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通过基于克隆特异性T细胞受体连接的聚合酶链反应分析的改进来提高微小残留白血病的检测。

Improved detection of minimal residual leukemia through modifications of polymerase chain reaction analyses based on clonospecific T cell receptor junctions.

作者信息

Seriu T, Hansen-Hagge T E, Erz D H, Bartram C R

机构信息

Department of Pediatrics II, University of Ulm, Germany.

出版信息

Leukemia. 1995 Feb;9(2):316-20.

PMID:7869770
Abstract

Polymerase chain reaction (PCR) techniques utilizing clonospecific T cell receptor (TCR) gamma or delta junctional regions constitute broadly applicable strategies to study the clinical relevance of minimal residual disease (MRD) in acute lymphoblastic leukemia (ALL) patients. For the majority of cases current PCR protocols allow the reliable detection of one neoplastic cell among 10(4) to 10(6) normal counterparts. Occasionally, however, PCR analysis fails to reach this level of sensitivity. Here we demonstrate by means of three representative ALL cases how modifications of PCR protocols can overcome some of the limitations. Thus usage of biotinylated PCR products of TCR delta junctional regions and their direct application as templates for the generation of clonospecific probes allows the introduction of a selection step and results in a significant reduction of unspecific background signals. According to our experience as well as data from other laboratories we also recommend the usage of synthetic oligonucleotides representing TCR gamma junctions as clone-specific primers for a consecutive round of amplification rather than as clonospecific probes. Both modifications improve and facilitate the detection of MRD in leukemias characterized by TCR gamma and TCR delta recombinations.

摘要

利用克隆特异性T细胞受体(TCR)γ或δ连接区的聚合酶链反应(PCR)技术,构成了研究急性淋巴细胞白血病(ALL)患者微小残留病(MRD)临床相关性的广泛适用策略。对于大多数病例,当前的PCR方案能够在10⁴至10⁶个正常细胞中可靠地检测到一个肿瘤细胞。然而,偶尔PCR分析无法达到这种灵敏度水平。在此,我们通过三个具有代表性的ALL病例展示了如何通过修改PCR方案来克服一些局限性。因此,使用TCRδ连接区的生物素化PCR产物并将其直接用作生成克隆特异性探针的模板,可引入一个筛选步骤,并显著减少非特异性背景信号。根据我们的经验以及其他实验室的数据,我们还建议使用代表TCRγ连接区的合成寡核苷酸作为连续一轮扩增的克隆特异性引物,而不是作为克隆特异性探针。这两种修改都改进并促进了以TCRγ和TCRδ重组为特征的白血病中MRD的检测。

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