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超微结构、免疫荧光和 RNA 证据支持与川崎病相关的“新”病毒假说。

Ultrastructural, immunofluorescence, and RNA evidence support the hypothesis of a "new" virus associated with Kawasaki disease.

机构信息

Department of Pediatrics, Feinberg School of Medicine, Children's Memorial Hospital, Northwestern University, Chicago, Illinois 60611, USA.

出版信息

J Infect Dis. 2011 Apr 1;203(7):1021-30. doi: 10.1093/infdis/jiq136.

Abstract

BACKGROUND

Intracytoplasmic inclusion bodies (ICI) have been identified in ciliated bronchial epithelium of Kawasaki disease (KD) patients using a synthetic antibody derived from acute KD arterial IgA plasma cells; ICI may derive from the KD etiologic agent.

METHODS

Acute KD bronchial epithelium was subjected to immunofluorescence for ICI and cytokeratin, high-throughput sequencing, and transmission electron microscopy (TEM). Interferon pathway gene expression profiling was performed on KD lung.

RESULTS

An intermediate filament cytokeratin "cage" was not observed around KD ICI, making it unlikely that ICI are overproduced or misfolded human protein aggregates. Many interferon-stimulated genes were detected in the bronchial epithelium, and significant modulation of the interferon response pathway was observed in the lung tissue of KD patients. No known virus was identified by sequencing. Aggregates of virus-like particles (VLP) were detected by TEM in all 3 acute KD patients from whom nonembedded formalin-fixed lung tissue was available.

CONCLUSIONS

KD ICI are most likely virus induced; bronchial cells with ICI contain VLP that share morphologic features among several different RNA viral families. Expedited autopsies and tissue fixation from acute KD fatalities are urgently needed to more clearly ascertain the VLP. These findings are compatible with the hypothesis that the infectious etiologic agent of KD may be a "new" RNA virus.

摘要

背景

使用源自急性川崎病动脉 IgA 浆细胞的合成抗体,在川崎病(KD)患者的纤毛支气管上皮中鉴定出细胞内包涵体(ICI);ICI 可能来自 KD 的病原体。

方法

对急性 KD 支气管上皮进行 ICI 和细胞角蛋白的免疫荧光、高通量测序和透射电子显微镜检查(TEM)。对 KD 肺进行干扰素途径基因表达谱分析。

结果

在 KD ICI 周围未观察到中间丝细胞角蛋白“笼”,这使得 ICI 不太可能是过量产生或错误折叠的人类蛋白聚集体。在支气管上皮中检测到许多干扰素刺激基因,并且在 KD 患者的肺组织中观察到干扰素反应途径的显著调节。通过测序未鉴定出已知病毒。通过 TEM 在所有 3 例可获得非包埋福尔马林固定肺组织的急性 KD 患者中均检测到病毒样颗粒(VLP)聚集体。

结论

KD ICI 很可能是病毒诱导的;含有 ICI 的支气管细胞含有 VLP,其形态特征在几种不同的 RNA 病毒家族中相似。迫切需要对急性 KD 死亡病例进行快速尸检和组织固定,以更清楚地确定 VLP。这些发现与 KD 的感染病原体可能是“新型”RNA 病毒的假说一致。

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