4.6 Article

IL-2 receptor γ-chain molecule is critical for intestinal T-cell reconstitution in humanized mice

Journal

MUCOSAL IMMUNOLOGY
Volume 5, Issue 5, Pages 555-566

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/mi.2012.31

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Funding

  1. National Institutes of Health [AI073146, AI071940, AI082608, AI082637, AI081613, 5T32AI005284]
  2. UNC Center for AIDS Research Grant [P30 AI50410]
  3. Research Fellowship of the Japan Society for the Promotion of Science (T.N.)

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Intestinal immune cells are important in host defense, yet the determinants for human lymphoid homeostasis in the intestines are poorly understood. In contrast, lymphoid homeostasis has been studied extensively in mice, where the requirement for a functional common gamma-chain molecule has been established. We hypothesized that humanized mice could offer insights into human intestinal lymphoid homeostasis if generated in a strain with an intact mouse common gamma-chain molecule. To address this hypothesis, we used three mouse strains (non-obese diabetic (NOD)/severe-combined immunodeficient (SCID) (N/S); NOD/SCID gamma-chain(-/-) (NSG); and Rag2(-/-) gamma-chain(-/-) (DKO)) and two humanization techniques (bone marrow liver thymus (BLT) and human CD34(+) cell bone marrow transplant of newborn mice (hu)) to generate four common types of humanized mice: N/S-BLT, NSG-BLT, NSG-hu, and DKO-hu mice. The highest levels of intestinal human T cells throughout the small and large intestines were observed in N/S-BLT mice, which have an intact common gamma-chain molecule. Furthermore, the small intestine lamina propria T-cell populations of N/S-BLT mice exhibit a human intestine-specific surface phenotype. Thus, the extensive intestinal immune reconstitution of N/S-BLT mice was both quantitatively and qualitatively better when compared with the other models tested such that N/S-BLT mice are well suited for the analysis of human intestinal lymphocyte trafficking and human-specific diseases affecting the intestines.

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