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首页> 外文期刊>Biology of Reproduction: Offical Journal of the Society for the Study of Reproduction >Seminal fluid drives expansion of the CD4+CD25+ T regulatory cell pool and induces tolerance to paternal alloantigens in mice.
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Seminal fluid drives expansion of the CD4+CD25+ T regulatory cell pool and induces tolerance to paternal alloantigens in mice.

机译:精液驱动CD4 + CD25 + T调节性细胞池的扩增,并诱导对小鼠父系同种异体抗原的耐受性。

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摘要

T regulatory (Treg) cells are implicated in maternal immune tolerance of the conceptus at implantation; however, the antigenic and regulatory signals controlling Treg cells in early pregnancy are undefined. To examine the role of male seminal fluid in tolerance induction, the effect of exposure to seminal fluid at mating on responsiveness to paternal alloantigens was examined using paternal tumor cell grafts and by delayed-type hypersensitivity (DTH) challenge on Day 3.5 postcoitum. Exposure to seminal fluid inhibited rejection of paternal tumor cells, independently of fertilization and embryo development, while seminal fluid from major histocompatability complex (MHC)-dissimilar males was less effective. Similarly, mating with intact males suppressed the DTH response to paternal alloantigens in an MHC-specific fashion. Excision of the seminal vesicle glands diminished the tolerance-inducing activity of seminal fluid. Mating with intact males caused an increase in CD4(+)CD25(+) cells expressing FOXP3 in the para-aortic lymph nodes draining the uterus, beyond the estrus-associated peak in cycling mice. The increase in CD4(+)CD25(+) cells was abrogated when males were vasectomized or seminal vesicles were excised. Collectively, these data provide evidence that exposure to seminal fluid at mating promotes a state of functional tolerance to paternal alloantigens that may facilitate maternal acceptance of the conceptus at implantation, and the effects of seminal fluid are likely to be mediated by expansion of the Treg cell pool. Both seminal plasma and sperm components of the seminal fluid are necessary to confer full tolerance and elicit the Treg cell response, potentially through provision of immune-deviating cytokines and antigens, respectively.
机译:T调节(Treg)细胞与植入时母体的母体免疫耐受有关。然而,怀孕初期控制Treg细胞的抗原和调节信号尚不确定。为了检查雄性精液在耐受性诱导中的作用,使用父系肿瘤细胞移植物和在交配后第3.5天通过延迟型超敏性(DTH)攻击,检查了交配时暴露于精液对父系同种异体抗原反应性的影响。暴露于精液会抑制父系肿瘤细胞的排斥,这与受精和胚胎发育无关,而来自主要组织相容性复合体(MHC)不同的雄性的精液效果较差。同样,与完整的雄性交配会以MHC特异性方式抑制DTH对父系同种异体抗原的反应。精囊腺的切除减少了精液的耐受性诱导活性。与完整的雄性交配导致主动脉旁淋巴结中引流子宫的CD4(+)CD25(+)细胞表达FOXP3增加,超过循环小鼠中与发情相关的峰值。当男性被切除或切除精囊时,CD4(+)CD25(+)细胞的增加被取消。总体而言,这些数据提供了证据,即交配时暴露于精液会促进对父系同种异体抗原的功能耐受状态,这可能有助于母体在植入时接受概念,并且精液的作用很可能是由Treg细胞的膨胀介导的。池。精液的精浆成分和精子成分都是赋予完全耐受力和引发Treg细胞反应所必需的,可能分别通过提供免疫减轻性细胞因子和抗原来实现。

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