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Microchimerism of maternal origin persists into adult life.

机译:母源性的微嵌合体持续到成年期。

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摘要

Recent studies indicate that fetal cells persist in maternal blood for decades after pregnancy. Maternal cells are known to engraft and persist in infants with immunodeficiency, but whether maternal cells persist long-term in immunocompetent offspring has not specifically been investigated. We developed sensitive human leukocyte antigen-specific (HLA-specific) PCR assays and targeted nonshared maternal HLA genes to test for persistent maternal microchimerism in subjects with scleroderma and in healthy normal subjects. Nonshared maternal-specific DNA was found in 6 of 9 scleroderma patients. In situ hybridization with double labeling for X and Y chromosome-specific sequences revealed female cells in peripheral blood samples from 2 male scleroderma patients. HLA-specific PCR also frequently revealed persistent maternal microchimerism in healthy control subjects. The mean age of all subjects with maternal microchimerism was 28 years (range: 9-49 years). With few exceptions, mothers of subjects with persistent maternal microchimerism were HLA incompatible with subjects for class I and class II alleles. These results clearly indicate that HLA-disparate maternal cells can persist in immunocompetent offspring well into adult life. The biological significance of maternal microchimerism and whether it might contribute to autoimmune disease requires further investigation.
机译:最近的研究表明,胎儿细胞在怀孕后会持续存在于母体血液中数十年。已知母体细胞在免疫缺陷婴儿中植入并持续存在,但母体细胞是否在免疫功能正常的后代中长期存在尚未得到具体研究。我们开发了灵敏的人类白细胞抗原特异性(HLA特异性)PCR检测和靶向非共享母体HLA基因,以检测硬皮病受试者和健康正常受试者的持续母体微嵌合体。在 9 例硬皮病患者中,有 6 例发现了非共享的母体特异性 DNA。X和Y染色体特异性序列的双标记原位杂交揭示了2名男性硬皮病患者外周血样本中的雌性细胞。HLA特异性PCR也经常显示健康对照受试者中持续的母体微嵌合体。所有患有母体微嵌合体的受试者的平均年龄为 28 岁(范围:9-49 岁)。除了少数例外,具有持续母体微嵌合体的受试者的母亲与I类和II类等位基因的受试者HLA不相容。这些结果清楚地表明,HLA不同的母体细胞可以在免疫功能正常的后代中持续存在到成年。母体微嵌合体的生物学意义以及它是否可能导致自身免疫性疾病需要进一步研究。

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