Induced-Pluripotent-Stem-Cell-Derived Primitive Macrophages Provide a Platform for Modeling Tissue-Resident Macrophage Differentiation and Function
Date
2017Author
See, Peter
Zhang, Jinqiu
Goh, Chi Ching
Gül, Ahmet
Hubert, Sandra
Lee, Bernett
Chen, Jinmiao
Huber, Tara
Ashihara, Eishi
Garel, Sonia
Pouladi, Mahmoud A.
Ginhoux, Florent
Low, Ivy
Shadan, Nurhidaya Binte
Lum, Josephine
Wei, Tay Seok
Mok, Esther
Kawanishi, Shohei
Kitamura, Yoshihisa
Larbi, Anis
Poidinger, Michael
Renia, Laurent
Ng, Lai Guan
Wolf, Yochai
Jung, Steffen
Onder, Tamer
Newell, Evan
Takata, Kazuyuki
Kozaki, Tatsuya
Lee, Christopher Zhe Wei
Thion, Morgane Sonia
Otsuka, Masayuki
Lim, Shawn
Utami, Kagistia Hana
Fidan, Kerem
Park, Dong Shin
Malleret, Benoit
Chakarov, Svetoslav
Low, Donovan
Low, Gillian
Garcia-Miralles, Marta
Zeng, Ruizhu
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Show full item recordAbstract
Tissue macrophages arise during embryogenesis from yolk-sac (YS) progenitors that give rise to primitive YS macrophages. Until recently, it has been impossible to isolate or derive sufficient numbers of YS-derived macrophages for further study, but data now suggest that induced pluripotent stem cells (iPSCs) can be driven to undergo a process reminiscent of YS-hematopoiesis in vitro. We asked whether iPSC-derived primitive macrophages (iMacs) can terminally differentiate into specialized macrophages with the help of growth factors and organ-specific cues. Co-culturing human or murine iMacs with iPSC-derived neurons promoted differentiation into microglia-like cells in vitro. Furthermore, murine iMacs differentiated in vivo into microglia after injection into the brain and into functional alveolar macrophages after engraftment in the lung. Finally, iPSCs from a patient with familial Mediterranean fever differentiated into iMacs with pro-inflammatory characteristics, mimicking the disease phenotype. Altogether, iMacs constitute a source of tissue-resident macrophage precursors that can be used for biological, pathophysiological, and therapeutic studies.
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