Human IL-3/GM-CSF knock-in mice support human alveolar macrophage development and human immune responses in the lung
Author(s) -
Tim Willinger,
Anthony Rongvaux,
Hitoshi Takizawa,
George D. Yancopoulos,
David M. Valenzuela,
Andrew Murphy,
Wojtek Auerbach,
Elizabeth E. Ey,
Sean Stevens,
Markus G. Manz,
Richard A. Flavell
Publication year - 2011
Publication title -
proceedings of the national academy of sciences
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.011
H-Index - 771
eISSN - 1091-6490
pISSN - 0027-8424
DOI - 10.1073/pnas.1019682108
Subject(s) - immune system , immunology , humanized mouse , alveolar macrophage , biology , innate immune system , pulmonary alveolar proteinosis , granulocyte macrophage colony stimulating factor , myeloid , macrophage , lung , cytokine , medicine , in vitro , biochemistry
Mice with a functional human immune system have the potential to allow in vivo studies of human infectious diseases and to enable vaccine testing. To this end, mice need to fully support the development of human immune cells, allow infection with human pathogens, and be capable of mounting effective human immune responses. A major limitation of humanized mice is the poor development and function of human myeloid cells and the absence of human immune responses at mucosal surfaces, such as the lung. To overcome this, we generated human IL-3/GM-CSF knock-in (hIL-3/GM-CSF KI) mice. These mice faithfully expressed human GM-CSF and IL-3 and developed pulmonary alveolar proteinosis because of elimination of mouse GM-CSF. We demonstrate that hIL-3/GM-CSF KI mice engrafted with human CD34(+) hematopoietic cells had improved human myeloid cell reconstitution in the lung. In particular, hIL-3/GM-CSF KI mice supported the development of human alveolar macrophages that partially rescued the pulmonary alveolar proteinosis syndrome. Moreover, human alveolar macrophages mounted correlates of a human innate immune response against influenza virus. The hIL-3/GM-CSF KI mice represent a unique mouse model that permits the study of human mucosal immune responses to lung pathogens.
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