C1q 与登革病毒结合可降低 THP-1 细胞感染和炎症分子转录水平。
C1q binding to dengue virus decreases levels of infection and inflammatory molecules transcription in THP-1 cells.
机构信息
Fondazione Ri.MED, Via Bandiera 11, 90133 Palermo, Italy; University of Pittsburgh Center for Vaccine Research, 3501 Fifth Avenue, 9th floor, Pittsburgh, PA 15261, USA.
University of Pittsburgh Center for Vaccine Research, 3501 Fifth Avenue, 9th floor, Pittsburgh, PA 15261, USA.
出版信息
Virus Res. 2014 Jan 22;179:231-4. doi: 10.1016/j.virusres.2013.11.007. Epub 2013 Nov 15.
Abstract
Dengue virus infection elicits a spectrum of clinical presentations ranging from asymptomatic to severe disease. The mechanisms leading to severe dengue are not known, however it has been reported that the complement system is hyper-activated in severe dengue. Screening of complement proteins demonstrated that C1q, a pattern recognition molecule, can bind directly to dengue virus envelope protein and to whole dengue virus serotype 2. Incubation of dengue virus serotype 2 with C1q prior to infection of THP-1 cells led to decreased virus infectivity and modulation of mRNA expression of immunoregulatory molecules suggesting reduced inflammatory responses.
摘要
登革热病毒感染引发了一系列临床表现,从无症状到严重疾病不等。导致严重登革热的机制尚不清楚,但据报道,补体系统在严重登革热中过度激活。补体蛋白的筛选表明,模式识别分子 C1q 可以直接与登革热病毒包膜蛋白和整个登革热病毒 2 型结合。在感染 THP-1 细胞之前,将登革热病毒 2 型与 C1q 孵育,导致病毒感染性降低,并调节免疫调节分子的 mRNA 表达,提示炎症反应减轻。
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