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Identification and characterization of a second novel human erythrovirus variant, a6.

机译:第二个新型人类红细胞病毒变种a6的鉴定和表征。

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Parvovirus B19 (B19), currently the only accepted member of the Erythrovirus genus, is the only parvovirus known to be pathogenic in humans. Recently a viral sequence, tentatively termed V9 which showed 11% variability from the published B19 sequences, was described from a patient with aplastic crisis. To search for additional parvovirus variants, we used the new NS1/7.5EC PCR assay whose primers were designed from a conserved region of the B19/V9 sequence and encompasses an MfeI restriction enzyme site that would allow differentiation between B19- and V9-like sequences. Screening of 225 serum and bone marrow samples and 62 plasma pools identified one new atypical parvovirus sequence, A6, from an anemic HIV-positive patient. A6 exhibited 88% similarity to B19 and 92% to V9, compared to >98% correspondence between reported B19 isolates. Based on the genome similarity to B19, an RT-PCR for A6 capsid transcripts was developed and used to test for A6 infectivity of UT7/Epo/S1 cells. Despite high viral titers, A6 viral transcripts were not detected. Thus, although the prevalence of B19 variants probably is low, the true clinical significance remains unknown. Current PCR analyses are unlikely to detect novel variants without the design of specific primers to the A6/V9/B19 common sequences.
机译:细小病毒B19(B19)是目前唯一公认的红病毒属成员,是唯一已知对人类致病的细小病毒。最近,一位再生障碍性疾病患者描述了一种病毒序列,暂定名为V9,与已发表的B19序列显示11%的变异性。为了搜索其他细小病毒变种,我们使用了新的NS1 / 7.5EC PCR检测法,其引物是从B19 / V9序列的保守区域设计的,并且包含一个MfeI限制性酶切位点,该位点可以区分B19和V9样序列。筛查225个血清和骨髓样本以及62个血浆库,从一名贫血的HIV阳性患者中鉴定出一种新的非典型细小病毒序列A6。与报道的B19分离株之间> 98%的对应性相比,A6与B19的相似性为88%,与V9的相似性为92%。基于与B19的基因组相似性,开发了A6衣壳转录本的RT-PCR,并用于测试UT7 / Epo / S1细胞的A6感染性。尽管病毒滴度很高,但未检测到A6病毒转录物。因此,尽管B19变异的患病率可能很低,但真正的临床意义仍然未知。如果不设计针对A6 / V9 / B19共同序列的特异性引物,当前的PCR分析不可能检测出新颖的变异体。

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