首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Prediction of reactivity to noninherited maternal antigen in MHC-mismatched, minor histocompatibility antigen-matched stem cell transplantation in a mouse model.
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Prediction of reactivity to noninherited maternal antigen in MHC-mismatched, minor histocompatibility antigen-matched stem cell transplantation in a mouse model.

机译:预测小鼠模型中MHC不匹配,次要组织相容性抗原匹配的干细胞移植对未遗传的母体抗原的反应性。

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摘要

The immunologic effects of developmental exposure to noninherited maternal Ags (NIMAs) are quite variable. Both tolerizing influence and inducing alloreaction have been observed on clinical transplantation. The role of minor histocompatibility Ags (MiHAs) in NIMA effects is unknown. MiHA is either matched or mismatched in NIMA-mismatched transplantation because a donor of the transplantation is usually limited to a family member. To exclude the participation of MiHA in a NIMA effect for MHC (H-2) is clinically relevant because mismatched MiHA may induce severe alloreaction. The aim of this study is to understand the mechanism of NIMA effects in MHC-mismatched, MiHA-matched hematopoietic stem cell transplantation. Although all offsprings are exposed to the maternal Ags, the NIMA effect for the H-2 Ag was not evident. However, they exhibit two distinct reactivities, low and high responder, to NIMA in utero and during nursing depending on the degree of maternal microchimerism. Low responders survived longer with less graft-versus-host disease. These reactivities were correlated with Foxp3 expression of peripheral blood CD4(+)CD25(+) cells after graft-versus-host disease induction and the number of IFN-gamma-producing cells stimulated with NIMA pretransplantation. These observations are clinically relevant and suggest that it is possible to predict the immunological tolerance to NIMA.
机译:发育性暴露于非遗传性母体Ag(NIMAs)的免疫学作用变化很大。在临床移植中已经观察到耐受影响和诱导同种反应。次要组织相容性Ags(MiHAs)在NIMA效应中的作用尚不清楚。在NIMA不匹配的移植中,MiHA是匹配的还是不匹配的,因为移植的供体通常仅限于家庭成员。排除MiHA参与MHC(H-2)的NIMA效应在临床上具有相关性,因为不匹配的MiHA可能引起严重的同种反应。这项研究的目的是了解NIMA在MHC不匹配,MiHA匹配的造血干细胞移植中的作用机制。尽管所有后代都暴露于母体Ags中,但HMA-2对NIMA的影响并不明显。然而,根据母体微嵌合体的程度,它们对子宫内和哺乳期的NIMA表现出两种不同的反应性,即低反应性和高反应性。低反应者存活时间更长,移植物抗宿主病更少。这些反应性与移植物抗宿主病诱导后外周血CD4(+)CD25(+)细胞的Foxp3表达以及NIMA移植前刺激的产生IFN-γ的细胞数量有关。这些观察结果在临床上是相关的,并暗示有可能预测对NIMA的免疫耐受性。

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