HIV-1 infection and CD4 T cell depletion in the humanized Rag2-/-γc-/- (RAG-hu) mouse model

doi:10.1186/1742-4690-3-76

Retrovirology
Volume 3

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Berges BK
Wheat WH
Palmer BE
Connick E
Akkina R

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Research

HIV-1 infection and CD4 T cell depletion in the humanized Rag2^-/-γc^-/-(RAG-hu) mouse model

Bradford K Berges¹ , William H Wheat¹ , Brent E Palmer² , Elizabeth Connick³ and Ramesh Akkina¹

¹Department of Microbiology, Immunology, and Pathology, Colorado State University, Fort Collins, CO 80523, USA

²Department of Medicine, University of Colorado Health Sciences Center, Denver, CO 80262, USA

³Division of Infectious Disease, University of Colorado Health Sciences Center, Denver, CO 80262, USA

author email corresponding author email

Retrovirology 2006, 3:76doi:10.1186/1742-4690-3-76


Published:	1 November 2006

Abstract

Background

The currently well-established humanized mouse models, namely the hu-PBL-SCID and SCID-hu systems played an important role in HIV pathogenesis studies. However, despite many notable successes, several limitations still exist. They lack multi-lineage human hematopoiesis and a functional human immune system. These models primarily reflect an acute HIV infection with rapid CD4 T cell loss thus limiting pathogenesis studies to a short-term period. The new humanized Rag2^-/-γc^-/-mouse model (RAG-hu) created by intrahepatic injection of CD34 hematopoietic stem cells sustains long-term multi-lineage human hematopoiesis and is capable of mounting immune responses. Thus, this model shows considerable promise to study long-term in vivo HIV infection and pathogenesis.

Results

Here we demonstrate that RAG-hu mice produce human cell types permissive to HIV-1 infection and that they can be productively infected by HIV-1 ex vivo. To assess the capacity of these mice to sustain long-term infection in vivo, they were infected by either X4-tropic or R5-tropic HIV-1. Viral infection was assessed by PCR, co-culture, and in situ hybridization. Our results show that both X4 and R5 viruses are capable of infecting RAG-hu mice and that viremia lasts for at least 30 weeks. Moreover, HIV-1 infection leads to CD4 T cell depletion in peripheral blood and thymus, thus mimicking key aspects of HIV-1 pathogenesis. Additionally, a chimeric HIV-1 NL4-3 virus expressing a GFP reporter, although capable of causing viremia, failed to show CD4 T cell depletion possibly due to attenuation.

Conclusion

The humanized RAG-hu mouse model, characterized by its capacity for sustained multi-lineage human hematopoiesis and immune response, can support productive HIV-1 infection. Both T cell and macrophage tropic HIV-1 strains can cause persistent infection of RAG-hu mice resulting in CD4 T cell loss. Prolonged viremia in the context of CD4 T cell depletion seen in this model mirrors the main features of HIV infection in the human. Thus, the RAG-hu mouse model of HIV-1 infection shows great promise for future in vivo pathogenesis studies, evaluation of new drug treatments, vaccines and novel gene therapy strategies.