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首页> 外文期刊>Archivum Immunologiae et Therapiae Experimentalis >Fetal-cell microchimerism, lymphopoiesis, and autoimmunity
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Fetal-cell microchimerism, lymphopoiesis, and autoimmunity

机译:胎儿细胞微嵌合体,淋巴细胞生成和自身免疫

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During all human and murine pregnancies, fetal cells enter the maternal circulation and tissues and may persist there for decades. The immune consequences of this phenomenon have been explored for many years as a potential origin of autoimmunity or protection from cancer in women after pregnancy. The leading hypothesis, suggesting that semi-allogenic fetal T cells may trigger a graft-versus-host type of disease, has been supported by several studies showing an increased frequency of fetal-cell microchimerism (FMc) in women affected with systemic sclerosis. However, a large proportion of healthy women or women affected with non-immune disorders also display fetal T cells, challenging the direct pathogenic role of such cells. In addition, recent evidence showing the transfer of various fetal progenitor cells to the mother during gestation has shed new light on the interpretation of microchimerism in autoimmunity. This review discusses the functional capacity of fetal hematopoietic progenitors to form T and B cells in maternal hematopoietic tissues, where they undergo an educational process probably resulting in tolerance to maternal antigens. Therefore, hypotheses other than the transfer of fetal cells to the mother’s circulation should be considered in explaining the observed association of FMc and autoimmune disorders. Keywords microchimerism - pregnancy - fetal T cells - lymphopoiesis - auto-immunity - stem cells
机译:在所有人类和鼠类怀孕期间,胎儿细胞都会进入母体循环和组织,并可能在那里持续数十年。多年以来,这种现象的免疫后果已被研究为孕妇自身免疫或预防癌症的潜在来源。领先的假设表明半同种异体的胎儿T细胞可能引发移植物抗宿主类型的疾病,这项研究得到了几项研究的支持,这些研究表明,患有系统性硬化症的女性​​胎儿细胞微嵌合体(FMc)的发生频率增加。但是,很大一部分健康的妇女或患有非免疫性疾病的妇女也显示出胎儿T细胞,从而挑战了这种细胞的直接致病作用。另外,最近的证据显示,在妊娠期间各种胎儿祖细胞向母亲的转移,为自身免疫中微嵌合体的解释提供了新的思路。这篇综述讨论了胎儿造血祖细胞在母体造血组织中形成T细胞和B细胞的功能能力,在那里他们经历了可能导致对母体抗原耐受的教育过程。因此,在解释观察到的FMc与自身免疫性疾病的关联时,应考虑除了将胎儿细胞转移到母亲的循环之外的其他假设。关键词微嵌合体-妊娠-胎儿T细胞-淋巴细胞生成-自身免疫-干细胞

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