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Production by Human Uterine Macrophages Up-Regulates Uterine Epithelial Cell Expression of Human
-Defensin 21


* Department of Physiology and
Department of Immunology and Microbiology, Dartmouth Medical School, Lebanon, NH 03756
The uterine endometrium coordinates a wide spectrum of physiologic and immunologic functions, including endometrial receptivity and implantation as well as defense against sexually transmitted pathogens. Macrophages and epithelial cells cooperatively mediate innate host defense against bacterial invasion through the generation of immunologic effectors, including cytokines and antimicrobial peptides. In this study, we demonstrate that stimulation of peripheral blood monocytes and uterine macrophages with bacterial LPS induces the production of biologically active proinflammatory IL-1
. High doses of estradiol enhance LPS-induced IL-1
expression in an estrogen receptor-dependent manner. Furthermore, both peripheral blood monocyte- and uterine macrophage-derived IL-1
induce secretion of antimicrobial human
-defensin 2 by uterine epithelial cells. These data indicate dynamic immunologic interaction between uterine macrophages and epithelial cells and implicate a role for estradiol in the modulation of the immune response.
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