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牛可透析白细胞提取物抗1型人类免疫缺陷病毒感染的抗病毒作用方式。

Antiviral mode of action of bovine dialyzable leukocyte extract against human immunodeficiency virus type 1 infection.

作者信息

Lara Humberto H, Ixtepan-Turrent Liliana, Garza-Treviño Elsa N, Badillo-Almaraz Jose I, Rodriguez-Padilla Cristina

机构信息

Laboratorio de Inmunología y Virología, Departamento de Microbiología e Inmunología, Universidad Autonoma de Nuevo Leon, Nuevo Leon, Mexico.

出版信息

BMC Res Notes. 2011 Nov 1;4:474. doi: 10.1186/1756-0500-4-474.

Abstract

BACKGROUND

Bovine dialyzable leukocyte extract (bDLE) is derived from immune leukocytes obtained from bovine spleen. DLE has demonstrated to reduce transcription of Human Immunodeficiency Virus Type 1 (HIV-1) and inactivate the nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB) signaling pathway. Therefore, we decided to clarify the mode of antiviral action of bDLE on the inhibition of HIV-1 infection through a panel of antiviral assays.

RESULTS

The cytotoxicity, HIV-1 inhibition activity, residual infectivity of bDLE in HIV-1, time of addition experiments, fusion inhibition of bDLE for fusogenic cells and the duration of cell protection even after the removal of bDLE were all assessed in order to discover more about the mode of the antiviral action.HIV-1 infectivity was inhibited by bDLE at doses that were not cytotoxic for HeLa-CD4-LTR-β-gal cells. Pretreatment of HIV-1 with bDLE did not decrease the infectivity of these viral particles. Cell-based fusion assays helped to determine if bDLE could inhibit fusion of Env cells against CD4 cells by membrane fusion and this cell-based fusion was inhibited only when CD4 cells were treated with bDLE. Infection was inhibited in 80% compared with the positive (without EDL) at all viral life cycle stages in the time of addition experiments when bDLE was added at different time points. Finally, a cell-protection assay against HIV-1 infection by bDLE was performed after treating host cells with bDLE for 30 minutes and then removing them from treatment. From 0 to 7 hours after the bDLE was completely removed from the extracellular compartment, HIV-1 was then added to the host cells. The bDLE was found to protect the cells from HIV-1 infection, an effect that was retained for several hours.

CONCLUSIONS

bDLE acted as an antiviral compound and prevented host cell infection by HIV-1 at all viral life cycle stages. These cell protection effects lingered for hours after the bDLE was removed. Interestingly, bDLE inhibited fusion of fusogenic cells by acting only on CD4 cells. bDLE had no virucidal effect, but could retain its antiviral effect on target cells after it was removed from the extracellular compartment, protecting the cells from infection for hours.bDLE, which has no reported side effects or toxicity in clinical trials, should therefore be further studied to determine its potential use as a therapeutic agent in HIV-1 infection therapy, in combination with known antiretrovirals.

摘要

背景

牛可透析白细胞提取物(bDLE)源自从牛脾脏获得的免疫白细胞。已证明DLE可减少1型人类免疫缺陷病毒(HIV-1)的转录,并使活化B细胞的核因子κ轻链增强子(NF-κB)信号通路失活。因此,我们决定通过一系列抗病毒试验来阐明bDLE对HIV-1感染抑制作用的抗病毒作用模式。

结果

为了更深入了解抗病毒作用模式,对bDLE的细胞毒性、HIV-1抑制活性、在HIV-1中的残余感染性、添加时间实验、bDLE对融合细胞的融合抑制作用以及即使在去除bDLE后细胞保护的持续时间进行了评估。bDLE在对HeLa-CD4-LTR-β-gal细胞无细胞毒性的剂量下抑制了HIV-1的感染性。用bDLE预处理HIV-1并未降低这些病毒颗粒的感染性。基于细胞的融合试验有助于确定bDLE是否可通过膜融合抑制Env细胞与CD4细胞的融合,并且仅当CD4细胞用bDLE处理时这种基于细胞的融合才被抑制。在添加时间实验中,当在不同时间点添加bDLE时,在所有病毒生命周期阶段,与阳性对照(无EDL)相比,感染被抑制了80%。最后,在用bDLE处理宿主细胞30分钟然后停止处理后,进行了bDLE对HIV-1感染的细胞保护试验。在bDLE从细胞外区室完全去除后的0至7小时内,然后将HIV-1添加到宿主细胞中。发现bDLE可保护细胞免受HIV-1感染,这种作用可持续数小时。

结论

bDLE作为一种抗病毒化合物,在所有病毒生命周期阶段均能预防宿主细胞被HIV-1感染。在去除bDLE后,这些细胞保护作用会持续数小时。有趣的是,bDLE仅通过作用于CD4细胞来抑制融合细胞的融合。bDLE没有杀病毒作用,但从细胞外区室去除后仍可对靶细胞保持其抗病毒作用,保护细胞免受感染达数小时。bDLE在临床试验中未报告有副作用或毒性反应,因此应进一步研究以确定其作为HIV-1感染治疗中的治疗剂与已知抗逆转录病毒药物联合使用的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/17a5/3219789/0fd2cb48a65a/1756-0500-4-474-1.jpg

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