AI Article Synopsis

  • Scientists are trying to create a safe way to protect people from diseases like HIV using gene-based treatments that deliver special antibodies.
  • They tested this method on rhesus macaques and found that the best results happened with a specific amount of the delivery system in each injection and more injections helped increase the effect.
  • The study showed that this gene therapy could work well to boost immunity, and it also suggested that testing on monkeys can help understand how it might work in humans later on.

Article Abstract

Gene based delivery of immunoglobulins promises to safely and durably provide protective immunity to individuals at risk of acquiring infectious diseases such as HIV. We used a rhesus macaque animal model to optimize delivery of naturally-arising, autologous anti-SIV neutralizing antibodies expressed by Adeno-Associated Virus 8 (AAV8) vectors. Vectored transgene expression was confirmed by quantitation of target antibody abundance in serum and mucosal surfaces. We tested the expression achieved at varying doses and numbers of injections. Expression of the transgene reached a saturation at about 2 x 10(12) AAV8 genome copies (gc) per needle-injection, a physical limitation that may not scale clinically into human trials. In contrast, expression increased proportionately with the number of injections. In terms of anti-drug immunity, anti-vector antibody responses were universally strong, while those directed against the natural transgene mAb were detected in only 20% of animals. An anti-transgene antibody response was invariably associated with loss of detectable plasma expression of the antibody. Despite having atypical glycosylation profiles, transgenes derived from AAV-directed muscle cell expression retained full functional activity, including mucosal accumulation, in vitro neutralization, and protection against repeated limiting dose SIVsmE660 swarm challenge. Our findings demonstrate feasibility of a gene therapy-based passive immunization strategy against infectious disease, and illustrate the potential for the nonhuman primate model to inform clinical AAV-based approaches to passive immunization.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6296672PMC
http://dx.doi.org/10.1371/journal.ppat.1007395DOI Listing

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