4.6 Article

Spatial and Genomic Correlates of HIV-1 Integration Site Targeting

期刊

CELLS
卷 11, 期 4, 页码 -

出版社

MDPI
DOI: 10.3390/cells11040655

关键词

HIV; AIDS; retroviral integration; nuclear speckles; speckle-associated domains; lamina-associated domains; LEDGF; p75; CPSF6

资金

  1. US National Institutes of Health [5P30AI060354, R01AI052014]

向作者/读者索取更多资源

HIV-1 integrase and capsid proteins interact with host proteins to direct viral DNA integration into gene-dense regions of the chromosome. Nuclear speckle-associated and speckle-proximal chromatin are strong predictive markers for integration, primarily in gene-dense regions and highly transcribed genes.
HIV-1 integrase and capsid proteins interact with host proteins to direct preintegration complexes to active transcription units within gene-dense regions of chromosomes for viral DNA integration. Analyses of spatially-derived genomic DNA coordinates, such as nuclear speckle-associated domains, lamina-associated domains, super enhancers, and Spatial Position Inference of the Nuclear (SPIN) genome states, have further informed the mechanisms of HIV-1 integration targeting. Critically, however, these different types of genomic coordinates have not been systematically analyzed to synthesize a concise description of the regions of chromatin that HIV-1 prefers for integration. To address this informational gap, we have extensively correlated genomic DNA coordinates of HIV-1 integration targeting preferences. We demonstrate that nuclear speckle-associated and speckle-proximal chromatin are highly predictive markers of integration and that these regions account for known HIV biases for gene-dense regions, highly transcribed genes, as well as the mid-regions of gene bodies. In contrast to a prior report that intronless genes were poorly targeted for integration, we find that intronless genes in proximity to nuclear speckles are more highly targeted than are spatially-matched intron-containing genes. Our results additionally highlight the contributions of capsid and integrase interactions with respective CPSF6 and LEDGF/p75 host factors in these HIV-1 integration targeting preferences.

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