Access

Letters to Nature

Nature 432, 1040-1045 (23 December 2004) | doi:10.1038/nature03068; Received 23 August 2004; Accepted 25 September 2004

Retinoblastoma promotes definitive erythropoiesis by repressing Id2 in fetal liver macrophages

Antonio Iavarone2,3, Emerson R. King, Xu-Ming Dai6, Gustavo Leone5, E. Richard Stanley6 & Anna Lasorella2,4

  1. Institute for Cancer Genetics, Department of Pathology, College of Physicians and Surgeons of Columbia University, New York, New York 10032, USA
  2. Institute for Cancer Genetics, Department of Neurology, College of Physicians and Surgeons of Columbia University, New York, New York 10032, USA
  3. Institute for Cancer Genetics, Department of Pediatrics, College of Physicians and Surgeons of Columbia University, New York, New York 10032, USA
  4. Human Cancer Genetics Program, Department of Molecular Virology, Immunology and Medical Genetics, The Ohio State University, Columbus, Ohio 43210, USA
  5. Department of Developmental and Molecular Biology, Albert Einstein College of Medicine, Bronx, New York 10461, USA

Correspondence to: Antonio Iavarone2,3 Email: ai2102@columbia.edu

Top

In mammals, the fetal liver is the first site of definitive erythropoiesis—the generation of mature, enucleated red cells. The functional unit for definitive erythropoiesis is the erythroblastic island, a multicellular structure composed of a central macrophage surrounded by erythroblasts at various stages of differentiation1, 2. Targeted disruption of the retinoblastoma (Rb) tumour suppressor gene in the mouse leads to embryonic death caused by failure of erythroblasts to enucleate3, 4, 5. The erythroid defect has been attributed to loss of Rb in cells that support erythropoiesis, but the identity of these cells is unknown6. Here we show that Rb-deficient embryos carry profound abnormalities of fetal liver macrophages that prevent physical interactions with erythroblasts. In contrast, wild-type macrophages bind Rb-deficient erythroblasts and lead them to terminal differentiation and enucleation. Loss of Id2, a helix–loop–helix protein that mediates the lethality of Rb-deficient embryos7, rescues the defects of Rb-deficient fetal liver macrophages. Rb promotes differentiation of macrophages by opposing the inhibitory functions of Id2 on the transcription factor PU.1, a master regulator of macrophage differentiation. Thus, Rb has a cell autonomous function in fetal liver macrophages, and restrains Id2 in these cells in order to implement definitive erythropoiesis.

MORE ARTICLES LIKE THIS

These links to content published by NPG are automatically generated.

NEWS AND VIEWS

Developmental biology No red cell is an island

Nature News and Views (23 Dec 2004)

RESEARCH

Interaction of tau protein with the dynactin complex

The EMBO Journal Article (31 Oct 2007)

The Rb tumor suppressor is required for stress erythropoiesis

The EMBO Journal Article (27 Oct 2004)

See all 9 matches for Research