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染色体整合型 HHV-6A 的高级染色质结构预测整合位点。

Higher-Order Chromatin Structures of Chromosomally Integrated HHV-6A Predict Integration Sites.

机构信息

Department of Biomedical and Health Sciences, College of Nursing and Health Sciences, University of Vermont, Burlington, VT, United States.

Institute of Virology, Freie Universität Berlin, Berlin, Germany.

出版信息

Front Cell Infect Microbiol. 2021 Feb 26;11:612656. doi: 10.3389/fcimb.2021.612656. eCollection 2021.

Abstract

Human herpesvirus -6A and 6B (HHV-6A/B) can integrate their genomes into the telomeres of human chromosomes. Viral integration can occur in several cell types, including germinal cells, resulting in individuals that harbor the viral genome in every cell of their body. The integrated genome is efficiently silenced but can sporadically reactivate resulting in various clinical symptoms. To date, the integration mechanism and the subsequent silencing of HHV-6A/B genes remains poorly understood. Here we investigate the genome-wide chromatin contacts of the integrated HHV-6A in latently-infected cells. We show that HHV-6A becomes transcriptionally silent upon infection of these cells over the course of seven days. In addition, we established an HHV-6-specific 4C-seq approach, revealing that the HHV-6A 3D interactome is associated with quiescent chromatin states in cells harboring integrated virus. Furthermore, we observed that the majority of virus chromatin interactions occur toward the distal ends of specific human chromosomes. Exploiting this finding, we established a 4C-seq method that accurately detects the chromosomal integration sites. We further implement long-read minION sequencing in the 4C-seq assay and developed a method to identify HHV-6A/B integration sites in clinical samples.

摘要

人类疱疹病毒-6A 和 6B(HHV-6A/B)可以将其基因组整合到人类染色体的端粒中。病毒整合可以发生在几种细胞类型中,包括生殖细胞,导致个体在其体内的每个细胞中都携带病毒基因组。整合的基因组被有效地沉默,但可以偶尔重新激活,导致各种临床症状。迄今为止,HHV-6A/B 基因的整合机制和随后的沉默仍知之甚少。在这里,我们研究了潜伏感染细胞中整合的 HHV-6A 的全基因组染色质接触。我们表明,在感染这些细胞的过程中,HHV-6A 在七天内转录沉默。此外,我们建立了一种 HHV-6 特异性的 4C-seq 方法,揭示了在携带整合病毒的细胞中,HHV-6A 3D 相互作用组与静止染色质状态相关。此外,我们观察到大多数病毒染色质相互作用发生在特定人类染色体的远端。利用这一发现,我们建立了一种 4C-seq 方法,可以准确检测染色体整合位点。我们进一步在 4C-seq 测定中利用长读长 MinION 测序,并开发了一种在临床样本中识别 HHV-6A/B 整合位点的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6b5e/7953476/58459d32fa6f/fcimb-11-612656-g001.jpg

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