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首页> 外文期刊>Transfusion: The Journal of the American Association of Blood Banks >Many genetically defined ABO subgroups exhibit characteristic flow cytometric patterns.
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Many genetically defined ABO subgroups exhibit characteristic flow cytometric patterns.

机译:许多遗传定义的ABO亚组表现出特征性的流式细胞仪模式。

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BACKGROUND: A flow cytometric method for detection of low levels of A/B antigen had been developed previously in our laboratory. The aim of this study was to investigate if this approach could be utilized to characterize different ABO subgroups and constitute a useful tool in a reference laboratory. STUDY DESIGN AND METHODS: Blood samples causing ABO discrepancies (n = 94) by routine serology were further analyzed by ABO genotyping and flow cytometry. To verify the specificity of the monoclonal anti-A and -B reagents and to establish normal flow cytometric patterns, samples from 80 blood donors with common phenotypes were also assessed. RESULTS: Distinguishable flow cytometric patterns were detected for several subgroups but were more apparent for A(weak) (n = 80) samples than B(weak) (n = 14). Two subgroups, A(finn) (n = 11) and A(3) (n = 10) displayed diagnostic features and were used to establish reproduciblity over time and between donors. In general, the consistency within subgroups was remarkable. The allelic enhancement phenomenon was clearly visualized among A(x) samples (n = 10) where different alleles in trans resulted in high, low, or no A antigen expression. Nonsubgroup samples including O/A and O/B chimeras or A(h) and B(h) para-Bombay phenotypes displayed clearly distinguishable histograms. Samples from pregnant women (n = 10) displayed acquired A antigen loss, apparently accentuated during the third trimester. CONCLUSIONS: Genetically defined ABO subgroups and other anomalous phenotypes displayed flow cytometric profiles that may contribute valuable information to the investigation of ABO discrepancies. We conclude that the presented assay may complement traditional serology and genetic analysis in the reference laboratory setting.
机译:背景:流式细胞术检测低水平的A / B抗原的方法先前已经在我们的实验室中开发出来。这项研究的目的是调查这种方法是否可用于表征不同的ABO亚组并在参考实验室中构成有用的工具。研究设计和方法:通过ABO基因分型和流式细胞仪进一步分析了由常规血清学引起的ABO差异(n = 94)的血液样本。为了验证单克隆抗A和B试剂的特异性并建立正常的流式细胞仪模式,还对来自80个具有常见表型的献血者的样品进行了评估。结果:在几个亚组中检测到了可分辨的流式细胞仪模式,但对于A(弱)(n = 80)样本比B(弱)(n = 14)样本更明显。两个亚组A(finn)(n = 11)和A(3)(n = 10)显示出诊断特征,并用于建立随时间推移和供体之间的可重复性。总的来说,亚组内的一致性是显着的。等位基因增强现象在A(x)样品(n = 10)中清晰可见,其中反式的等位基因导致高,低或无A抗原表达。非亚组样本包括O / A和O / B嵌合体或A(h)和B(h)对孟买表型,显示出明显可区分的直方图。孕妇(n = 10)的样本显示获得性A抗原丢失,在妊娠中期明显加剧。结论:遗传定义的ABO亚组和其他异常表型显示流式细胞仪配置文件,可能有助于调查ABO差异的有价值的信息。我们得出的结论是,在参考实验室环境中,提出的检测方法可以补充传统的血清学和基因分析。

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