首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Productive cytomegalovirus (CMV) infection exclusively in CD13-positive peripheral blood mononuclear cells from CMV-infected individuals: implications for prevention of CMV transmission.
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Productive cytomegalovirus (CMV) infection exclusively in CD13-positive peripheral blood mononuclear cells from CMV-infected individuals: implications for prevention of CMV transmission.

机译:生产性巨细胞病毒(CMV)仅感染来自CMV感染个体的CD13阳性外周血单核细胞感染:对预防CMV传播的意义。

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BACKGROUND: Monocytes are suggested to harbor latent cytomegalovirus (CMV) in peripheral blood, which concurs with the finding that all CMV-susceptible cells carry the CD13 surface molecule. Here, we investigated whether all latently and productively CMV-infected peripheral blood mononuclear cells (PBMCs) could be eliminated by depletion of CD13-expressing cells. METHODS: Depletion of CD13-positive cells was performed with monoclonal antibodies and magnetic cell separation (MACS) beads followed by MACS. CMV DNA and cDNA were amplified by polymerase chain reaction with specific primers for two CMV genes, major immediate early and phosphoprotein 150. The presence of infectious virus was tested by incubating homogenized in vitro- or in vivo-infected PBMCs with human fibroblasts. CMV infection of fibroblasts was detected by intracellular expression of CMV proteins. RESULTS: Elimination of CD13-positive PBMCs removed productively in vitro- and in vivo-infected cells, as demonstrated by detection of infectious virus only in PBMC fractions containing CD13-positive cells. In support of this finding, CMV RNA was not detected in pure CD13-negative cell fractions. Furthermore, CMV DNA was found exclusively in CD13-positive PBMCs obtained from patients with acute CMV infection. CONCLUSIONS: Our data suggest that CMV replicates exclusively in CD13-positive PBMCs. These findings have important clinical applications, because the elimination of CD13-positive cells may reduce the risk for transmission of latent CMV in blood products and bone marrow grafts and thereby also decrease the risk for CMV-induced complications, such as chronic graft-versus-host disease in bone marrow transplant patients.
机译:背景:建议单核细胞在外周血中带有潜伏巨细胞病毒(CMV),这与所有CMV易感细胞都带有CD13表面分子的发现是一致的。在这里,我们研究了是否可以通过消耗表达CD13的细胞消除所有潜在和生产性CMV感染的外周血单核细胞(PBMC)。方法:使用单克隆抗体和磁性细胞分离(MACS)磁珠,然后进行MACS进行CD13阳性细胞的耗竭。通过与两个CMV基因(主要即早和磷蛋白150)的特异性引物通过聚合酶链反应扩增CMV DNA和cDNA。通过将均质的体外或体内感染的PBMC与人成纤维细胞温育来测试感染性病毒的存在。通过细胞内CMV蛋白表达检测成纤维细胞的CMV感染。结果:消除CD13阳性PBMC可以有效地去除体外和体内感染的细胞,如仅在含有CD13阳性细胞的PBMC组分中检测到传染性病毒所证明的。为了支持这一发现,在纯CD13阴性细胞级分中未检测到CMV RNA。此外,CMV DNA仅存在于从急性CMV感染患者获得的CD13阳性PBMC中。结论:我们的数据表明CMV仅在CD13阳性PBMC中复制。这些发现具有重要的临床应用价值,因为消除CD13阳性细胞可降低血液制品和骨髓移植物中潜在CMV传播的风险,从而也降低了CMV引起并发症的风险,例如慢性移植物抗-骨髓移植患者的宿主疾病。

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