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短链脂肪酸对人脐静脉内皮细胞对人巨细胞病毒感染易感性的影响。

The effect of short-chain fatty acids on the susceptibility of human umbilical vein endothelial cells to human cytomegalovirus infection.

作者信息

Wu Q H, Ascensao J, Almeida G, Forman S J, Shanley J D

机构信息

Department of Medicine, University of Connecticut Health Center, Farmington 06030.

出版信息

J Virol Methods. 1994 Apr;47(1-2):37-50. doi: 10.1016/0166-0934(94)90064-7.

Abstract

We have compared the replication of three strains of human cytomegalovirus (HCMV), HCMV AD-169, HCMV Towne, or HCMV RC-256, an insertional mutant of Towne containing the LacZ gene of E. coli, in human umbilical vein endothelial cells (HUVEC) and human forskin fibroblasts (HFF). We also examine the effects of salts of short-chain fatty acids on the susceptibility of HUVEC to infection by HCMV. All three virus strains replicated in both cell types, but 10-to 100-fold less virus was produced in HUVEC cells than HFF. For all virus strains, expression of HCMV IE-1 antigen in HFF was > 70% 24 h after inoculation. In contrast, the number of HUVEC exhibiting IE-1 antigen at 24 h was < 15%. Treatment of HUVEC with sodium butyrate, sodium hexanoate, or sodium propionate prior to virus inoculation increased the IE-1 and late HCMV antigen expression in a dose- and time-dependent manner. Virus yield was also increased. This increased susceptibility was inhibited by cycloheximide and tunicamycin, indicating a requirement for new cellular protein synthesis. Treatment with both sodium hexanoate and propionate after virus inoculation increased HUVEC susceptibility to HCMV infection. Treatment of HUVEC with sodium butyrate after virus inoculation also increased HCMV IE-1 antigen expression, but only after removal of the drug. These studies demonstrate that the susceptibility of HUVEC to HCMV infection can be increased by the treatment of the host cell with salts of short-chain fatty acids, such as sodium butyrate, before or after virus inoculation.

摘要

我们比较了三株人巨细胞病毒(HCMV),即HCMV AD-169、HCMV Towne,以及HCMV RC-256(Towne的一个插入突变体,含有大肠杆菌的LacZ基因)在人脐静脉内皮细胞(HUVEC)和人包皮成纤维细胞(HFF)中的复制情况。我们还研究了短链脂肪酸盐对HUVEC受HCMV感染易感性的影响。所有三株病毒在两种细胞类型中均能复制,但在HUVEC细胞中产生的病毒量比在HFF中少10至100倍。对于所有病毒株,接种后24小时HCMV IE-1抗原在HFF中的表达>70%。相比之下,24小时时呈现IE-1抗原的HUVEC数量<15%。在病毒接种前用丁酸钠、己酸钠或丙酸钠处理HUVEC,可使IE-1和晚期HCMV抗原的表达呈剂量和时间依赖性增加。病毒产量也增加。这种增加的易感性被放线菌酮和衣霉素抑制,表明需要新的细胞蛋白质合成。在病毒接种后用己酸钠和丙酸钠处理均增加了HUVEC对HCMV感染的易感性。在病毒接种后用丁酸钠处理HUVEC也增加了HCMV IE-1抗原的表达,但仅在去除药物后。这些研究表明,在病毒接种前或接种后用短链脂肪酸盐(如丁酸钠)处理宿主细胞,可增加HUVEC对HCMV感染的易感性。

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