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Assessment of transcriptomal analysis of varicella-zoster-virus gene expression in patients with and without post-herpetic neuralgia

机译:疱疹后神经痛和非疱疹后神经痛患者水痘-带状疱疹病毒基因表达的转录组分析评估

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Varicella-Zoster virus (VZV) is a human herpes virus that reactivates from a latent state in human trigeminal and dorsal root ganglia to cause herpes zoster (shingles) which is a painful vesicular dermatomal skin eruption. The major complication of herpes zoster is post-herpetic neuralgia (PHN) which is a serious condition occurring especially in individuals over 50 years. PHN is extremely painful, may be permanent, and is frequently very refractory to all treatment. The ability to identify those patients with herpes zoster who are likely to develop PHN would be highly beneficial as it would allow pre-emptive anti-viral therapy. We have assessed the potential of using long oligonucleotide VZV microarrays to determine whether MeWo cells infected with VZV isolates obtained from 13 patients with zoster who had subsequently developed PHN showed significant transcriptomal differences from MeWo cells infected with viruses isolated from ten zoster patients who had not developed PHN. We found that viral gene expression from sample to sample within a group (PHN patients or non-PHN patients) varied as much, or more, than the viral gene expression between those groups. Quantitative real-time polymerase chain reaction studies carried out on 11 open reading frames on four representative viral infected MeWo cell lines (two from each group) confirmed the transcriptomal heterogeneity between the two groups. Growth curve analyses of ten representative infected cell lines (five from each group) showed that PHN and non-PHN-associated viruses replicated equally efficiently. Taken together, these findings suggest that viral microarray-based transcriptomal measurements are unlikely to prove of clinical utility in predicting the incidence of PHN.
机译:水痘带状疱疹病毒(VZV)是一种人疱疹病毒,它从人三叉神经和背根神经节的潜伏状态重新激活,导致带状疱疹(带状疱疹),这是一种痛苦的水疱性皮肤皮肤喷发。带状疱疹的主要并发症是带状疱疹后神经痛(PHN),这是一种严重的状况,尤其是在50岁以上的人群中。 PHN极度疼痛,可能是永久性的,并且通常对所有治疗都难以治愈。识别那些可能发展为PHN的带状疱疹患者的能力将非常有益,因为它将允许先发制人的抗病毒治疗。我们评估了使用长寡核苷酸VZV芯片来确定感染从后来患PHN的13位带状疱疹患者获得的VZV分离株感染的MeWo细胞与从感染了10个尚未发育的带状疱疹患者中分离的病毒感染的MeWo细胞是否存在明显的转录组差异的潜力PHN。我们发现,在一组(PHN患者或非PHN患者)中,样本之间的病毒基因表达与这些组之间的病毒基因表达变化相同或更多。在四个代表性病毒感染的MeWo细胞系(每组两个)上的11个开放阅读框上进行的实时定量聚合酶链反应研究证实了两组之间的转录组异质性。对十种代表性感染细胞系(每组五种)的生长曲线分析表明,PHN和非PHN相关病毒均有效复制。综上所述,这些发现表明基于病毒微阵列的转录组测量不太可能证明其在预测PHN发病率方面的临床实用性。

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