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分泌型天冬氨酸蛋白酶在人类口腔念珠菌病模型及口腔患者样本中的差异表达

Differential expression of secreted aspartyl proteinases in a model of human oral candidosis and in patient samples from the oral cavity.

作者信息

Schaller M, Schäfer W, Korting H C, Hube B

机构信息

Institute for General Botany, Applied Molecular Biology III, University of Hamburg, Germany.

出版信息

Mol Microbiol. 1998 Jul;29(2):605-15. doi: 10.1046/j.1365-2958.1998.00957.x.

Abstract

Candida albicans, an opportunistic pathogen in humans, secretes secretory aspartyl proteinases (Saps), which have been correlated with virulence. We examined the temporal regulation of the mRNA expression of seven known members of the SAP gene family by reverse transcription polymerase chain reaction (RT-PCR) in (i) an in vitro model of oral candidosis based on reconstituted human epithelium (RHE); and (ii) clinical samples from patients with oral candidosis. SAP1 and SAP3 transcripts were first detected 42 h after inoculation of RHE, while at the same time, slight morphological alterations in the epithelium were documented by light microscopy. SAP6 expression occurred 6 h later concomitantly with germ tube formation of some infecting Candida cells and severe lesions of the epithelial tissue. SAP2 and SAP8 RT-PCR products were first detected 60 h after infection, while SAP4 and SAP5 transcripts were never discovered. Thus, a temporal progression of SAP expression in the order SAP1 and SAP3 > SAP6 > SAP2 and SAP8 was observed at the same time as increasing RHE damage occurred. At the protein level, Sap antigen was found within the C. albicans yeast cells and the epithelial cells by immunoelectron microscopy using an anti-Sap murine monoclonal antibody directed against the gene products Sap1-3. Expression of SAP1-3 and 6 was also detected by RT-PCR in samples from patients suffering from oral candidosis. Our results suggest that the pathogenesis of experimental and clinical oral candidosis is associated with the differential and temporal regulation of SAP gene expression.

摘要

白色念珠菌是人类的一种机会致病菌,可分泌分泌型天冬氨酸蛋白酶(Saps),这些酶与毒力相关。我们通过逆转录聚合酶链反应(RT-PCR),在以下两种情况下检测了SAP基因家族七个已知成员mRNA表达的时间调控:(i)基于重组人上皮(RHE)的口腔念珠菌病体外模型;(ii)口腔念珠菌病患者的临床样本。接种RHE后42小时首次检测到SAP1和SAP3转录本,与此同时,光学显微镜记录到上皮细胞有轻微形态改变。SAP6表达在6小时后出现,同时一些感染的念珠菌细胞形成芽管,上皮组织出现严重病变。感染后60小时首次检测到SAP2和SAP8的RT-PCR产物,而从未发现SAP4和SAP5转录本。因此,随着RHE损伤加剧,观察到SAP表达按SAP1和SAP3 > SAP6 > SAP2和SAP8的顺序呈时间性进展。在蛋白质水平,通过使用针对基因产物Sap1-3的抗Sap鼠单克隆抗体进行免疫电子显微镜观察,在白色念珠菌酵母细胞和上皮细胞中发现了Sap抗原。在口腔念珠菌病患者的样本中,通过RT-PCR也检测到了SAP1-3和6的表达。我们的结果表明,实验性和临床口腔念珠菌病的发病机制与SAP基因表达的差异和时间调控有关。

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