Acetylcholine contributes to control the physiological inflammatory response during the peri-implantation period

被引:8
|
作者
Paparini, D. [1 ]
Gori, S. [2 ]
Grasso, E. [1 ]
Scordo, W. [3 ]
Calo, G. [1 ]
Perez Leiros, C. [1 ]
Ramhorst, R. [1 ]
Salamone, G. [2 ]
机构
[1] Univ Buenos Aires, Fac Ciencias Exactas & Nat, Dept Quim Biol, IQUIBICEN CONICET, Buenos Aires, DF, Argentina
[2] Acad Nacl Med Buenos Aires, Inst Med Expt IMEX CONICET, Buenos Aires, DF, Argentina
[3] Hosp Italiano Buenos Aires, Serv Med Transfus, Buenos Aires, DF, Argentina
关键词
dendritic cells; monocytes; non-neuronal acetylcholine; trophoblast cells; NONNEURONAL CHOLINERGIC SYSTEM; TROPHOBLAST CELLS; RECEPTOR SUBTYPES; TOLERANCE; PREGNANCY; MACROPHAGES; ACTIVATION; POLARIZATION; IMPLANTATION; PLASTICITY;
D O I
10.1111/apha.12494
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
BackgroundMaternal antigen-presenting cells attracted to the pregnant uterus interact with trophoblast cells and modulate their functional profile to favour immunosuppressant responses. Non-neuronal cholinergic system is expressed in human cytotrophoblast cells and in immune cells with homeostatic regulatory functions. AimThe aim of this work was to evaluate whether non-neuronal acetylcholine conditions maternal monocyte and DC migration and activation profiles. MethodsWe used an in vitro model resembling maternal-placental interface represented by the co-culture of human trophoblast cells (Swan-71 cell line) and monocytes or DC. ResultsWhen cytotrophoblast cells were treated with neostigmine (Neo) to concentrate endogenous acetylcholine levels, monocyte migration was increased. In parallel, high levels of IL-10 and decreased levels of TNF- were observed upon interaction of maternal monocytes with trophoblast cells. This effect was synergized by Neo and was prevented by atropine, a muscarinic acetylcholine receptor antagonist. Similarly, trophoblast cells increased the migration of DC independently of Neo treatment; however, enhanced IL-10 and MCP-1 synthesis in trophoblast-DC co-cultures with no changes in TNF- and IL-6 was observed. In fact, there were no changes in HLA-DR, CD86 or CD83 expression. Finally, trophoblast cells treated with Neo increased the expression of two antigen-presenting cells attracting chemokines, MCP-1, MIP-1 and RANTES through muscarinic receptors, and it was prevented by atropine. ConclusionsOur present results support a novel role of acetylcholine synthesized by trophoblast cells to modulate antigen-presenting cell migration and activation favouring an immunosuppressant profile that contributes to immune homeostasis maintenance at the maternal-foetal interface.
引用
收藏
页码:237 / 247
页数:11
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