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BK Polyomavirus MicroRNA Levels in Exosomes Are Modulated by Non-Coding Control Region Activity and Down-Regulate Viral Replication When Delivered to Non-Infected Cells Prior to Infection

机译：外来体中的BK多瘤病毒MicroRNA水平受非编码控制区活性的调节并在感染前交付至未感染细胞时下调病毒复制。

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In immunosuppressed patients, BKPyV-variants emerge carrying rearranged non-coding control-regions (rr-NCCRs) that increase early viral gene region (EVGR) expression and replication capacity. BKPyV also encodes microRNAs, which have been reported to downregulate EVGR-encoded large T-antigen transcripts, to decrease viral replication in infected cells and to be secreted in exosomes. To investigate the interplay of NCCR and microRNAs, we compared archetype- and rr-NCCR-BKPyV infection in cell culture. We found that laboratory and clinical rr-NCCR-BKPyV-strains show higher replication rates but significantly lower microRNA levels than archetype virus intracellularly and in exosomes. To investigate whether rr-NCCR or increased EVGR activity modulated microRNA levels, we examined the (sp1-4)NCCR-BKPyV, which has an archetype NCCR-architecture but shows increased EVGR expression due to point mutations inactivating one Sp1 binding site. We found that microRNA levels following (sp1-4)NCCR-BKPyV infection were as low as in rr-NCCR-variants. Thus, NCCR rearrangements are not required for lower miRNA levels. Accordingly, Sp1 siRNA knock-down decreased microRNA levels in archetype BKPyV infection but had no effect on (sp1-4)- or rr-NCCR-BKPyV. However, rr-NCCR-BKPyV replication was downregulated by exosome preparations carrying BKPyV-microRNA prior to infection. To explore the potential relevance in humans, urine samples from 12 natalizumab-treated multiple sclerosis patients were analysed. In 7 patients, rr-NCCR-BKPyV were detected showing high urine BKPyV loads but low microRNAs levels, whereas the opposite was seen in 5 patients with archetype BKPyV. We discuss the results in a dynamic model of BKPyV replication according to NCCR activity and exosome regulation, which integrates immune selection pressure, spread to new host cells and rr-NCCR emergence.

机译：在免疫抑制的患者中，BKPyV变异体出现带有重排的非编码控制区（rr-NCCR），从而增加了早期病毒基因区（EVGR）的表达和复制能力。 BKPyV还编码microRNA，据报道它们可下调EVGR编码的大T抗原转录本，从而减少病毒在感染细胞中的复制并在外泌体中分泌。为了研究NCCR和microRNA的相互作用，我们比较了细胞培养中原型和rr-NCCR-BKPyV感染。我们发现实验室和临床rr-NCCR-BKPyV菌株显示出较高的复制率，但与细胞内和外泌体中的原型病毒相比，其microRNA水平明显降低。若要研究rr-NCCR或增加的EVGR活性是否能调节microRNA水平，我们检查了（sp1-4）NCCR-BKPyV，它具有原型NCCR架构，但由于点突变使一个Sp1结合位点失活而显示出EVGR表达增加。我们发现（sp1-4）NCCR-BKPyV感染后的microRNA水平与rr-NCCR变体一样低。因此，较低的miRNA水平不需要NCCR重排。因此，Sp1 siRNA敲低降低了原型BKPyV感染中的microRNA水平，但对（sp1-4）-或 rr-NCCR-BKPyV 没有影响。然而，感染前携带 BKPyV -microRNA的外来体制剂会下调 rr-NCCR-BKPyV 复制。为了探索与人类的潜在相关性，分析了来自那他珠单抗治疗的12例多发性硬化症患者的尿液样本。在7例患者中，检测到 rr-NCCR-BKPyV 表现出高尿液 BKPyV 载量但microRNA水平较低，而5例原型 BKPyV < / em>。我们将根据 NCCR 活性和外来体调节，在 BKPyV 复制的动态模型中讨论结果，该模型整合了免疫选择压力，扩散到新的宿主细胞和 rr- NCCR 的出现。 展开▼

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期刊名称 Viruses

作者
Francesco Martelli; Zongsong Wu; Serena Delbue; Fabian H. Weissbach; Maria Chiara Giulioli; Pasquale Ferrante; Hans H. Hirsch; Simone Giannecchini;
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年(卷),期 2018(10),9

年度 2018

页码 466

总页数 21

原文格式 PDF

正文语种

中图分类人体病毒学（致病病毒）;病毒（滤过性病毒）;

关键词
polyomavirus non-coding control region microRNA exosomes persistence immunosuppression BK virus;

机译：多瘤病毒;非编码控制区;microRNA;外来体;持续性;免疫抑制;BK病毒;

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专利

1. Possible antiviral effect of ciprofloxacin treatment on polyomavirus BK replication and analysis of non-coding control region sequences [J] . Ilaria Umbro, Elena Anzivino, Francesca Tinti, Virology Journal . 2013,第1期

机译：环丙沙星治疗对多瘤病毒BK复制的可能抗病毒作用以及非编码控制区序列的分析

2. Polyomavirus BK with rearranged noncoding control region emerge in vivo in renal transplant patients and increase viral replication and cytopathology [J] . Rainer Gosert, Christine H. Rinaldo, Georg A. Funk, The Journal of Experomental Medicine . 2008,第4期

机译：具有重排非编码控制区的多瘤病毒BK在肾移植患者体内出现并增加病毒复制和细胞病理学

3. Polyomavirus BK-encoded microRNA suppresses autoregulation of viral replication [J] . TianY.-C., LiY.-J., ChenH.-C., Biochemical and Biophysical Research Communications . 2014,第3期

机译：Polyomavirus BK编码的microRNA抑制了病毒复制的自身

4. Possible antiviral effect of ciprofloxacin treatment on polyomavirus BK replication and analysis of non-coding control region sequences [O] . Ilaria Umbro, Elena Anzivino, Francesca Tinti, 2013

机译：环丙沙星治疗对多瘤病毒BK复制的可能抗病毒作用以及非编码控制区序列的分析

5. BK Polyomavirus MicroRNA Levels in Exosomes Are Modulated by Non-Coding Control Region Activity and Down-Regulate Viral Replication When Delivered to Non-Infected Cells Prior to Infection [O] . Francesco Martelli, Zongsong Wu, Serena Delbue, 2018

机译：当在感染之前递送到未感染的细胞时，通过非编码控制区域活性和下调病毒复制来调节外瘤中的BK多瘤病毒微小RORNA水平

1. Genetically engineered hepatitis c virus (hcv) nucleic acid clone, plasmid clone that houses a life-size hcv cdna, dna or rna transcribed from the full-length hcv cdna, transfected and in vitro infected host cell line with hcv, non-human animal infected with hcv, hcv viral particle, in vitro test system, hcv cell free, hcv vaccine and hcv test set and processes for identifying a cell line that is permissive and an animal that is permissive for hcv infection, to select hcv with adaptive mutations that allow higher levels of hcv replication in a permissive cell line, to infect an animal with hcv, to spread hcv in vitro, to transduce an animal susceptible to hcv infection with a heterologous gene, to produce hcv viral particles, hcv particle proteins and hcv antibodies, to separate agents capable of to modulate hcv replication, to prepare a hcv nucleic acid and to detect hcv antibodies in a biological sample from a patient. [P] . 外国专利： BR9808147A . 2000-03-28

机译：基因工程丙型肝炎病毒（hcv）核酸克隆，质粒克隆，其中包含从全长hcv cdna转录而来的真人大小的hcv cdna，dna或rna，并通过非人类动物的hcv转染和体外感染宿主细胞系被hcv感染，hcv病毒颗粒，体外测试系统，无hcv细胞，hcv疫苗和hcv测试仪的感染以及鉴定允许的细胞系和允许感染hvv的动物的过程，以选择具有以下适应性突变的hcv：允许在允许的细胞系中进行更高水平的hvv复制，以hvv感染动物，在体外传播hvv，用异源基因转导易感染hvv的动物，产生hvv病毒颗粒，hvv颗粒蛋白和hvv抗体分离能够调节hcv复制的试剂，制备hcv核酸并检测患者生物样品中的hcv抗体。

2. viral, cloning or expression vector, transgenic microorganism, pharmaceutical composition, kit for detecting an htrt polynucleotide or fragment thereof, uses of a polynucleotide, a peptide, a transgenic microorganism and a vector, and methods for obtaining a htrt recombinant peptide, to inhibit htrt expression, to increase the replicative ability of a cell, to detect an htrt polynucleotide or fragment thereof, to evaluate a condition associated with altered htrt expression, to express a heterologous gene, to selectively extinguish a trt-expressing cell, and to map a test compound for an ability to modulate trt promoter activity [P] . 外国专利： BRPI9712254B1 . 2019-01-15

机译：病毒，克隆或表达载体，转基因微生物，药物组合物，用于检测htrt多核苷酸或其片段的试剂盒，多核苷酸，肽，转基因微生物和载体的用途以及获得htrt重组肽以抑制htrt的方法表达，以增加细胞的复制能力，检测htrt多核苷酸或其片段，评估与htrt表达改变有关的条件，表达异源基因，选择性灭绝表达trt的细胞，并进行检测具有调节trt启动子活性的能力的化合物

3. Modulating dendritic cell activity, e.g. for treatment of viral infections, NK-sensitive tumors or autoimmune diseases, using inhibitors or specific tyrosine kinases, e.g. c-abl, bcr/abl and c-kit [P] . 外国专利： FR2844452A1 . 2004-03-19

机译：调节树突状细胞的活性，例如使用抑制剂或特定的酪氨酸激酶，例如用于治疗病毒感染，NK敏感性肿瘤或自身免疫性疾病的药物c-abl，bcr / abl和c-kit

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BK Polyomavirus MicroRNA Levels in Exosomes Are Modulated by Non-Coding Control Region Activity and Down-Regulate Viral Replication When Delivered to Non-Infected Cells Prior to Infection

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