Literature DB >> 16969370

Maternal microchimerism in healthy adults in lymphocytes, monocyte/macrophages and NK cells.

Laurence S Loubière1, Nathalie C Lambert, Laura J Flinn, Timothy D Erickson, Zhen Yan, Katherine A Guthrie, Kathy T Vickers, J Lee Nelson.   

Abstract

During pregnancy some maternal cells reach the fetal circulation. Microchimerism (Mc) refers to low levels of genetically disparate cells or DNA. Maternal Mc has recently been found in the peripheral blood of healthy adults. We asked whether healthy women have maternal Mc in T and B lymphocytes, monocyte/macrophages and NK cells and, if so, at what levels. Cellular subsets were isolated after fluorescence activated cell sorting. A panel of HLA-specific real-time quantitative PCR assays was employed targeting maternal-specific HLA sequences. Maternal Mc was expressed as the genome equivalent (gEq) number of microchimeric cells per 100,000 proband cells. Thirty-one healthy adult women probands were studied. Overall 39% (12/31) of probands had maternal Mc in at least one cellular subset. Maternal Mc was found in T lymphocytes in 25% (7/28) and B lymphocytes in 14% (3/21) of probands. Maternal Mc levels ranged from 0.9 to 25.6 and 0.9 to 25.3 gEq/100,000 in T and B lymphocytes, respectively. Monocyte/macrophages had maternal Mc in 16% (4/25) and NK cells in 28% (5/18) of probands with levels from 0.3 to 36 and 1.8 to 3.2 gEq/100,000, respectively. When compared to fetal Mc, as assessed by quantification of male DNA in women with sons, maternal Mc was substantially less prevalent in all cellular subsets; fetal Mc prevalence in T and B lymphocytes, monocyte/macrophages and NK cells was 58, 75, 50 and 62% (P=0.01, P=0.005, P=0.04, P=0.05) respectively. In summary, maternal Mc was identified among lymphoid and myeloid compartments of peripheral blood in healthy adult women. Maternal Mc was less frequent than fetal Mc in all cellular subsets tested. Studies are needed to investigate the immunological effects and function of maternal Mc and to explore whether maternal Mc in cellular subsets has biological effects on her progeny.

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Year:  2006        PMID: 16969370     DOI: 10.1038/labinvest.3700471

Source DB:  PubMed          Journal:  Lab Invest        ISSN: 0023-6837            Impact factor:   5.662


  58 in total

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Authors:  Lucie Leveque; Kiarash Khosrotehrani
Journal:  Chimerism       Date:  2011-07-01

2.  Effect of parity on fetal and maternal microchimerism: interaction of grafts within a host?

Authors:  Hilary S Gammill; Katherine A Guthrie; Tessa M Aydelotte; Kristina M Adams Waldorf; J Lee Nelson
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3.  Microchimerism and regulation in living related kidney transplant families.

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4.  Maternal microchimerism is prevalent in cord blood in memory T cells and other cell subsets, and persists post-transplant.

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5.  The pendulum swings: Tolerance versus priming to NIMA.

Authors:  Shannon J Opiela; Becky Adkins
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Review 7.  Fetal regulatory T cells and peripheral immune tolerance in utero: implications for development and disease.

Authors:  Trevor D Burt
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Review 8.  Tolerance to noninherited maternal antigens in mice and humans.

Authors:  Partha Dutta; William J Burlingham
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9.  Maternal alloantigens promote the development of tolerogenic fetal regulatory T cells in utero.

Authors:  Jeff E Mold; Jakob Michaëlsson; Trevor D Burt; Marcus O Muench; Karen P Beckerman; Michael P Busch; Tzong-Hae Lee; Douglas F Nixon; Joseph M McCune
Journal:  Science       Date:  2008-12-05       Impact factor: 47.728

10.  Birth weight and coronary artery disease. The effect of gender and diabetes.

Authors:  Maria Banci; Patrizia Saccucci; Alessandro Dofcaci; Ilaria Sansoni; Andrea Magrini; Egidio Bottini; Fulvia Gloria-Bottini
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