A review of trafficking and activation of uterine natural killer cells
MJ van den Heuvel, X Xie, C Tayade… - American journal of …, 2005 - Wiley Online Library
MJ van den Heuvel, X Xie, C Tayade, C Peralta, Y Fang, S Leonard, VA Paffaro Jr…
American journal of reproductive immunology, 2005•Wiley Online LibraryProblem Enrichment of uterine natural killer (uNK) cells occurs during pregnancy in many
species. However, functions of uNK cells and regulation of their uterine homing are not fully
defined. In mice and women, uNK cells contribute to angiogenesis, a role reviewed here and
now addressed in a mammal with an alternative placental type. Methods of study To address
lymphocyte functions, RNA from murine or porcine endometrium and lymphocytes purified
from endometrium were analyzed using real‐time or reverse transcription PCR. To address …
species. However, functions of uNK cells and regulation of their uterine homing are not fully
defined. In mice and women, uNK cells contribute to angiogenesis, a role reviewed here and
now addressed in a mammal with an alternative placental type. Methods of study To address
lymphocyte functions, RNA from murine or porcine endometrium and lymphocytes purified
from endometrium were analyzed using real‐time or reverse transcription PCR. To address …
Problem
Enrichment of uterine natural killer (uNK) cells occurs during pregnancy in many species. However, functions of uNK cells and regulation of their uterine homing are not fully defined. In mice and women, uNK cells contribute to angiogenesis, a role reviewed here and now addressed in a mammal with an alternative placental type.
Methods of study
To address lymphocyte functions, RNA from murine or porcine endometrium and lymphocytes purified from endometrium were analyzed using real‐time or reverse transcription PCR. To address homing potential, human blood CD56+ lymphocytes were evaluated using both RNA and functional adhesion to endothelium presented under shear force in frozen sections of gestation day 7 C57Bl/6J implantation sites. Women were serially sampled over a menstrual cycle or a clinical preparatory cycle for embryo transfer.
Results
Activation of murine uNK cells is associated with much greater increases in transcription for Eomes than for T‐bet (Tbx21). Lymphocytes from normal porcine implantation sites transcribe vascular endothelial growth factor, placental growth factor, interferon‐gamma and hypoxia‐inducible factor (HIF)‐1α. In fertile women, increases in L‐selectin‐ and α4‐integrin‐mediated interactions between CD56+ cells and endothelium occur at luteinizing hormone (LH) surge (cycling women) to oocyte pick up or embryo transfer, then return to pre‐LH levels.
Conclusions
Uterine lymphocytes may universally promote pregnancy‐associated endometrial angiogenesis. Recruitment of uNK precursor cells from blood appears to occur in a window promoted by rising plasma estrogen and LH and limited by rising progesterone.
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