray Microtomography, Enzyme replacement therapy, Dependovirus, Alkaline Phosphatase, medicine.disease, OSTEOMALACIA AND RICKETS, Phenotype, 030104 developmental biology, Endocrinology, Asfotase alfa, Quality of Life, Alkaline phosphatase, Original Article, business

Abstract

Hypophosphatasia (HPP) is caused by loss‐of‐function mutations in the ALPL gene that encodes tissue‐nonspecific alkaline phosphatase (TNAP), whose deficiency results in the accumulation of extracellular inorganic pyrophosphate (PPi), a potent mineralization inhibitor. Skeletal and dental hypomineralization characterizes HPP, with disease severity varying from life‐threatening perinatal or infantile forms to milder forms that manifest in adulthood or only affect the dentition. Enzyme replacement therapy (ERT) using mineral‐targeted recombinant TNAP (Strensiq/asfotase alfa) markedly improves the life span, skeletal phenotype, motor function, and quality of life of patients with HPP, though limitations of ERT include frequent injections due to a short elimination half‐life of 2.28 days and injection site reactions. We tested the efficacy of a single intramuscular administration of adeno‐associated virus 8 (AAV8) encoding TNAP‐D10 to increase the life span and improve the skeletal and dentoalveolar phenotypes in TNAP knockout (Alpl −/−) mice, a murine model for severe infantile HPP. Alpl −/− mice received 3 × 1011 vector genomes/body of AAV8‐TNAP‐D10 within 5 days postnatal (dpn). AAV8‐TNAP‐D10 elevated serum ALP activity and suppressed plasma PPi. Treatment extended life span of Alpl −/− mice, and no ectopic calcifications were observed in the kidneys, aorta, coronary arteries, or brain in the 70 dpn observational window. Treated Alpl −/− mice did not show signs of rickets, including bowing of long bones, enlargement of epiphyses, or fractures. Bone microstructure of treated Alpl −/− mice was similar to wild type, with a few persistent small cortical and trabecular defects. Histology showed no measurable osteoid accumulation but reduced bone volume fraction in treated Alpl −/− mice versus controls. Treated Alpl −/− mice featured normal molar and incisor dentoalveolar tissues, with the exceptions of slightly reduced molar enamel and alveolar bone density. Histology showed the presence of cementum and normal periodontal ligament attachment. These results support gene therapy as a promising alternative to ERT for the treatment of HPP. © 2021 The Authors. Journal of Bone and Mineral Research published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research (ASBMR).

Published

2021

365. Delivering AAV to the Central Nervous and Sensory Systems

Author

Casey A. Maguire, Cole Peters, and Killian S. Hanlon

Subjects

0301 basic medicine, Cell type, Transgene, Genetic enhancement, Genetic Vectors, Sensory system, Toxicology, Article, Viral vector, 03 medical and health sciences, 0302 clinical medicine, Mainstream medicine, Humans, Medicine, Transgenes, Nerve Tissue, Mendelian disorders, Gene, Pharmacology, business.industry, Gene Transfer Techniques, Genetic Therapy, Dependovirus, 030104 developmental biology, business, Neuroscience, 030217 neurology & neurosurgery

Abstract

As gene therapy enters mainstream medicine, it is more important than ever to have a grasp of exactly how to leverage it for maximum benefit. The development of new targeting strategies and tools makes treating patients with genetic diseases possible. Many Mendelian disorders are amenable to gene replacement or correction. These often affect post-mitotic tissues, meaning that a single stably expressing therapy can be applied. Recent years have seen the development of a large number of novel viral vectors for delivering specific therapies. These new vectors - predominately recombinant adeno-associated virus (AAV) variants - target nervous tissues with differing efficiencies. This review gives an overview of current gene therapies in the brain, ear, and eye, and describes the optimal approaches, depending on cell type and transgene. Overall, this work aims to serve as a primer for gene therapy in the central nervous and sensory systems.

Published

2021

366. Viral Vector Delivery of DREADDs for CNS Therapy

Author

Nicholas D. Mazarakis and Ceri A Pickering

Subjects

Central Nervous System, Genetic enhancement, Genetic Vectors, Ligands, Designer Drugs, Receptors, G-Protein-Coupled, Viral vector, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, Genetics, Animals, Humans, Medicine, Gene silencing, Molecular Targeted Therapy, Receptor, Molecular Biology, Genetics (clinical), 030304 developmental biology, G protein-coupled receptor, Neurons, 0303 health sciences, biology, business.industry, Lentivirus, Brain, Genetic Therapy, Chemogenetics, Dependovirus, biology.organism_classification, Drug Design, 030220 oncology & carcinogenesis, Pseudotyping, Molecular Medicine, business, Neuroscience, Signal Transduction

Abstract

Designer Receptors Exclusively Activated by Designer Drugs (DREADDs) are genetically modified G-protein-coupled receptors (GPCRs), that can be activated by a synthetic ligand which is otherwise inert at endogenous receptors. DREADDs can be expressed in cells in the central nervous system (CNS) and subsequently offer the opportunity for remote and reversible silencing or activation of the target cells when the synthetic ligand is systemically administered. In neuroscience, DREADDs have thus far shown to be useful tools for several areas of research and offer considerable potential for the development of gene therapy strategies for neurological disorders. However, in order to design a DREADD-based gene therapy, it is necessary to first evaluate the viral vector delivery methods utilised in the literature to deliver these chemogenetic tools. This review evaluates each of the prominent strategies currently utilised for DREADD delivery, discussing their respective advantages and limitations. We focus on adeno-associated virus (AAV)-based and lentivirus-based systems, and the manipulation of these through cell-type specific promoters and pseudotyping. Furthermore, we address how virally mediated DREADD delivery could be improved in order to make it a viable gene therapy strategy and thus expand its translational potential.

Published

2021

367. Adeno-Associated Virus Vector for Central Nervous System Gene Therapy

Author

Danqing Zhu, Paola A. Lopez, David V. Schaffer, and Adam J. Schieferecke

Subjects

0301 basic medicine, Genetic enhancement, Genetic Vectors, Central nervous system, Gene delivery, Bioinformatics, medicine.disease_cause, Virus, 03 medical and health sciences, 0302 clinical medicine, Genome editing, Central Nervous System Diseases, medicine, Animals, Humans, Vector (molecular biology), Molecular Biology, Gene, Adeno-associated virus, business.industry, Genetic Therapy, Dependovirus, Phenotype, 030104 developmental biology, medicine.anatomical_structure, Molecular Medicine, business, 030217 neurology & neurosurgery

Abstract

The past several years have witnessed significant advances in the development of therapeutic gene delivery for neurological disorders of the central nervous system (CNS). In particular, genome-wide sequencing analysis has deepened our understanding of mutations that underlie many monogenic disorders, which in turn has contributed to clinical advances involving adeno-associated virus (AAV) vector delivery of replacement genes to treat recessive disorders. Moreover, gene therapy has been further bolstered with advances in genome editing tools that allow researchers to silence, repair, and amend endogenous genes. However, despite strong preclinical and clinical progress, challenges remain, including delivery and safety. Here, we discuss advances in AAV engineering, recent developments in cargo design, and translation of these technologies towards clinical progress.

Published

2021

368. Intracerebroventricular Administration of AAV9-PHP.B SYN1-EmGFP Induces Widespread Transgene Expression in the Mouse and Monkey Central Nervous System

Author

Blair R. Leavitt, Yoland Smith, Kazi Rahman, Diane Choi, Terri L. Petkau, Andrea J. Korecki, Elizabeth M. Simpson, Austin Hill, Ge Lu, and Adriana Galván

Subjects

Central Nervous System, Synapsin I, Transgene, Genetic Vectors, Green Fluorescent Proteins, Central nervous system, Hippocampus, Biology, medicine.disease_cause, Viral vector, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Neuropil, Animals, Transgenes, Molecular Biology, Adeno-associated virus, Research Articles, 030304 developmental biology, 0303 health sciences, Dependovirus, Synapsins, Macaca mulatta, Cell biology, medicine.anatomical_structure, Cerebral cortex, 030220 oncology & carcinogenesis, Molecular Medicine

Abstract

Viral vectors made from adeno-associated virus (AAV) have emerged as preferred tools in basic and translational neuroscience research to introduce or modify genetic material in cells of interest. The use of viral vectors is particularly attractive in nontransgenic species, such as nonhuman primates. Injection of AAV solutions into the cerebrospinal fluid is an effective method to achieve a broad distribution of a transgene in the central nervous system. In this study, we conducted injections of AAV9-PHP.B, a recently described AAV capsid mutant, in the lateral ventricle of mice and rhesus macaques. To enhance the expression of the transgene (the tag protein emerald green fluorescent protein [EmGFP]), we used a gene promoter that confers high neuron-specific expression of the transgene, the human synapsin 1 (SYN1) promoter. The efficacy of the viral vector was first tested in mice. Our results show that intracerebroventricular injections of AAV9-PHP.B SYN1-EmGFP-woodchuck hepatitis virus posttranscriptional regulatory element resulted in neuronal EmGFP expression throughout the mice and monkey brains. We have provided a thorough characterization of the brain regions expressing EmGFP in both species. EmGFP was observed in neuronal cell bodies over the whole cerebral cortex and in the cerebellum, as well as in some subcortical regions, including the striatum and hippocampus. We also observed densely labeled neuropil in areas known to receive projections from these regions. Double fluorescence studies demonstrated that EmGFP was expressed by several types of neurons throughout the mouse and monkey brain. Our results demonstrate that a single injection in the lateral ventricle is an efficient method to obtain transgene expression in many cortical and subcortical regions, obviating the need of multiple intraparenchymal injections to cover large brain areas. The use of intraventricular injections of AAV9-PHP.B SYN1-EmGFP could provide a powerful approach to transduce widespread areas of the brain and may contribute to further development of methods to genetically target-specific populations of neurons.

Published

2021

369. Adeno-associated viral (AAV) vector-mediated therapeutics for diabetic cardiomyopathy – current and future perspectives

Author

Rebecca H Ritchie, Miles J De Blasio, Mitchel Tate, and Darnel Prakoso

Subjects

Diabetic Cardiomyopathies, Genetic enhancement, Genetic Vectors, Disease, Bioinformatics, Viral vector, Coronary artery disease, Diabetic Cadiomyopathy, Diabetes mellitus, Diabetic cardiomyopathy, Virology, medicine, Diabetes Mellitus, Animals, Humans, Vector (molecular biology), Review Articles, Uncategorized, Diabetes & Metabolic Disorders, diabetes, business.industry, Pharmacology & Toxicology, Gene Transfer Techniques, AAV, General Medicine, Gene Therapy, Genetic Therapy, Dependovirus, medicine.disease, Cardiovascular System & Vascular Biology, Heart failure, Translational Science, business

Abstract

Diabetes increases the prevalence of heart failure by 6–8-fold, independent of other comorbidities such as hypertension and coronary artery disease, a phenomenon termed diabetic cardiomyopathy. Several key signalling pathways have been identified that drive the pathological changes associated with diabetes-induced heart failure. This has led to the development of multiple pharmacological agents that are currently available for clinical use. While fairly effective at delaying disease progression, these treatments do not reverse the cardiac damage associated with diabetes. One potential alternative avenue for targeting diabetes-induced heart failure is the use of adeno-associated viral vector (AAV) gene therapy, which has shown great versatility in a multitude of disease settings. AAV gene therapy has the potential to target specific cells or tissues, has a low host immune response and has the possibility to represent a lifelong cure, not possible with current conventional pharmacotherapies. In this review, we will assess the therapeutic potential of AAV gene therapy as a treatment for diabetic cardiomyopathy.

Published

2021

370. Subpial delivery of adeno-associated virus 9-synapsin-caveolin-1 (AAV9-SynCav1) preserves motor neuron and neuromuscular junction morphology, motor function, delays disease onset, and extends survival in hSOD1G93A mice.

Author

Wang, Shanshan, Wang, Shanshan, Ichinomiya, Taiga, Savchenko, Paul, Wang, Dongsheng, Sawada, Atsushi, Li, Xiaojing, Duong, Tiffany, Li, Wenxi, Bonds, Jacqueline A, Kim, Eun Jung, Miyanohara, Atsushi, Roth, David M, Patel, Hemal H, Patel, Piyush M, Tadokoro, Takahiro, Marsala, Martin, Head, Brian P, Wang, Shanshan, Wang, Shanshan, Ichinomiya, Taiga, Savchenko, Paul, Wang, Dongsheng, Sawada, Atsushi, Li, Xiaojing, Duong, Tiffany, Li, Wenxi, Bonds, Jacqueline A, Kim, Eun Jung, Miyanohara, Atsushi, Roth, David M, Patel, Hemal H, Patel, Piyush M, Tadokoro, Takahiro, Marsala, Martin, and Head, Brian P

Abstract

Elevating neuroprotective proteins using adeno-associated virus (AAV)-mediated gene delivery shows great promise in combating devastating neurodegenerative diseases. Amyotrophic lateral sclerosis (ALS) is one such disease resulting from loss of upper and lower motor neurons (MNs) with 90-95% of cases sporadic (SALS) in nature. Due to the unknown etiology of SALS, interventions that afford neuronal protection and preservation are urgently needed. Caveolin-1 (Cav-1), a membrane/lipid rafts (MLRs) scaffolding and neuroprotective protein, and MLR-associated signaling components are decreased in degenerating neurons in postmortem human brains. We previously showed that, when crossing our SynCav1 transgenic mouse (TG) with the mutant human superoxide dismutase 1 (hSOD1G93A) mouse model of ALS, the double transgenic mouse (SynCav1 TG/hSOD1G93A) exhibited better motor function and longer survival. The objective of the current study was to test whether neuron-targeted Cav-1 upregulation in the spinal cord using AAV9-SynCav1 could improve motor function and extend longevity in mutant humanized mouse and rat (hSOD1G93A) models of familial (F)ALS. Methods: Motor function was assessed by voluntary running wheel (RW) in mice and forelimb grip strength (GS) and motor evoked potentials (MEP) in rats. Immunofluorescence (IF) microscopy for choline acetyltransferase (ChAT) was used to assess MN morphology. Neuromuscular junctions (NMJs) were measured by bungarotoxin-a (Btx-a) and synaptophysin IF. Body weight (BW) was measured weekly, and the survival curve was determined by Kaplan-Meier analysis. Results: Following subpial gene delivery to the lumbar spinal cord, male and female hSOD1G93A mice treated with SynCav1 exhibited delayed disease onset, greater running-wheel performance, preserved spinal alpha-motor neuron morphology and NMJ integrity, and 10% increased longevity, independent of affecting expression of the mutant hSOD1G93A protein. Cervical subpial SynCav1 delivery to hSOD

Published

2022

371. Global Seroprevalence of Pre-existing Immunity Against AAV5 and Other AAV Serotypes in People with Hemophilia A.

Author

Klamroth, Robert, Klamroth, Robert, Hayes, Gregory, Andreeva, Tatiana, Gregg, Keith, Suzuki, Takashi, Mitha, Ismail Haroon, Hardesty, Brandon, Shima, Midori, Pollock, Toni, Slev, Patricia, Oldenburg, Johannes, Ozelo, Margareth C, Stieltjes, Natalie, Castet, Sabine-Marie, Mahlangu, Johnny, Peyvandi, Flora, Kazmi, Rashid, Schved, Jean-François, Leavitt, Andrew D, Callaghan, Michael, Pan-Petesch, Brigitte, Quon, Doris V, Andrews, Jayson, Trinh, Alex, Li, Mingjin, Wong, Wing Yen, Klamroth, Robert, Klamroth, Robert, Hayes, Gregory, Andreeva, Tatiana, Gregg, Keith, Suzuki, Takashi, Mitha, Ismail Haroon, Hardesty, Brandon, Shima, Midori, Pollock, Toni, Slev, Patricia, Oldenburg, Johannes, Ozelo, Margareth C, Stieltjes, Natalie, Castet, Sabine-Marie, Mahlangu, Johnny, Peyvandi, Flora, Kazmi, Rashid, Schved, Jean-François, Leavitt, Andrew D, Callaghan, Michael, Pan-Petesch, Brigitte, Quon, Doris V, Andrews, Jayson, Trinh, Alex, Li, Mingjin, and Wong, Wing Yen

Abstract

Adeno-associated virus (AAV)-mediated gene therapy may provide durable protection from bleeding events and reduce treatment burden for people with hemophilia A (HA). However, pre-existing immunity against AAV may limit transduction efficiency and hence treatment success. Global data on the prevalence of AAV serotypes are limited. In this global, prospective, noninterventional study, we determined the prevalence of pre-existing immunity against AAV2, AAV5, AAV6, AAV8, and AAVrh10 among people ≥12 years of age with HA and residual FVIII levels ≤2 IU/dL. Antibodies against each serotype were detected using validated, electrochemiluminescent-based enzyme-linked immunosorbent assays. To evaluate changes in antibody titers over time, 20% of participants were retested at 3 and 6 months. In total, 546 participants with HA were enrolled at 19 sites in 9 countries. Mean (standard deviation) age at enrollment was 36.0 (14.87) years, including 12.5% younger than 18 years, and 20.0% 50 years of age and older. On day 1, global seroprevalence was 58.5% for AAV2, 34.8% for AAV5, 48.7% for AAV6, 45.6% for AAV8, and 46.0% for AAVrh10. Considerable geographic variability was observed in the prevalence of pre-existing antibodies against each serotype, but AAV5 consistently had the lowest seroprevalence across the countries studied. AAV5 seropositivity rates were 51.8% in South Africa (n = 56), 46.2% in Russia (n = 91), 40% in Italy (n = 20), 37.2% in France (n = 86), 26.8% in the United States (n = 71), 26.9% in Brazil (n = 26), 28.1% in Germany (n = 89), 29.8% in Japan (n = 84), and 5.9% in the United Kingdom (n = 17). For all serotypes, seropositivity tended to increase with age. Serostatus and antibody titer were generally stable over the 6-month sampling period. As clinical trials of AAV-mediated gene therapies progress, data on the natural prevalence of antibodies against various AAV serotypes may become increasingly important.

Published

2022

372. AAV Deployment of Enhancer-Based Expression Constructs In Vivo in Mouse Brain.

Author

Warren, Tracy L, Warren, Tracy L, Lambert, Jason T, Nord, Alex S, Warren, Tracy L, Warren, Tracy L, Lambert, Jason T, and Nord, Alex S

Abstract

Enhancers are binding platforms for a diverse array of transcription factors that drive specific expression patterns of tissue- and cell-type-specific genes. Multiple means of assessing non-coding DNA and various chromatin states have proven useful in predicting the presence of enhancer sequences in the genome, but validating the activity of these sequences and finding the organs and developmental stages they are active in is a labor-intensive process. Recent advances in adeno-associated virus (AAV) vectors have enabled the widespread delivery of transgenes to mouse tissues, enabling in vivo enhancer testing without necessitating a transgenic animal. This protocol shows how a reporter construct that expresses EGFP under the control of a minimal promoter, which does not drive significant expression on its own, can be used to study the activity patterns of candidate enhancer sequences in the mouse brain. An AAV-packaged reporter construct is delivered to the mouse brain and incubated for 1-4 weeks, after which the animal is sacrificed, and brain sections are observed under a microscope. EGFP appears in cells in which the tested enhancer is sufficient to initiate gene expression, pinpointing the location and developmental stage in which the enhancer is active in the brain. Standard cloning methods, low-cost AAV packaging, and expanding AAV serotypes and methods for in vivo delivery and standard imaging readout make this an accessible approach for the study of how gene expression is regulated in the brain.

Published

2022

373. Fundus imaging of retinal ganglion cells transduced by retrograde transport of rAAV2-retro.

Author

Nanjappa, Rakesh, Nanjappa, Rakesh, Dilbeck, Mikayla D, Economides, John R, Horton, Jonathan C, Nanjappa, Rakesh, Nanjappa, Rakesh, Dilbeck, Mikayla D, Economides, John R, and Horton, Jonathan C

Abstract

Access of adeno-associated virus (AAV) to ganglion cells following intravitreal injection for gene therapy is impeded by the internal limiting membrane of the retina. As an alternative, one could transduce ganglion cells via retrograde transport after virus injection into a retinal target nucleus. It is unknown if recombinant AAV2-retro (rAAV2-retro), a variant of AAV2 developed specifically for retrograde transport, is capable of transducing retinal ganglion cells. To address this issue, equal volumes of rAAV2-retro-hSyn-EGFP and rAAV2-retro-hSyn-mCherry were mixed in a micropipette and injected into the rat superior colliculus. The time-course of viral transduction was tracked by performing serial in vivo fundus imaging. Cells that were labeled by the fluorophores within the first week remained consistent in distribution and relative signal strength on follow-up imaging. Most transduced cells were double-labeled, but some were labeled by only EGFP or mCherry. Fundus images were later aligned with retinal wholemounts. Ganglion cells in the wholemounts matched precisely the cells imaged by fundus photography. As seen in the fundus images, ganglion cells in wholemounts were sometimes labeled by only EGFP or mCherry. Overall, there was detectable label in 32-41% of ganglion cells. Analysis of the number of cells labeled by 0, 1, or 2 fluorophores, based on Poisson statistics, yielded an average of 0.66 virions transducing each ganglion cell. Although this represents a low number relative to the quantity of virus injected into the superior colliculus, the ganglion cells showed sustained and robust fluorescent labeling. In the primate, injection of rAAV2-retro into the lateral geniculate nucleus might provide a viable approach for the transduction of ganglion cells, bypassing the obstacles that have prevented effective gene delivery via intravitreal injection.

Published

2022

374. Immune Responses and Immunosuppressive Strategies for Adeno-Associated Virus-Based Gene Therapy for Treatment of Central Nervous System Disorders: Current Knowledge and Approaches.

Author

Prasad, Suyash, Prasad, Suyash, Dimmock, David P, Greenberg, Benjamin, Walia, Jagdeep S, Sadhu, Chanchal, Tavakkoli, Fatemeh, Lipshutz, Gerald S, Prasad, Suyash, Prasad, Suyash, Dimmock, David P, Greenberg, Benjamin, Walia, Jagdeep S, Sadhu, Chanchal, Tavakkoli, Fatemeh, and Lipshutz, Gerald S

Abstract

Adeno-associated viruses (AAVs) are being increasingly used as gene therapy vectors in clinical studies especially targeting central nervous system (CNS) disorders. Correspondingly, host immune responses to the AAV capsid or the transgene-encoded protein have been observed in various clinical and preclinical studies. Such immune responses may adversely impact patients' health, prevent viral transduction, prevent repeated dosing strategies, eliminate transduced cells, and pose a significant barrier to the potential effectiveness of AAV gene therapy. Consequently, multiple immunomodulatory strategies have been used in attempts to limit immune-mediated responses to the vector, enable readministration of AAV gene therapy, prevent end-organ toxicity, and increase the duration of transgene-encoded protein expression. Herein we review the innate and adaptive immune responses that may occur during CNS-targeted AAV gene therapy as well as host- and treatment-specific factors that could impact the immune response. We also summarize the available preclinical and clinical data on immune responses specifically to CNS-targeted AAV gene therapy and discuss potential strategies for incorporating prophylactic immunosuppression regimens to circumvent adverse immune responses.

Published

2022

375. Engineered AAVs for non-invasive gene delivery to rodent and non-human primate nervous systems.

Author

Chen, Xinhong, Chen, Xinhong, Ravindra Kumar, Sripriya, Adams, Cameron D, Yang, Daping, Wang, Tongtong, Wolfe, Damien A, Arokiaraj, Cynthia M, Ngo, Victoria, Campos, Lillian J, Griffiths, Jessica A, Ichiki, Takako, Mazmanian, Sarkis K, Osborne, Peregrine B, Keast, Janet R, Miller, Cory T, Fox, Andrew S, Chiu, Isaac M, Gradinaru, Viviana, Chen, Xinhong, Chen, Xinhong, Ravindra Kumar, Sripriya, Adams, Cameron D, Yang, Daping, Wang, Tongtong, Wolfe, Damien A, Arokiaraj, Cynthia M, Ngo, Victoria, Campos, Lillian J, Griffiths, Jessica A, Ichiki, Takako, Mazmanian, Sarkis K, Osborne, Peregrine B, Keast, Janet R, Miller, Cory T, Fox, Andrew S, Chiu, Isaac M, and Gradinaru, Viviana

Abstract

Gene therapy offers great promise in addressing neuropathologies associated with the central and peripheral nervous systems (CNS and PNS). However, genetic access remains difficult, reflecting the critical need for the development of effective and non-invasive gene delivery vectors across species. To that end, we evolved adeno-associated virus serotype 9 (AAV9) capsid in mice and validated two capsids, AAV-MaCPNS1 and AAV-MaCPNS2, across rodent species (mice and rats) and non-human primate (NHP) species (marmosets and rhesus macaques). Intravenous administration of either AAV efficiently transduced the PNS in rodents and both the PNS and CNS in NHPs. Furthermore, we used AAV-MaCPNS1 in mice to systemically deliver the following: (1) the neuronal sensor jGCaMP8s to record calcium signal dynamics in nodose ganglia and (2) the neuronal actuator DREADD to dorsal root ganglia to mediate pain. This conclusively demonstrates the translatability of these two systemic AAVs across four species and their functional utility through proof-of-concept studies in mice.

Published

2022

376. Eliminating Panglossian thinking in development of AAV therapeutics

Author

Declan Noone, Glenn F. Pierce, Radoslaw Kaczmarek, David Page, Brian O'Mahony, and Mark W. Skinner

Subjects

Pharmacology, Opinion, business.industry, Genetic Vectors, Drug Discovery, Genetics, MEDLINE, Molecular Medicine, Medicine, Engineering ethics, Dependovirus, business, Molecular Biology

Published

2021

377. Cardioprotective factors against myocardial infarction selected in vivo from an AAV secretome library

Author

Ruozi, Giulia, Bortolotti, Francesca, Mura, Antonio, Tomczyk, Mateusz, Falcione, Antonella, Martinelli, Valentina, Vodret, Simone, Braga, Luca, Dal Ferro, Matteo, Cannatà, Antonio, Zentilin, Lorena, Sinagra, Gianfranco, Zacchigna, Serena, Giacca, Mauro, Ruozi, Giulia, Bortolotti, Francesca, Mura, Antonio, Tomczyk, Mateusz, Falcione, Antonella, Martinelli, Valentina, Vodret, Simone, Braga, Luca, Dal Ferro, Matteo, Cannatà, Antonio, Zentilin, Lorena, Sinagra, Gianfranco, Zacchigna, Serena, and Giacca, Mauro

Subjects

Fibrosi, Myocardial Infarction, Nerve Tissue Proteins, Neoplasm Protein, Mice, Animals, Myocytes, Cardiac, Eye Proteins, Myofibroblasts, Cytokine, Secretome, Heart Failure, Myofibroblast, Ventricular Remodeling, Animal, Eye Protein, General Medicine, Dependovirus, Dependoviru, Fibrosis, Neoplasm Proteins, Mice, Inbred C57BL, Disease Models, Animal, Nerve Tissue Protein, Cytokines

Abstract

Therapies for patients with myocardial infarction and heart failure are urgently needed, in light of the breadth of these conditions and lack of curative treatments. To systematically identify previously unidentified cardioactive biologicals in an unbiased manner in vivo, we developed cardiac FunSel, a method for the systematic, functional selection of effective factors using a library of 1198 barcoded adeno-associated virus (AAV) vectors encoding for the mouse secretome. By pooled vector injection into the heart, this library was screened to functionally select for factors that confer cardioprotection against myocardial infarction. After two rounds of iterative selection in mice, cardiac FunSel identified three proteins [chordin-like 1 (Chrdl1), family with sequence similarity 3 member C (Fam3c), and Fam3b] that preserve cardiomyocyte viability, sustain cardiac function, and prevent pathological remodeling. In particular, Chrdl1 exerted its protective activity by binding and inhibiting extracellular bone morphogenetic protein 4 (BMP4), which resulted in protection against cardiomyocyte death and induction of autophagy in cardiomyocytes after myocardial infarction. Chrdl1 also inhibited fibrosis and maladaptive cardiac remodeling by binding transforming growth factor–β (TGF-β) and preventing cardiac fibroblast differentiation into myofibroblasts. Production of secreted and circulating Chrdl1, Fam3c, and Fam3b from the liver also protected the heart from myocardial infarction, thus supporting the use of the three proteins as recombinant factors. Together, these findings disclose a powerful method for the in vivo, unbiased selection of tissue-protective factors and describe potential cardiac therapeutics.

Published

2022

378. Endobronchial Gene Delivery for Pulmonary Hypertension in a Large Animal Model

Author

Olympia, Bikou and Kiyotake, Ishikawa

Subjects

Disease Models, Animal, Hypertension, Pulmonary, Genetic Vectors, Animals, Humans, Genetic Therapy, Dependovirus

Abstract

Pulmonary hypertension (PH) is a devastating disease with high morbidity and mortality. Despite significant progress in the pharmacotherapy, current treatments only ameliorate the symptoms and cannot heal PH. Gene therapy may target the roots of the disease and holds evident promise. The current bottleneck for lung gene therapy is the delivery method. The requirements for the delivery mode are efficiency, safety, and the ability to target the anatomical site of interest, while avoiding off-target effects. Aerosolized gene delivery has been used in several studies and proven to be an efficient mode of administration for lung gene therapy. In this chapter, we describe a protocol of endobronchial aerosolization for PH gene therapy in a large animal model. Testing of a gene therapy in large animals is essential before clinical testing, since the lung anatomy and (patho)physiology differ immensely between humans and rodents, where most of the proof-of-concept studies are tested. The gene delivery vector is being aerosolized in the peripheral bronchi using a sprayer inserted through a flexible bronchoscope. This delivery mode results in efficient lung uptake and less off-target distribution relative to other airway delivery methods.

Published

2022

379. AAV-Mediated Somatic Gene Editing for Cardiac and Skeletal Muscle in a Large Animal Model

Author

Tilman, Ziegler, Tarik, Bozoglu, and Christian, Kupatt

Subjects

Dystrophin, Gene Editing, Muscular Dystrophy, Duchenne, Disease Models, Animal, Swine, Genetic Vectors, Animals, Genetic Therapy, CRISPR-Cas Systems, Dependovirus, Muscle, Skeletal, RNA, Guide, Kinetoplastida

Abstract

Here we describe a protocol to produce a recombinant adeno-associated viral vector (rAAV)-based system to deliver the CRISPR-Cas9 complex into porcine skeletal muscle and myocardial cells. We initially describe the genomic composition of the rAAV-CRISPR vectors used in our lab. Furthermore, we give a step-by-step instruction into the production of recombinant viral vectors with high yields and purity. Lastly we describe the minimally invasive injection regimes to target the myocardium in a pig.

Published

2022

380. Updates on Cardiac Gene Therapy Research and Methods: Overview of Cardiac Gene Therapy

Author

Francisco J, Romeo, Spyros A, Marvopoulos, and Kiyotake, Ishikawa

Subjects

Genetic Vectors, Gene Transfer Techniques, Heart, Genetic Therapy, Dependovirus

Abstract

Gene therapy has made a significant progress in clinical translation over the past few years with several gene therapy products currently approved or anticipating approval for clinical use. Cardiac gene therapy lags behind that of other areas of diseases, with no application of cardiac gene therapy yet approved for clinical use. However, several clinical trials for gene therapy targeting the heart are underway, and innovative research studies are being conducted to close the gap. The second edition of Cardiac Gene Therapy in Methods in Molecular Biology provides protocols for cutting-edge methodologies used in these studies. In this chapter, we discuss recent updates on cardiac gene therapy studies and provide an overview of the chapters in the book.

Published

2022

381. Design and Production of Heart Chamber-Specific AAV9 Vectors

Author

Alina S, Bilal, Donna J, Thuerauf, Erik A, Blackwood, and Christopher C, Glembotski

Subjects

Mice, Genetic Vectors, Gene Transfer Techniques, Animals, Heart Atria, Dependovirus, Serogroup

Abstract

Adeno-associated virus serotype 9 (AAV9) is often used in heart research involving gene delivery due to its cardiotropism, high transduction efficiency, and little to no pathogenicity, making it highly applicable for gene manipulation, in vivo. However, current AAV9 technology is limited by the lack of strains that can selectively express and elucidate gene function in an atrial- and ventricular-specific manner. In fact, study of gene function in cardiac atria has been limited due to the lack of an appropriate tool to study atrial gene expression in vivo, hindering progress in the study of atrial-specific diseases such as atrial fibrillation, the most common cardiac arrhythmia in the USA.This chapter describes the method for the design and production of such chamber-specific AAV9 vectors, with the use of Nppa and Myl2 promoters to enhance atrial- and ventricular-specific expression. While several gene promoter candidates were considered and tested, Nppa and Myl2 were selected for use here because of their clearly defined regulatory elements that confer cardiac chamber-specific expression. Accordingly, Nppa (-425/+25) and Myl2 (-226/+36) promoter fragments are inserted into AAV9 vectors. The atrial- and ventricular-specific expression conferred by these new recombinant AAV9 was confirmed in a double-fluorescent Cre-dependent reporter mouse model. At only 450 and 262 base pairs of Nppa and Myl2 promoters, respectively, these AAV9 that drive chamber-specific AAV9 transgene expression address two major limitations of AAV9 technology, i.e., achieving chamber-specificity while maximizing space in the AAV genome for insertion of larger transgenes.

Published

2022

382. Assessing Recombinant AAV Shedding After Cardiac Gene Therapy

Author

Melad, Farraha and Eddy, Kizana

Subjects

Genetic Vectors, Genetic Therapy, Dependovirus, Adenoviridae, Cell Line

Abstract

Gene therapy based on recombinant adeno-associated viral (rAAV) vectors has recently made significant progress as a clinical therapeutic. Unlike most traditional medications, gene therapy vectors can be biologically active when shed into the surrounding environment. Here we describe methods for collection and storage of multiple biological specimen samples and a PCR-based method for detection of shed adeno-associated viral (AAV) particles. We also describe a method for use of an infectious replication assay utilizing a cell line stably expressing AAV Rep and Cap genes and superinfection with adenovirus 5 to detect functionality in shed AAV particles.

Published

2022

383. Cell-Based Determination of Neutralizing Antibodies Against Adeno-Associated Virus in Cardiac Gene Therapy

Author

Anjali J, Ravichandran, Renata, Mazurek, and Kiyotake, Ishikawa

Subjects

Genetic Vectors, Humans, Genetic Therapy, Dependovirus, Antibodies, Viral, Serogroup, Antibodies, Neutralizing

Abstract

The field of cardiac gene therapy has seen the rising use of adeno-associated viral (AAV) vectors as a promising therapeutic option for cardiac diseases and heart failure. To achieve intended results of AAV delivery, a majority of clinical studies screen patients for existing neutralizing antibodies that could inhibit the effects of the administered AAV and confound treatment efficacy. The cell-based neutralizing antibody assay offers a method of quantifying and identifying a patient's existing neutralizing antibodies against specific serotypes. Combined with the luciferase assay, the neutralizing antibody assay tests the ability of patient antibodies in the blood to prevent gene transduction of AAV-encoded luciferase gene at ranging serial dilutions. This chapter provides a protocol and experimental techniques to determine the presence of neutralizing antibodies against AAV in the blood.

Published

2022

384. Selective Anti-AAV Antibody Depletion by Hemapheresis and Immunoadsorption

Author

Alejandro, Orlowski and Thomas, Weber

Subjects

Genetic Vectors, Blood Component Removal, Animals, Humans, Genetic Therapy, Dependovirus, Antibodies, Viral, Antibodies, Neutralizing, Rats

Abstract

One of the greatest barriers for the use of adeno-associated vectors (AAV) in gene therapy is the presence of pre-existing antibodies against AAV in the general population. Since many of the anti-AAV antibodies have the ability to neutralize the transduction target tissues, even patients with low antibody titers must be excluded from clinical trials or therapy. In recent years, various methods have been proposed to overcome this problem, unfortunately with limited success. In this chapter, we describe in detail a protocol for hemapheresis with an immunoadsorption matrix to remove specifically anti-AAV antibodies in an in vivo rat model. Furthermore, this chapter describes in detail the methods to determine the efficiency of hemapheresis and immunoadsorption.

Published

2022

385. Cardiac Targeted Adeno-Associated Virus Injection in Rats

Author

Michael G, Katz, Yoav, Hadas, Adam S, Vincek, Nataly, Shtraizent, Eric, Schadt, and Efrat, Eliyahu

Subjects

Genetic Vectors, Gene Transfer Techniques, Animals, Heart, Genetic Therapy, Dependovirus, Rats

Abstract

Gene therapy is a promising approach in the treatment of cardiovascular diseases. The vectors available for cardiovascular gene therapy have significantly improved over time. Cardiac tropism is a primary characteristic of an ideal vector along with a long-term expression profile and a minimal risk of cellular immune response. Preclinical and clinical studies have demonstrated that adeno-associated viral (AAV) vectors are one of the most attractive vehicles for gene transfer. AAV has gained great popularity in the last years because of its biological properties and advantages over other viral vector systems. In this chapter we will describe methods for intracardiac delivery of AAV vector in rats.

Published

2022

386. Adeno-associated virus (AAV)-mediated Cre recombinase expression in melanopsin ganglion cells without leaky expression in rod/cone photoreceptors

Author

Aaron N. Reifler and Kwoon Y. Wong

Subjects

Mice, Light, General Neuroscience, Retinal Cone Photoreceptor Cells, Animals, Dependovirus, Photoreceptor Cells, Vertebrate

Abstract

Constituting about 5 % of mouse retinal ganglion cells (RGCs), intrinsically photosensitive retinal ganglion cells (ipRGCs) express the photopigment melanopsin (gene symbol Opn4) and drive such photoresponses as pupil constriction, melatonin suppression, and circadian photoentrainment. Opn4We have constructed a recombinant serotype-2 adeno-associated virus, rAAV2-Opn4-Cre, with the improved Cre recombinase (iCre) gene under the control of a ∼3kbp Opn4 promoter sequence, and injected it intravitreally into mice to transduce inner retinal neurons while sparing the outer retina.We introduced rAAV2-Opn4-Cre into Cre reporter mice in which enhanced green fluorescent protein (EGFP) expression indicates Cre expression. Single-cell electrophysiological recordings and intracellular dye fills showed that 84 % of the EGFP+ cells were ipRGCs including M1-M6 types, while 16 % were conventional RGCs.Whereas Opn4rAAV2-Opn4-Cre has overcome a significant limitation of Opn4

Published

2022

387. Identification of Novel Retinal Pericyte-Targeting rAAV Vectors Through Directed Evolution

Author

Dwani D. Patel, Damien Marsic, Ramesh Periasamy, Sergei Zolotukhin, and Daniel M. Lipinski

Subjects

Ophthalmology, Macular Degeneration, Mice, Diabetic Retinopathy, Transduction, Genetic, Genetic Vectors, Biomedical Engineering, Animals, Dependovirus, Pericytes

Abstract

Retinal pericytes play a vital role in maintaining retinal homeostasis, and their dysfunction underlies pathogenesis in such vascular eye diseases as diabetic retinopathy and wet age-related macular degeneration. Consequently, retinal pericytes are attractive therapeutic targets for gene therapy, but effectively targeting pericytes with recombinant adeno-associated virus (rAAV) vectors remains a challenge.We introduced genetic modifications into the surface-exposed variable regions of the rAAV2/2 capsid to generate a complex library (1 × 107) of capsid mutants that were then screened for preferential tropism toward retinal pericytes. Using the Tg(Cspg4-DsRed.T1)1Akik/J reporter mouse model, which has red fluorescent pericytes that can be isolated via flow cytometry in order to recover vector genomes, we performed three rounds of screening and identified seven putative mutants capable of transducing retinal pericytes.Following intravitreal administration of mutant vectors packaging ubiquitously expressing green fluorescent protein reporters and postmortem flow cytometry of enzymatically digested retinae, two mutants in particular, Peri-E and Peri-G, demonstrated significantly greater transduction of retinal pericytes than unmodified rAAV2/2 (1.4-fold and 2.8-fold, respectively).Although difficult to characterize the effect of each point mutation in the context of multiple amino acid variations from the wild-type AAV2 sequence, we identified several point mutations that may play critical roles in limiting HSPG binding, evading neutralization by murine A20 monoclonal antibodies, modulating antigenicity, and evading ubiquitination to ultimately improve transduction efficiency of retinal pericytes.Identification of novel retinal pericyte targeting rAAV vectors enables the development of new, long-lasting gene therapies for retinal diseases such as diabetic retinopathy and wet age-related macular degeneration.

Published

2022

388. In Vivo Wide-Field and Two-Photon Calcium Imaging from a Mouse using a Large Cranial Window

Author

Satoshi, Manita, Eiji, Shigetomi, Haruhiko, Bito, Schuichi, Koizumi, and Kazuo, Kitamura

Subjects

Neurons, Mice, Photons, Animals, Calcium, Neocortex, Dependovirus

Abstract

Wide-field calcium imaging from the mouse's neocortex allows one to observe cortex-wide neural activity related to various brain functions. On the other hand, two-photon imaging can resolve the activity of local neural circuits at the single-cell level. It is critical to make a large cranial window to perform multiple-scale analysis using both imaging techniques in the same mouse. To achieve this, one must remove a large section of the skull and cover the exposed cortical surface with transparent materials. Previously, glass skulls and polymer-based cranial windows have been developed for this purpose, but these materials are not easily fabricated. The present protocol describes a simple method for making a large cranial window consisting of commercially available polyvinylidene chloride (PVDC) wrapping film, a transparent silicone plug, and a cover glass. For imaging the dorsal surface of an entire hemisphere, the window size was approximately 6 x 3 mm

Published

2022

389. Stability and Dissociation of Adeno-Associated Viral Capsids by Variable Temperature-Charge Detection-Mass Spectrometry

Author

Marius M. Kostelic, Jack P. Ryan, Levi S. Brown, Tyler W. Jackson, Chih-Chieh Hsieh, Ciara K. Zak, Henry M. Sanders, Yang Liu, Victor Shugui Chen, Michael Byrne, Craig A. Aspinwall, Erin S. Baker, and Michael T. Marty

Subjects

Capsid, Temperature, Capsid Proteins, Dependovirus, Mass Spectrometry, Analytical Chemistry

Abstract

Adeno-associated viral (AAV) vectors have emerged as gene therapy and vaccine delivery systems. Differential scanning fluorimetry or differential scanning calorimetry is commonly used to measure the thermal stability of AAVs, but these global methods are unable to distinguish the stabilities of different AAV subpopulations in the same sample. To address this challenge, we combined charge detection-mass spectrometry (CD-MS) with a variable temperature (VT) electrospray source that controls the temperature of the solution prior to electrospray. Using VT-CD-MS, we measured the thermal stabilities of empty and filled capsids. We found that filled AAVs ejected their cargo first and formed intermediate empty capsids before completely dissociating. Finally, we observed that pH stress caused a major decrease in thermal stability. This new approach better characterizes the thermal dissociation of AAVs, providing the simultaneous measurement of the stabilities and dissociation pathways of different subpopulations.

Published

2022

390. Immunogenicity and toxicity of AAV gene therapy

Author

Hildegund C J, Ertl

Subjects

Genetic Vectors, Immunology, Humans, Immunology and Allergy, Capsid Proteins, Genetic Therapy, Transgenes, Dependovirus

Abstract

Gene transfer using adeno-associated viral (AAV) vectors has made tremendous progress in the last decade and has achieved cures of debilitating diseases such as hemophilia A and B. Nevertheless, progress is still being hampered by immune responses against the AAV capsid antigens or the transgene products. Immunosuppression designed to blunt T cell responses has shown success in some patients but failed in others especially if they received very high AAV vectors doses. Although it was initially thought that AAV vectors induce only marginal innate responses below the threshold of systemic symptoms recent trials have shown that complement activation can results in serious adverse events. Dorsal root ganglia toxicity has also been identified as a complication of high vector doses as has severe hepatotoxicity. Most of the critical complications occur in patients who are treated with very high vector doses indicating that the use of more efficient AAV vectors to allow for dose sparing or giving smaller doses repeatedly, the latter in conjunction with antibody or B cell depleting measures, should be explored.

Published

2022

391. Adeno-associated virus infection and its impact in human health: an overview

Author

Thaís B Sant’Anna and Natalia M Araujo

Subjects

Infectious Diseases, Carcinoma, Hepatocellular, Pregnancy, Virology, Placenta, Liver Neoplasms, Genetic Vectors, Humans, Female, Cervix Uteri, Dependovirus

Abstract

Discovered as a contaminant of adenovirus stocks in the 1960s, adeno-associated virus (AAV) is a mono-stranded DNA virus that depends on helper factors to replicate. Even though AAV is endemic in the human population (35–80%), it is remarkable that many issues concerning the natural infection by this virus remain unanswered. In this study, we reflect on the main basic aspects of AAV biology and provide an overview of the studies exploring the impact of AAV infection on human health, focusing on three major research areas including, (i) cervical and (ii) liver cancer, and (iii) reproductive system disorders. Conflicting results have been obtained into the association of AAV infection with the occurrence of adverse reproductive outcomes, such as placental complications, spontaneous abortion, and fertility disorders, or with a protective role in HPV-related cervical carcinogenesis. Noteworthy, recent reports have identified AAV insertional mutagenesis as a novel risk factor for the development of hepatocellular carcinoma. This latest finding raises concern regarding the widespread usage of AAV vectors in liver-targeted gene therapy.

Published

2022

392. The tyrosine capsid mutations on retrograde adeno-associated virus accelerates gene transduction efficiency

Author

Ryota, Nakahama, Aika, Saito, Sensho, Nobe, Kazuya, Togashi, Ikuo K, Suzuki, Akira, Uematsu, and Kazuo, Emoto

Subjects

Mice, Cellular and Molecular Neuroscience, Capsid, Transduction, Genetic, Genetic Vectors, Mutation, Animals, Tyrosine, Dependovirus, Molecular Biology

Abstract

Adeno-associated virus (AAV) vector is a critical tool for gene delivery through its durable transgene expression and safety profile. Among many serotypes, AAV2-retro is typically utilized for dissecting neural circuits with its retrograde functionality. However, this vector requires a relatively long-term incubation period (over 2 weeks) to obtain enough gene expression levels presumably due to low efficiency in gene transduction. Here, we aimed to enhance transgene expression efficiency of AAV2-retro vectors by substituting multiple tyrosine residues with phenylalanines (YF mutations) in the virus capsid, which is previously reported to improve the transduction efficiency of AAV2-infected cells by evading host cell responses. We found that AAV2-retro with YF mutations (AAV2-retroYF)-mediated transgene expression was significantly enhanced in the primary culture of murine cortical neurons at 1 week after application, comparable to that of the conventional AAV2-retro at 2 week after application. Moreover, transgene expressions in the retrogradely labeled neurons mediated by AAV2-retroYF were significantly increased both in the cortico-cortical circuits and in the subcortical circuits in vivo, while the retrograde functionality of AAV2-retroYF was equally effective as that of AAV2-retro. Our data indicate that YF mutations boost AAV2-retro-mediated retrograde gene transduction in vivo and suggest that the AAV2-retroYF should be useful for efficient targeting of the projection-defined neurons, which is suited to applications for dissecting neural circuits during development as well as future clinical applications.

Published

2022

393. AAV and hepatitis: Cause or coincidence?

Author

Ype P. de Jong and Roland W. Herzog

Subjects

Pharmacology, Drug Discovery, Genetics, Molecular Medicine, Humans, Dependovirus, Molecular Biology, Hepatitis

Published

2022

394. Emerging Gene Manipulation Strategies for the Treatment of Monogenic Eye Disease

Author

Frederick R. Burgess, Hildegard Nikki Hall, and Roly Megaw

Subjects

Adult, cis-trans-Isomerases, Leber, Eye Diseases, Genetic Vectors, Leber Congenital Amaurosis, General Medicine, Genetic Therapy, RPE65, Dependovirus, gene therapy, Ophthalmology, retinitis pigmentosa, Mutation, Humans, Child, Luxturna

Abstract

Genetic eye diseases, representing a wide spectrum of simple and complex conditions, are one of the leading causes of visual loss in children and working adults, and progress in the field has led to changes in disease investigation, diagnosis, and management. The past 15 years have seen the emergence of novel therapies for these previously untreatable conditions to the extent that we now have a licensed therapy for one form of genetic eye disease and many more in clinical trial. This is a systematic review of published and ongoing clinical trials of gene therapies for monogenic eye diseases. Databases of clinical trials and the published literature were searched for interventional studies of gene therapies for eye diseases. Standard methodological procedures were used to assess the relevance of search results. A total of 59 registered clinical trials are referenced, showing the significant level of interest in the potential for translation of these therapies from bench to bedside. The breadth of therapy design is encouraging, providing multiple possible therapeutic mechanisms. Some fundamental questions regarding gene therapy for genetic eye diseases remain, such as optimal dosing, the relative benefits of adeno-associated virus (AAV)-packaging and the potential for a significant inflammatory response to the therapy itself. As a result, despite the promise of the eye as a target, it has proven difficult to deliver clinically effective gene therapies to the eye. Despite setbacks, the licensing of Luxturna (voretigene neparvovec, Novartis) for the treatment of RPE65-mediated Leber congenital amaurosis (LCA) is a major advance in efforts to treat these rare, but devastating, causes of visual loss.

Published

2022

395. Recombinant Adeno-Associated Viral Vector-Mediated Gene Transfer of

Author

Melad, Farraha, Renuka, Rao, Sindhu, Igoor, Thi Y L, Le, Michael A, Barry, Christopher, Davey, Cindy, Kok, James J H, Chong, and Eddy, Kizana

Subjects

Biological Clocks, Genetic Vectors, Action Potentials, Animals, Myocytes, Cardiac, Dependovirus, Rats, Sinoatrial Node

Abstract

Sinoatrial node dysfunction can manifest as bradycardia, leading to symptoms of syncope and sudden cardiac death. Electronic pacemakers are the current standard of care but are limited due to a lack of biological chronotropic control, cost of revision surgeries, and risk of lead- and device-related complications. We therefore aimed to develop a biological alternative to electronic devices by using a clinically relevant gene therapy vector to demonstrate conversion of cardiomyocytes into sinoatrial node-like cells in an in vitro context. Neonatal rat ventricular myocytes were transduced with recombinant adeno-associated virus vector 6 encoding either

Published

2022

396. Sterile protection and transmission blockade by a multistage anti-malarial vaccine in the pre-clinical study

Author

Mitsuhiro Iyori, Andrew M. Blagborough, Tetsushi Mizuno, Yu-ichi Abe, Mio Nagaoka, Naoto Hori, Iroha Yamagoshi, Dari F. Da, William F. Gregory, Ammar A. Hasyim, Yutaro Yamamoto, Akihiko Sakamoto, Kunitaka Yoshida, Hiroaki Mizukami, Hisatoshi Shida, Shigeto Yoshida, and Apollo - University of Cambridge Repository

Subjects

plasmodium falciparum, PfCSP, Immunology, malaria, Protozoan Proteins, Antibodies, Protozoan, LC16m8Δ, adeno-associated virus (AAV), Dependovirus, Antimalarials, Disease Models, Animal, Mice, Pfs25, vaccine, Malaria Vaccines, Immunology and Allergy, Animals, Humans, Malaria, Falciparum

Abstract

Peer reviewed: True, The Malaria Vaccine Technology Roadmap 2013 (World Health Organization) aims to develop safe and effective vaccines by 2030 that will offer at least 75% protective efficacy against clinical malaria and reduce parasite transmission. Here, we demonstrate a highly effective multistage vaccine against both the pre-erythrocytic and sexual stages of Plasmodium falciparum that protects and reduces transmission in a murine model. The vaccine is based on a viral-vectored vaccine platform, comprising a highly-attenuated vaccinia virus strain, LC16m8Δ (m8Δ), a genetically stable variant of a licensed and highly effective Japanese smallpox vaccine LC16m8, and an adeno-associated virus (AAV), a viral vector for human gene therapy. The genes encoding P. falciparum circumsporozoite protein (PfCSP) and the ookinete protein P25 (Pfs25) are expressed as a Pfs25-PfCSP fusion protein, and the heterologous m8Δ-prime/AAV-boost immunization regimen in mice provided both 100% protection against PfCSP-transgenic P. berghei sporozoites and up to 100% transmission blocking efficacy, as determined by a direct membrane feeding assay using parasites from P. falciparum-positive, naturally-infected donors from endemic settings. Remarkably, the persistence of vaccine-induced immune responses were over 7 months and additionally provided complete protection against repeated parasite challenge in a murine model. We propose that application of the m8Δ/AAV malaria multistage vaccine platform has the potential to contribute to the landmark goals of the malaria vaccine technology roadmap, to achieve life-long sterile protection and high-level transmission blocking efficacy.

Published

2022

397. Adeno-associated virus-based malaria booster vaccine following attenuated replication-competent vaccinia virus LC16m8Δ priming

Author

Ammar A. Hasyim, Mitsuhiro Iyori, Tetsushi Mizuno, Yu-ichi Abe, Iroha Yamagoshi, Yenni Yusuf, Intan Syafira, Mohammad Shahnaij, Akihiko Sakamoto, Yutaro Yamamoto, Hiroaki Mizukami, Hisatoshi Shida, and Shigeto Yoshida

Subjects

Mice, Infectious Diseases, Sporozoites, Malaria Vaccines, Animals, Parasitology, Vaccinia virus, Dependovirus, Malaria

Abstract

We previously demonstrated that boosting with adeno-associated virus (AAV) type 1 (AAV1) can induce highly effective and long-lasting protective immune responses against malaria parasites when combined with replication-deficient adenovirus priming in a rodent model. In the present study, we compared the efficacy of two different AAV serotypes, AAV1 and AAV5, as malaria booster vaccines following priming with the attenuated replication-competent vaccinia virus strain LC16m8Δ (m8Δ), which harbors the fusion gene encoding both the pre-erythrocytic stage protein, Plasmodium falciparum circumsporozoite (PfCSP) and the sexual stage protein (Pfs25) in a two-dose heterologous prime-boost immunization regimen. Both regimens, m8Δ/AAV1 and m8Δ/AAV5, induced robust anti-PfCSP and anti-Pfs25 antibodies. To evaluate the protective efficacy, the mice were challenged with sporozoites twice after immunization. At the first sporozoite challenge, m8Δ/AAV5 achieved 100% sterile protection whereas m8Δ/AAV1 achieved 70% protection. However, at the second challenge, 100% of the surviving mice from the first challenge were protected in the m8Δ/AAV1 group whereas only 55.6% of those in the m8Δ/AAV5 group were protected. Regarding the transmission-blocking efficacy, we found that both immunization regimens induced high levels of transmission-reducing activity (99%) and transmission-blocking activity (95%). Our data indicate that the AAV5-based multistage malaria vaccine is as effective as the AAV1-based vaccine when administered following an m8Δ-based vaccine. These results suggest that AAV5 could be a viable alternate vaccine vector as a malaria booster vaccine.

Published

2022

398. Secretion of functional α1-antitrypsin is cell type dependent: Implications for intramuscular delivery for gene therapy

Author

Haiping Ke, Kevin P. Guay, Terence R. Flotte, Lila M. Gierasch, Anne Gershenson, and Daniel N. Hebert

Subjects

Cricetulus, Multidisciplinary, Transduction, Genetic, Cricetinae, alpha 1-Antitrypsin, alpha 1-Antitrypsin Deficiency, Muscle Fibers, Skeletal, Hepatocytes, Animals, Humans, CHO Cells, Genetic Therapy, Dependovirus

Abstract

Heterologous expression of proteins is used widely for the biosynthesis of biologics, many of which are secreted from cells. In addition, gene therapy and messenger RNA (mRNA) vaccines frequently direct the expression of secretory proteins to nonnative host cells. Consequently, it is crucial to understand the maturation and trafficking of proteins in a range of host cells including muscle cells, a popular therapeutic target due to the ease of accessibility by intramuscular injection. Here, we analyzed the production efficiency for α1-antitrypsin (AAT) in Chinese hamster ovary cells, commonly used for biotherapeutic production, and myoblasts (embryonic progenitor cells of muscle cells) and compared it to the production in the major natural cells, liver hepatocytes. AAT is a target protein for gene therapy to address pathologies associated with insufficiencies in native AAT activity or production. AAT secretion and maturation were most efficient in hepatocytes. Myoblasts were the poorest of the cell types tested; however, secretion of active AAT was significantly augmented in myoblasts by treatment with the proteostasis regulator suberoylanilide hydroxamic acid, a histone deacetylase inhibitor. These findings were extended and validated in myotubes (mature muscle cells) where AAT was transduced using an adeno-associated viral capsid transduction method used in gene therapy clinical trials. Overall, our study sheds light on a possible mechanism to enhance the efficacy of gene therapy approaches for AAT and, moreover, may have implications for the production of proteins from mRNA vaccines, which rely on the expression of viral glycoproteins in nonnative host cells upon intramuscular injection.

Published

2022

399. Intravitreal Injections in the Ovine Eye

Author

Nadia Mitchell and Samantha Jane Murray

Subjects

Sheep, General Immunology and Microbiology, General Chemical Engineering, General Neuroscience, Genetic Vectors, Intravitreal Injections, Animals, Genetic Therapy, Dependovirus, General Biochemistry, Genetics and Molecular Biology, Retina

Abstract

There are several methods for the delivery of therapeutic agents to the retina, including intravitreal (IVT), subretinal, suprachoroidal, periocular, or topical administration. IVT drug delivery involves an injection into the vitreous humor of the eye, a gelatinous substance that fills the posterior chamber of the eye and maintains the shape of the eye globe. Although the IVT route is less specifically targeted than subretinal delivery, it is much less invasive and is widely used in clinical settings for a range of ocular diseases. We previously demonstrated the efficacy of intravitreal delivery of an adeno-associated virus (AAV)-mediated gene therapy product (AAV9.CLN5) in sheep with a naturally occurring CLN5 form of neuronal ceroid lipofuscinosis (NCL). Affected sheep received IVT gene therapy in one eye, with the other untreated eye serving as an internal control. Retinal structure and function were maintained in the treated eye up to 15 months after treatment, while the untreated eye displayed progressively declining function and severe atrophy during postmortem examination. Based on the sheep studies, the CLN5 gene therapy product was cleared as a candidate investigational new drug (IND) by the United States Food and Drug Administration in September 2021. This paper details the surgical protocol for IVT delivery of a therapeutic viral vector to the ovine eye.

Published

2022

400. Engineered AAVs for non-invasive gene delivery to rodent and non-human primate nervous systems

Author

Xinhong Chen, Sripriya Ravindra Kumar, Cameron D. Adams, Daping Yang, Tongtong Wang, Damien A. Wolfe, Cynthia M. Arokiaraj, Victoria Ngo, Lillian J. Campos, Jessica A. Griffiths, Takako Ichiki, Sarkis K. Mazmanian, Peregrine B. Osborne, Janet R. Keast, Cory T. Miller, Andrew S. Fox, Isaac M. Chiu, and Viviana Gradinaru

Subjects

Central Nervous System, Mice, Transduction, Genetic, General Neuroscience, viruses, Genetic Vectors, Gene Transfer Techniques, Animals, Rodentia, Genetic Therapy, Dependovirus, Macaca mulatta, Rats

Abstract

Gene therapy offers great promise in addressing neuropathologies associated with the central and peripheral nervous systems (CNS and PNS). However, genetic access remains difficult, reflecting the critical need for the development of effective and non-invasive gene delivery vectors across species. To that end, we evolved adeno-associated virus serotype 9 (AAV9) capsid in mice and validated two capsids, AAV-MaCPNS1 and AAV-MaCPNS2, across rodent species (mice and rats) and non-human primate (NHP) species (marmosets and rhesus macaques). Intravenous administration of either AAV efficiently transduced the PNS in rodents and both the PNS and CNS in NHPs. Furthermore, we used AAV-MaCPNS1 in mice to systemically deliver the following: (1) the neuronal sensor jGCaMP8s to record calcium signal dynamics in nodose ganglia and (2) the neuronal actuator DREADD to dorsal root ganglia to mediate pain. This conclusively demonstrates the translatability of these two systemic AAVs across four species and their functional utility through proof-of-concept studies in mice.

Published

2022