Severe Toxicity in Nonhuman Primates and Piglets Following High-Dose Intravenous Administration of an Adeno-Associated Virus Vector Expressing Human SMN

Hinderer, Christian; Katz, Nathan; Buza, Elizabeth L.; Dyer, Cecilia; Goode, Tamara; Bell, Peter; Richman, Laura K.; Wilson, James M.

doi:10.1089/hum.2018.015

Cited by 566 publications

(511 citation statements)

References 33 publications

(44 reference statements)

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“…Another example, where results from rodent studies do not translate directly to studies with large animal models, is the recent observation that high doses (2e14 GC/kg) of rAAV9 vectors can lead to severe acute toxicity in piglets and non-human primates when delivered intravenously [91,92]. In this case, and different from the trial results reported by Manno et al [59], the toxicity was likely due to an acute, innate immune response (around 5 days after vector administration).…”

Section: Lessons Learned From Ex-vivo Successmentioning

confidence: 99%

Lessons learned from lung and liver in-vivo gene therapy: implications for the future

Haasteren

Hyde

Gill

2018

Expert Opinion on Biological Therapy

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Introduction: Ex-vivo gene therapy has had significant clinical impact over the last couple of years and in-vivo gene therapy products are being approved for clinical use. Gene therapy and gene editing approaches have huge potential to treat genetic disease and chronic illness. Areas covered: This article provides a review of in-vivo approaches for gene therapy in the lung and liver, exploiting non-viral and viral vectors with varying serotypes and pseudotypes to target-specific cells. Antibody responses inhibiting viral vectors continue to constrain effective repeat administration. Lessons learned from ex-vivo gene therapy and genome editing are also discussed. Expert opinion: The fields of lung and liver in-vivo gene therapy are thriving and a comparison highlights obstacles and opportunities for both. Overcoming immunological issues associated with repeated administration of viral vectors remains a key challenge. The addition of targeted small molecules in combination with viral vectors may offer one solution. A substantial bottleneck to the widespread adoption of in-vivo gene therapy is how to ensure sufficient capacity for clinical-grade vector production. In the future, the exploitation of gene editing approaches for in-vivo disease treatment may facilitate the resurgence of non-viral gene transfer approaches, which tend to be eclipsed by more efficient viral vectors.

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Section: Lessons Learned From Ex-vivo Successmentioning

confidence: 99%

Lessons learned from lung and liver in-vivo gene therapy: implications for the future

Haasteren

Hyde

Gill

2018

Expert Opinion on Biological Therapy

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“…For example, a recent experiment in rhesus monkeys found that the high doses of AAV that may need to be delivered intravenously for some therapies could be prohibitively toxic. 52 In three out of three primates and three out of three piglets, the investigators found that the high doses of AAV used resulted in severe toxicity, including hepatocellular necrosis and axonopathies in both the central and peripheral nervous system of the monkeys, and neuronal degeneration in the dorsal root ganglia of the piglets. In commenting on this report, Flotte et al 53 noted that the doses used in the animals with these serious outcomes are nevertheless being used in human trials that so far have not encountered dose-limiting toxicity, and that the toxicity encountered in the primates and piglets could have been due to some unidentified contaminants in the viral preparation.…”

Section: Clinical Trial Issuesmentioning

confidence: 99%

“…A second reason for caution is that the limitations of gene therapy vectors for treatments requiring distribution to the entire body, as some gene‐editing treatments might require, are still being learned and may not always be appreciated. For example, a recent experiment in rhesus monkeys found that the high doses of AAV that may need to be delivered intravenously for some therapies could be prohibitively toxic . In three out of three primates and three out of three piglets, the investigators found that the high doses of AAV used resulted in severe toxicity, including hepatocellular necrosis and axonopathies in both the central and peripheral nervous system of the monkeys, and neuronal degeneration in the dorsal root ganglia of the piglets.…”

Section: Challenge 1: Avoiding Overoptimismmentioning

confidence: 99%

How will the field of gene therapy survive its success?

Kaemmerer¹

2018

Bioengineering & Transla Med

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In August 2017, for the first time, a gene therapy was approved for market release in the United States. That approval was followed by two others before the end of the year. This article cites primary literature, review articles concerning particular biotechnologies, and press releases by the FDA and others in order to provide an overview of the current status of the field of gene therapy with respect to its translation into practice. Technical hurdles that have been overcome in the past decades are summarized, as are hurdles that need to be the subject of continued research. Then, some social and practical challenges are identified that must be overcome if the field of gene therapy, having survived past failures, is to achieve not only technical and clinical but also market success. One of these, the need for an expanded capacity for the manufacturing of viral vectors to be able to meet the needs of additional gene therapies that will be coming soon, is a challenge that the talents of current and future bioengineers may help address.

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“…Remarkably, this treatment triggered elevated serum aminotransferase levels in only few patients and these were attenuated by prednisolone. In contrast, a separate study employing pigs and NHPs exposed to dose‐matched AAV9 expressing the same transgene and administered similarly showed massive vector and transgene‐related toxicity, motor neuron degeneration, and even fatalities (Hinderer et al, ). The discrepancy between large animal models and clinical observations is difficult to reconcile but may highlight the inherent limitations of animal models as predictors of outcome for human studies.…”

Section: Adeno‐associated Viruses—research Tools and Gene Therapymentioning

confidence: 99%

Adeno‐associated virus‐based Alzheimer's disease mouse models and potential new therapeutic avenues

Ittner

Klugmann

2019

British J Pharmacology

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Alzheimer's disease (AD) is a highly prevalent neurodegenerative condition that presents with cognitive decline. The current understanding of underlying disease mechanisms remains incomplete. Genetically modified mouse models have been instrumental in deciphering pathomechanisms in AD. While these models were typically generated by classical transgenesis and genome editing, the use of adeno‐associated viruses (AAVs) to model and investigate AD in mice, as well as to develop novel gene‐therapy approaches, is emerging. Here, we reviewed literature that used AAVs to study and model AD and discuss potential gene therapy strategies. Linked Articles This article is part of a themed section on Therapeutics for Dementia and Alzheimer's Disease: New Directions for Precision Medicine. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v176.18/issuetoc

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Severe Toxicity in Nonhuman Primates and Piglets Following High-Dose Intravenous Administration of an Adeno-Associated Virus Vector Expressing Human SMN

Cited by 566 publications

References 33 publications

Lessons learned from lung and liver in-vivo gene therapy: implications for the future

Lessons learned from lung and liver in-vivo gene therapy: implications for the future

How will the field of gene therapy survive its success?

Adeno‐associated virus‐based Alzheimer's disease mouse models and potential new therapeutic avenues

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