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Tissue distribution of erythropoietin and erythropoietin receptor in the developing human fetus.

作者信息

Juul S E, Yachnis A T, Christensen R D

机构信息

Department of Pediatrics, University of Florida College of Medicine, JHMHC, Gainesville 32610-0296, USA.

出版信息

Early Hum Dev. 1998 Oct;52(3):235-49. doi: 10.1016/s0378-3782(98)00030-9.

DOI:10.1016/s0378-3782(98)00030-9
PMID:9808074
Abstract

OBJECTIVE

Erythropoietin receptors (Epo-R) have been demonstrated on several nonhematopoietic cell types in animal models and in cell culture. Our objective was to determine the tissue distribution and cellular specificity of erythropoietin (Epo) and its receptor in the developing human fetus.

STUDY DESIGN

The expression of Epo and Epo-R mRNA was ascertained by RT-PCR for organs ranging in maturity from 5 to 24 weeks postconception. The cellular location of protein immunoreactivity was then determined using specific antiEpo and antiEpo-R antibodies. Antibody specificity was established by Western analysis.

RESULTS

mRNA for Epo and Epo-R was found in all organs in the first two trimesters. Immunolocalization of Epo was limited to the liver parenchymal cells, kidney interstitial cells and proximal tubules, neural retina of the eye, and adrenal cortex. As development progressed, immunoreactivity in the kidney became more prominent. In contrast, immunoreactivity for Epo-R was widespread throughout the body, in cell types including endothelial cells, myocardiocytes, macrophages, retinal cells, cells of the adrenal cortex and medulla, as well as in small bowel, spleen, liver, kidney, and lung.

CONCLUSIONS

The distribution of Epo and its receptor is more widespread in the developing human than was initially postulated. Epo-R is expressed on many cell types during early fetal development, leading us to speculate that Epo acts in concert with somatic growth and development factors during this period. Further investigation is required to understand the nonhematopoietic role of Epo during human development.

摘要

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