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Role for Spi-C in the development of red pulp macrophages and splenic iron homeostasis

Authors :
Kohyama, Masako
Ise, Wataru
Edelson, Brian T.
Wilker, Peter R.
Hildner, Kai
Mejial, Carlo
Frazier, William A.
Murphy, Theresa L.
Murphy, Kenneth M.
Source :
Nature. January 15, 2009, Vol. 457 Issue 7227, p318, 4 p.
Publication Year :
2009

Abstract

Tissue macrophages comprise a heterogeneous group of cell types differing in location, surface markers and function (1). Red pulp macrophages are a distinct splenic subset involved in removing senescent red blood cells (2). Transcription factors such as PU.1 (also known as Sfpil) and C/EBPa (Cebpa) have general roles in myelomonocytic development (3,4), but the transcriptional basis for producing tissue macrophage subsets remains unknown. Here we show that Spi-C (encoded by Spic), a PU.1-related transcription factor, selectively controls the development of red pulp macrophages. Spi-C is highly expressed in red pulp macrophages, but not monocytes, dendritic cells or other tissue macrophages. [Spic.sup.-/-] mice have a cell-autonomous defect in the development of red pulp macrophages that is corrected by retroviral Spi-C expression in bone marrow cells, but have normal monocyte and other macrophage subsets. Red pulp macrophages highly express genes involved in capturing circulating haemoglobin and in iron regulation. [Spic.sup.-/-] mice show normal trapping of red blood cells in the spleen, but fail to phagocytose these red blood cells efficiently, and develop an iron overload localized selectively to splenic red pulp. Thus, Spi-C controls development of red pulp macrophages required for red blood cell recycling and iron homeostasis.<br />Spi-C belongs to the Spi subfamily of Ets transcription factors, which includes PU.1 and Spi-B (5,6), and was initially reported to be expressed in B cells (5,7). We compared expression [...]

Details

Language :
English
ISSN :
00280836
Volume :
457
Issue :
7227
Database :
Gale General OneFile
Journal :
Nature
Publication Type :
Academic Journal
Accession number :
edsgcl.192591411