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自然获得性微嵌合体。

Naturally acquired microchimerism.

作者信息

Gammill Hilary S, Nelson J Lee

机构信息

Department of Clinical Research, Fred Hutchinson Cancer Research Center, University of Washington, Seattle, Washington, USA.

出版信息

Int J Dev Biol. 2010;54(2-3):531-43. doi: 10.1387/ijdb.082767hg.

DOI:10.1387/ijdb.082767hg
PMID:19924635
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2887685/
Abstract

Bi-directional transplacental trafficking occurs routinely during the course of normal pregnancy, from fetus to mother and from mother to fetus. In addition to a variety of cell-free substances, it is now well recognized that some cells are also exchanged. Microchimerism refers to a small number of cells (or DNA) harbored by one individual that originated in a genetically different individual. While microchimerism can be the result of iatrogenic interventions such as transplantation or transfusion, by far the most common source is naturally acquired microchimerism from maternal-fetal trafficking during pregnancy. Microchimerism is a subject of much current interest for a number of reasons. During pregnancy, fetal microchimerism can be sought from the mothers blood for the purpose of prenatal diagnosis. Moreover, studies of fetal microchimerism during pregnancy may offer insight into complications of pregnancy, such as preeclampsia, as well as insights into the pathogenesis of autoimmune diseases such as rheumatoid arthritis which usually ameliorates during pregnancy. Furthermore, it is now known that microchimerism persists decades later, both fetal microchimerism in women who have been pregnant and maternal microchimerism in her progeny. Investigation of the long-term consequences of fetal and maternal microchimerism is another exciting frontier of active study, with initial results pointing both to adverse and beneficial effects. This review will provide an overview of microchimerism during pregnancy and of current knowledge regarding long-term effects of naturally acquired fetal and maternal microchimerism.

摘要

在正常妊娠过程中,双向胎盘转运是常规发生的,包括从胎儿到母亲以及从母亲到胎儿。除了各种无细胞物质外,现在人们已经充分认识到一些细胞也会发生交换。微嵌合体是指一个个体中存在的少量细胞(或DNA),这些细胞起源于基因不同的另一个个体。虽然微嵌合体可能是移植或输血等医源性干预的结果,但目前最常见的来源是孕期母婴转运自然获得的微嵌合体。微嵌合体目前备受关注,原因有很多。在孕期,可以从母亲血液中寻找胎儿微嵌合体用于产前诊断。此外,孕期胎儿微嵌合体的研究可能有助于深入了解妊娠并发症,如先兆子痫,以及自身免疫性疾病如类风湿关节炎的发病机制,类风湿关节炎通常在孕期会有所缓解。此外,现在已知微嵌合体在几十年后仍会持续存在,包括曾怀孕女性体内的胎儿微嵌合体以及其后代体内的母体微嵌合体。对胎儿和母体微嵌合体长期影响的研究是另一个活跃的研究前沿领域,初步结果显示既有不利影响也有有益影响。本综述将概述孕期微嵌合体以及目前关于自然获得的胎儿和母体微嵌合体长期影响的知识。

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Can the Supplementation of Oocytes with Extra Copies of mtDNA Impact Development Without Being Transmitted? A Molecular Account.向卵母细胞补充额外拷贝的线粒体DNA(mtDNA)能否在不发生遗传的情况下影响发育?分子层面的解释。
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本文引用的文献

1
Survival after T cell-depleted haploidentical stem cell transplantation is improved using the mother as donor.使用母亲作为供体可提高T细胞去除的单倍体同基因干细胞移植后的生存率。
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Heredity--venturing beyond genetics.遗传——超越遗传学的探索。
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Chimerism occurs in thyroid, lung, skin and lymph nodes of women with sons.怀有儿子的女性的甲状腺、肺、皮肤和淋巴结中会出现嵌合体现象。
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Maternal immune activation does not affect maternal microchimeric cells.母体免疫激活不会影响母体微嵌合细胞。
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Pregnancy induced displacement of preexisting microchimeric cells in the absence of maternal B and T cells.妊娠诱导母体内已存在的微嵌合细胞迁移,而不依赖于母体内的 B 和 T 细胞。
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Deciphering the Role of Maternal Microchimerism in Offspring Autoimmunity: A Narrative Review.解析母源性微小嵌合体在子代自身免疫中的作用:叙述性综述。
Medicina (Kaunas). 2024 Sep 5;60(9):1457. doi: 10.3390/medicina60091457.
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Presence of fetal microchimerisms in the heart and effect on cardiac repair.胎儿微嵌合体在心脏中的存在及其对心脏修复的影响。
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Fetal microchimerism, pregnancy epiphenomenon or kinship indicator?胎儿微嵌合体:妊娠附带现象还是亲属关系指标?
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Characterization of fetal microchimeric immune cells in mouse maternal hearts during physiologic and pathologic pregnancies.生理和病理妊娠期间小鼠母体心脏中胎儿微嵌合免疫细胞的特征分析。
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Genetics of Sex Differences in Immunity.免疫性别差异的遗传学基础。
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Murine maternal cell microchimerism: analysis using real-time PCR and in vivo imaging.小鼠母体细胞微嵌合体:利用实时聚合酶链反应和体内成像技术进行分析
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