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Publication : Expression and regulation of chemokine genes in the mouse uterus during pregnancy.

First Author  Wood GW Year  1999
Journal  Cytokine Volume  11
Issue  12 Pages  1038-45
PubMed ID  10623429 Mgi Jnum  J:60131
Mgi Id  MGI:1352797 Doi  10.1006/cyto.1999.0513
Citation  Wood GW, et al. (1999) Expression and regulation of chemokine genes in the mouse uterus during pregnancy. Cytokine 11(12):1038-45
abstractText  Leukocytes accumulate in the pregnant mouse uterus following mating, during implantation and during placental development. Changes in leukocyte number are primarily due to recruitment from the blood, not local proliferation, but the underlying recruitment mechanisms are poorly understood. Mating-induced granulocyte and macrophage recruitment is due in part to pro-inflammatory and chemotactic factors present in seminal plasma. Accumulation of macrophages later in pregnancy appears to be caused in part by ovarian hormone-stimulated CSF-1 production and in part by other as yet unidentified uterine chemotactic factors. The current study was performed to assess chemokine production in the uterus during pregnancy. Northern blotting was used to demonstrate NSI/KC (KC), macrophage chemotactic protein-1 (MCP-1), macrophage inflammatory protein one alpha (MIP1alpha) and regulated inactivation, normal T expressed and secreted protein (RANTES) mRNA in the uterus. Oestrogen and progesterone induced intrauterine production of all four chemokines and may have done so through the autocrine/paracrine activities of IL-1. The data suggest that C-C chemokines play a role in accumulation of macrophages in the uterus during pregnancy. Copyright 1999 Academic Press.
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