Literature DB >> 20087317

Intensive pharmacological immunosuppression allows for repetitive liver gene transfer with recombinant adenovirus in nonhuman primates.

Antonio Fontanellas1, Sandra Hervás-Stubbs, Itsaso Mauleón, Juan Dubrot, Uxua Mancheño, María Collantes, Ana Sampedro, Carmen Unzu, Carlos Alfaro, Asis Palazón, Cristian Smerdou, Alberto Benito, Jesús Prieto, Iván Peñuelas, Ignacio Melero.   

Abstract

Repeated administration of gene therapies is hampered by host immunity toward vectors and transgenes. Attempts to circumvent antivector immunity include pharmacological immunosuppression or alternating different vectors and vector serotypes with the same transgene. Our studies show that B-cell depletion with anti-CD20 monoclonal antibody and concomitant T-cell inhibition with clinically available drugs permits repeated liver gene transfer to a limited number of nonhuman primates with recombinant adenovirus. Adenoviral vector-mediated transfer of the herpes simplex virus type 1 thymidine kinase (HSV1-tk) reporter gene was visualized in vivo with a semiquantitative transgene-specific positron emission tomography (PET) technique, liver immunohistochemistry, and immunoblot for the reporter transgene in needle biopsies. Neutralizing antibody and T cell-mediated responses toward the viral capsids were sequentially monitored and found to be repressed by the drug combinations tested. Repeated liver transfer of the HSV1-tk reporter gene with the same recombinant adenoviral vector was achieved in macaques undergoing a clinically feasible immunosuppressive treatment that ablated humoral and cellular immune responses. This strategy allows measurable gene retransfer to the liver as late as 15 months following the first adenoviral exposure in a macaque, which has undergone a total of four treatments with the same adenoviral vector.

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Year:  2010        PMID: 20087317      PMCID: PMC2862529          DOI: 10.1038/mt.2009.312

Source DB:  PubMed          Journal:  Mol Ther        ISSN: 1525-0016            Impact factor:   11.454


  50 in total

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4.  Sequestration of adenoviral vector by Kupffer cells leads to a nonlinear dose response of transduction in liver.

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5.  Administration of helper-dependent adenoviral vectors and sequential delivery of different vector serotype for long-term liver-directed gene transfer in baboons.

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Review 2.  Adenoviral vector immunity: its implications and circumvention strategies.

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6.  Adenovirus Biodistribution is Modified in Sensitive Animals Compared to Naïve Animals.

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7.  Transient and intensive pharmacological immunosuppression fails to improve AAV-based liver gene transfer in non-human primates.

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8.  Oncolytic adenoviruses armed with thymidine kinase can be traced by PET imaging and show potent antitumoural effects by ganciclovir dosing.

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9.  Systemic delivery of oncolytic viruses: hopes and hurdles.

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10.  Ultrasound-assisted nonviral gene transfer of AQP1 to the irradiated minipig parotid gland restores fluid secretion.

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