Successful treatment of canine leukocyte adhesion deficiency by foamy virus vectors
Author: ["Thomas R Bauer Jr","James M Allen","Mehreen Hai","Laura M Tuschong","Iram F Khan","Erik M Olson","Rima L Adler","Tanya H Burkholder","Yu-chen Gu","David W Russell","Dennis D Hickstein"]
Publication: Nature Medicine
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Abstract
Recent successes in treating genetic immunodeficiencies have demonstrated the therapeutic potential of stem cell gene therapy1,2,3,4. However, the use of gammaretroviral vectors in these trials led to insertional activation of nearby oncogenes and leukemias in some study subjects, prompting studies of modified or alternative vector systems5. Here we describe the use of foamy virus vectors to treat canine leukocyte adhesion deficiency (CLAD). Four of five dogs with CLAD that received nonmyeloablative conditioning and infusion of autologous, CD34+ hematopoietic stem cells transduced by a foamy virus vector expressing canine CD18 had complete reversal of the CLAD phenotype, which was sustained more than 2 years after infusion. In vitro assays showed correction of the lymphocyte proliferation and neutrophil adhesion defects that characterize CLAD. There were no genotoxic complications, and integration site analysis showed polyclonality of transduced cells and a decreased risk of integration near oncogenes as compared to gammaretroviral vectors. These results represent the first successful use of a foamy virus vector to treat a genetic disease, to our knowledge, and suggest that foamy virus vectors will be effective in treating human hematopoietic diseases.
Cite this article
Bauer, T., Allen, J., Hai, M. et al. Successful treatment of canine leukocyte adhesion deficiency by foamy virus vectors. Nat Med 14, 93–97 (2008). https://doi.org/10.1038/nm1695
