ADENOVIRUS-MEDIATED GENE TRANSFER IN RAT LIVER OF INTERLEUKIN 4 BUT NOT INTERLEUKIN 10 PRODUCES SEVERE ACUTE HEPATITIS

Several immune responses are either limited to or concentrated in a given organ. Cytokines produced during ongoing immune responses have organ-localized effects that can be only partially mimicked upon their systemic delivery. Recombinant adenoviruses are efficient vectors to induce transient organ-...

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Bibliographic Details
Published in:Cytokine (Philadelphia, Pa.) Pa.), 1997-11, Vol.9 (11), p.818-829
Main Authors: David, Anne, Chetritt, Jerôme, Coupel-Clauce, Hélène, Tesson, Laurent, Cassard, Armelle, Blancho, Gilles, Charreau, Béatrice, Sigalla, Jeanne, Buzelin, Françoise, Le Mauff, Brigitte, Soulillou, Jean-Paul, Anegon, Ignacio
Format: Article
Language:English
Subjects:
Acute Disease
Adenoviridae - pathogenicity
Animals
gene transfer
Gene Transfer Techniques - adverse effects
hepatitis
Hepatitis, Viral, Animal - etiology
Hepatitis, Viral, Animal - transmission
inflammation
interleukin 10
interleukin 4
Interleukin-10 - biosynthesis
Interleukin-10 - genetics
Interleukin-4 - biosynthesis
Interleukin-4 - genetics
Liver - metabolism
Liver - pathology
Liver - virology
Liver Function Tests
Male
Rats
Rats, Wistar
recombinant adenovirus
RNA, Messenger - metabolism
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Summary:Several immune responses are either limited to or concentrated in a given organ. Cytokines produced during ongoing immune responses have organ-localized effects that can be only partially mimicked upon their systemic delivery. Recombinant adenoviruses are efficient vectors to induce transient organ-localized cytokine expression. This allows in vivo analysis of the effects of cytokines produced spatially and temporally in a manner comparable to that observed during immune responses. The authors generated recombinant adenovirus for rat IL-4 (AdIL-4) and IL-10 (AdIL-10) to analyse the in vivo effects of these two important immunoregulatory molecules after gene transfer in the liver. It was first established that AdIL-4 and AdIL-10 were able to direct the production of biologically active cytokines by different rat cell types in vitro. Intraportal injection of doses of up to 10 10pfu of AdIL-10 or control non-coding recombinant adenovirus were well tolerated, and hepatic histology showed only mild alterations. Conversely, animals receiving more than 2.5×10 9pfu of AdIL-4 showed dose-dependent mortality, with clinical signs of hepatic dysfunction. Liver histology in animals receiving 2.5×10 9pfu of AdIL-4 showed severe acute hepatitis with maximal lesions between day 7 and 14 and almost complete normalization by day 28 after gene transfer. The leukocyte infiltrate was composed primarily of mononuclear cells, but eosinophils and mast cells were significantly increased as compared to control animals. Hepatic function was also altered in animals that received AdIL-4, with kinetics similar to that of histological lesions. Our study describes a model for investigating cytokine function in vivo through liver-localized transgene expression mediated by adenoviral vectors and demonstrates that liver production of IL-4 but not IL-10 results in acute severe hepatitis.
ISSN:1043-4666
1096-0023
DOI:10.1006/cyto.1997.0234