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利用 HLA 靶向流式细胞术对血细胞进行分选,可分离出纯合且有活力的微嵌合体细胞群体。

HLA-targeted flow cytometric sorting of blood cells allows separation of pure and viable microchimeric cell populations.

机构信息

Department of Immunohematology and Blood Transfusion, Leiden University Medical Center, The Netherlands.

出版信息

Blood. 2011 Nov 10;118(19):e149-55. doi: 10.1182/blood-2011-06-362053. Epub 2011 Sep 19.

Abstract

Microchimerism is defined by the presence of low levels of nonhost cells in a person. We developed a reliable method for separating viable microchimeric cells from the host environment. For flow cytometric cell sorting, HLA antigens were targeted with human monoclonal HLA antibodies (mAbs). Optimal separation of microchimeric cells (present at a proportion as low as 0.01% in artificial mixtures) was obtained with 2 different HLA mAbs, one targeting the chimeric cells and the other the background cells. To verify purity of separated cell populations, flow-sorted fractions of 1000 cells were processed for DNA analysis by HLA-allele-specific and Y-chromosome-directed real-time quantitative PCR assays. After sorting, PCR signals of chimeric DNA markers in the positive fractions were significantly enhanced compared with those in the presort samples, and they were similar to those in 100% chimeric control samples. Next, we demonstrate applicability of HLA-targeted FACS sorting after pregnancy by separating chimeric maternal cells from child umbilical cord mononuclear cells. Targeting allelic differences with anti-HLA mAbs with FACS sorting allows maximal enrichment of viable microchimeric cells from a background cell population. The current methodology enables reliable microchimeric cell detection and separation in clinical specimens.

摘要

微嵌合体是指一个人身体中存在低水平的非宿主细胞。我们开发了一种从宿主环境中分离存活的微嵌合细胞的可靠方法。对于流式细胞分选,使用人源单克隆 HLA 抗体 (mAb) 靶向 HLA 抗原。通过使用 2 种不同的 HLA mAb ,一种针对嵌合体细胞,另一种针对背景细胞,最佳地分离了微嵌合细胞(在人工混合物中存在的比例低至 0.01%)。为了验证分离细胞群体的纯度,通过 HLA 等位基因特异性和 Y 染色体定向实时定量 PCR 分析对 1000 个细胞的流式分选馏分进行了 DNA 分析。分选后,阳性馏分中嵌合 DNA 标记的 PCR 信号与预分选样品相比显著增强,并且与 100%嵌合对照样品相似。接下来,我们通过从儿童脐带单核细胞中分离嵌合母体细胞来证明 HLA 靶向 FACS 分选在妊娠后的适用性。使用抗 HLA mAb 通过 FACS 分选靶向等位基因差异可最大限度地从背景细胞群体中富集存活的微嵌合细胞。目前的方法学可在临床标本中实现可靠的微嵌合细胞检测和分离。

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