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人类免疫缺陷病毒 1 型(HIV-1)在巨噬细胞中整合引起的基因表达网络拓扑变化。

Changes in the topology of gene expression networks by human immunodeficiency virus type 1 (HIV-1) integration in macrophages.

机构信息

Bioinformatics Lab, Department of Biology, University of Puerto Rico, Rio Piedras, PO Box 23360, Puerto Rico.

出版信息

Virus Res. 2012 Jan;163(1):91-7. doi: 10.1016/j.virusres.2011.08.015. Epub 2011 Aug 27.

Abstract

One key step of human immunodeficiency virus type 1 (HIV-1) infection is the integration of its viral cDNA. This process is mediated through complex networks of host-virus interactions that alter several normal cell functions of the host. To study the complexity of disturbances in cell gene expression networks by HIV-1 integration, we constructed a network of human macrophage genes located close to chromatin regions rich in proviruses. To perform the network analysis, we selected 28 genes previously identified as the target of cDNA integration and their transcriptional profiles were obtained from GEO Profiles (NCBI). A total of 2770 interactions among the 28 genes located around the HIV-1 proviruses in human macrophages formed a highly dense main network connected to five sub-networks. The overall network was significantly enriched by genes associated with signal transduction, cellular communication and regulatory processes. To simulate the effects of HIV-1 integration in infected macrophages, five genes with the most number of interaction in the normal network were turned off by putting in zero the correspondent expression values. The HIV-1 infected network showed changes in its topology and alteration in the macrophage functions reflected in a re-programming of biosynthetic and general metabolic process. Understanding the complex virus-host interactions that occur during HIV-1 integration, may provided valuable genomic information to develop new antiviral treatments focusing on the management of some specific gene expression networks associated with viral integration. This is the first gene network which describes the human macrophages genes interactions related with HIV-1 integration.

摘要

人类免疫缺陷病毒 1 型(HIV-1)感染的一个关键步骤是其病毒 cDNA 的整合。这个过程是通过宿主-病毒相互作用的复杂网络介导的,这些相互作用改变了宿主的几个正常细胞功能。为了研究 HIV-1 整合对细胞基因表达网络的复杂性干扰,我们构建了一个靠近富含前病毒染色质区域的人巨噬细胞基因网络。为了进行网络分析,我们选择了 28 个先前被确定为 cDNA 整合靶点的基因,它们的转录谱来自 GEO 简介(NCBI)。位于人类巨噬细胞 HIV-1 前病毒附近的 28 个基因之间的 2770 个相互作用形成了一个高度密集的主网络,连接到五个子网络。整个网络显著富集了与信号转导、细胞通讯和调节过程相关的基因。为了模拟 HIV-1 整合感染巨噬细胞的影响,我们通过将对应表达值设置为零,关闭了正常网络中具有最多相互作用的五个基因。感染 HIV-1 的网络显示出拓扑结构的变化,以及巨噬细胞功能的改变,反映了生物合成和一般代谢过程的重新编程。了解 HIV-1 整合过程中发生的复杂病毒-宿主相互作用,可能为开发新的抗病毒治疗方法提供有价值的基因组信息,这些方法侧重于管理与病毒整合相关的一些特定基因表达网络。这是第一个描述与 HIV-1 整合相关的人巨噬细胞基因相互作用的基因网络。

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