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PubMed articles by:
Pomier, C.
Alcaraz, M.
Debacq, C.
Mortreux, F.
Retrovirology. 2009; 6: 30.
Published online 2009 April 3. doi: 10.1186/1742-4690-6-30.
PMCID: PMC2670259
Copyright © 2009 Pomier et al; licensee BioMed Central Ltd.
A dose-effect relationship for deltaretrovirus-dependent leukemogenesis in sheep
Carole Pomier,1 Maria Teresa Sanchez Alcaraz,2 Christophe Debacq,2 Agnes Lançon,1 Pierre Kerkhofs,4 Lucas Willems,2 Eric Wattel,#1,3 and Franck Mortreuxcorresponding author#1
1CNRS FRE-3011 - Université Lyon I, Oncovirologie et Biothérapies, Centre Léon Bérard, Lyon, France
2FUSAGx, Molecular and cellular biology, Gembloux, Belgium
3Hôpital Edouard Herriot, Service d'Hématologie, Pavillon E, Lyon, France
4Veterinary and Agrochemical Research Centre, Department of Virology, Uccle, Belgium
corresponding authorCorresponding author.
#Contributed equally.
Carole Pomier: ptepoms/at/yahoo.fr; Maria Teresa Sanchez Alcaraz: mteresasanchez/at/hotmail.com; Christophe Debacq: christophe.j.debacq/at/gskbio.com; Agnes Lançon: lancon/at/lyon.fnclcc.fr; Pierre Kerkhofs: piker/at/var.fgov.be; Lucas Willems: willems.l/at/fsagx.ac.be; Eric Wattel: wattel/at/lyon.fnclcc.fr; Franck Mortreux: mortreux/at/lyon.fnclcc.fr
Received November 12, 2008; Accepted April 3, 2009.
This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
 
Abstract
Background
Retrovirus-induced tumors develop in a broad range of frequencies and after extremely variable periods of time, from only a few days to several decades, depending mainly on virus type. For hitherto unexplained reasons, deltaretroviruses cause hematological malignancies only in a minority of naturally infected organisms and after a very prolonged period of clinical latency.
Results
Here we demonstrate that the development of malignancies in sheep experimentally infected with the deltaretrovirus bovine leukemia virus (BLV) depends only on the level of BLV replication. Animals were experimentally infected with leukemogenic or attenuated, but infectious, BLV molecular clones and monitored prospectively through 8 months for viral replication. As early as 2 weeks after infection and subsequently at any time during follow-up, leukemogenic viruses produced significantly higher absolute levels of reverse transcription (RT), clonal expansion of infected cells, and circulating proviruses with RT- and somatic-dependent mutations than attenuated viruses. These differences were only quantitative, and both kinds of viruses triggered parallel temporal fluctuations of host lymphoid cells, viral loads, infected cell clonality and proliferation.
Conclusion
Deltaretrovirus-associated leukemogenesis in sheep appears to be a two-hit process over time depending on the amounts of first horizontally and then vertically expanded viruses.
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