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首页> 外文期刊>Bone marrow transplantation >Retroviral vector insertions in T-lymphocytes used for suicide gene therapy occur in gene groups with specific molecular functions.
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Retroviral vector insertions in T-lymphocytes used for suicide gene therapy occur in gene groups with specific molecular functions.

机译:用于自杀基因治疗的T淋巴细胞中逆转录病毒载体的插入发生在具有特定分子功能的基因组中。

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Graft-versus-host disease (GvHD) is a severe complication in the context of allogeneic stem cell transplantation and adoptive immunotherapy. The transfer of a suicide gene into donor T-lymphocytes (TLCs) allows selective elimination of GvHD-causing cells. As retroviral gene transfer into hematopoietic stem cells can induce leukaemia, there is an urgent need also to analyze retroviral integration sites in TLCs. We examined suicide gene-transduced TLCs in four grafts and from four transplanted patients. One-hundred and fifteen integration sites were detected in vitro. Of these 90 could be mapped to the human genome; 50% (45) were located in genes and 32% (29) were detected 10 kb upstream or downstream of transcription start sites. We found a significant overrepresentation of genes encoding for proteins with receptor activity, signal transducer activity, transcription regulator activity, nucleic acid binding activity and translation regulator activity. Similar data were obtained from patient samples. Our results point to preferred vector integration patterns, which are specific for the target cell population and probably independent of selection processes. Thus, future preclinical analysis of the integration repertoire with abundant amounts of transduced cells could allow a prediction also for the in vivo situation, where target cells are scarce.
机译:在同种异体干细胞移植和过继免疫疗法的背景下,移植物抗宿主病(GvHD)是一种严重的并发症。自杀基因转移到供体T淋巴细胞(TLC)中可以选择性消除引起GvHD的细胞。由于逆转录病毒基因转移到造血干细胞中会诱发白血病,因此迫切需要分析TLC中的逆转录病毒整合位点。我们检查了四名移植患者和四名移植患者的自杀基因转导TLC。在体外检测到一百一十五个整合位点。在这90种中,可以定位到人类基因组。 50%(45)位于基因中,而32%(29)位于转录起始位点上游或下游10 kb。我们发现编码具有受体活性,信号转导活性,转录调节活性,核酸结合活性和翻译调节活性的蛋白质的基因的显着过量表达。从患者样本中获得了相似的数据。我们的结果指出了首选的载体整合模式,该模式对靶细胞群具有特异性,并且可能与选择过程无关。因此,将来对大量转导细胞的整合库进行临床前分析可以预测靶细胞稀少的体内情况。

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