An update on canine adenovirus type 2 and its vectors.

Viruses

Institut de Génétique Moléculaire de Montpellier, CNRS UMR 5535, 1919 Route de Mende Montpellier, 34293 France.

Published: September 2010

AI Article Synopsis

  • Adenovirus vectors, particularly human-derived adenoviruses (HAd), have shown promise for effective gene transfer and immune response induction, but clinical use may be hampered by existing immunity in patients.
  • Canine adenovirus serotype 2 (CAV-2) offers a valuable alternative, as it can be engineered to avoid immune responses and has strong neural targeting capabilities.
  • CAV-2 vectors are being explored for various applications, including treating neurodegenerative diseases, developing vaccines, and creating hybrid vectors for targeted therapies.

Article Abstract

Adenovirus vectors have significant potential for long- or short-term gene transfer. Preclinical and clinical studies using human derived adenoviruses (HAd) have demonstrated the feasibility of flexible hybrid vector designs, robust expression and induction of protective immunity. However, clinical use of HAd vectors can, under some conditions, be limited by pre-existing vector immunity. Pre-existing humoral and cellular anti-capsid immunity limits the efficacy and duration of transgene expression and is poorly circumvented by injections of larger doses and immuno-suppressing drugs. This review updates canine adenovirus serotype 2 (CAV-2, also known as CAdV-2) biology and gives an overview of the generation of early region 1 (E1)-deleted to helper-dependent (HD) CAV-2 vectors. We also summarize the essential characteristics concerning their interaction with the anti-HAd memory immune responses in humans, the preferential transduction of neurons, and its high level of retrograde axonal transport in the central and peripheral nervous system. CAV-2 vectors are particularly interesting tools to study the pathophysiology and potential treatment of neurodegenerative diseases, as anti-tumoral and anti-viral vaccines, tracer of synaptic junctions, oncolytic virus and as a platform to generate chimeric vectors.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3185752PMC
http://dx.doi.org/10.3390/v2092134DOI Listing

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