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人巨细胞病毒趋化因子(UL146/UL147)和细胞因子受体基因(UL144)中的多态性不能预测先天性感染儿童的后遗症。

Polymorphisms within human cytomegalovirus chemokine (UL146/UL147) and cytokine receptor genes (UL144) are not predictive of sequelae in congenitally infected children.

作者信息

Heo Jinho, Petheram Susie, Demmler Gail, Murph Jody R, Adler Stuart P, Bale James, Sparer Tim E

机构信息

The University of Tennessee, Department of Microbiology, 1414 Cumberland Ave., Knoxville, TN 37996, USA.

出版信息

Virology. 2008 Aug 15;378(1):86-96. doi: 10.1016/j.virol.2008.05.002. Epub 2008 Jun 16.

Abstract

Human cytomegalovirus (HCMV) viral chemokine, UL146, and TNF alpha-like receptor UL144 genes show a high degree of hypervariability in clinical isolates. These proteins are predicted to be immune modulators and may contribute to the pathogenesis of HCMV infections. We analyzed the UL146 and UL144 genetic variation of 51 HCMV isolates from congenitally infected children and 13 isolates from children in childcare. There was no statistically significant correlation between UL146 and UL144 genotypes and HCMV disease and/or sequelae. However, there were some groups that had a relatively large proportion of asymptomatic outcomes. These included UL146 group 8 (7/8 asymptomatic) and UL146 group 10 (3/3 asymptomatic). UL144 group B had 11/15 (73%) asymptomatic. UL146 and UL144 genes remained stable in serial isolates from children in daycare for intervals up to three years. These results indicate that most UL146 and UL144 genotypes do not predict clinical sequelae following congenital HCMV infections.

摘要

人巨细胞病毒(HCMV)的病毒趋化因子UL146和肿瘤坏死因子α样受体UL144基因在临床分离株中表现出高度的高变异性。这些蛋白质被预测为免疫调节剂,可能有助于HCMV感染的发病机制。我们分析了51例先天性感染儿童的HCMV分离株和13例托育儿童的分离株的UL146和UL144基因变异。UL146和UL144基因型与HCMV疾病和/或后遗症之间没有统计学上的显著相关性。然而,有一些组的无症状结局比例相对较大。这些包括UL146第8组(7/8无症状)和UL146第10组(3/3无症状)。UL144 B组有11/15(73%)无症状。在日托儿童长达三年的连续分离株中,UL146和UL144基因保持稳定。这些结果表明,大多数UL146和UL144基因型不能预测先天性HCMV感染后的临床后遗症。

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