4.8 Article

Evolutionary Epigenomics of Retrotransposon-Mediated Methylation Spreading in Rice

期刊

MOLECULAR BIOLOGY AND EVOLUTION
卷 35, 期 2, 页码 365-382

出版社

OXFORD UNIV PRESS
DOI: 10.1093/molbev/msx284

关键词

retrotransposon; epigenomics; transposable element; Oryza sativa

资金

  1. National Science Foundation Plant Genome Research Program [IOS-1546218]
  2. Zegar Family Foundation [A16-0051]
  3. NYU Abu Dhabi Research Institute [G1205]
  4. New York University-High Performance Computing
  5. Division Of Integrative Organismal Systems
  6. Direct For Biological Sciences [1546218] Funding Source: National Science Foundation

向作者/读者索取更多资源

Plant genomes contain numerous transposable elements (TEs), and many hypotheses on the evolutionary drivers that restrict TE activity have been postulated. Few models, however, have focused on the evolutionary epigenomic interaction between the plant host and its TE. The host genome recruits epigenetic factors, such as methylation, to silence TEs but methylation can spread beyond the TE sequence and influence the expression of nearby host genes. In this study, we investigated this epigenetic trade-off between TE and proximal host gene silencing by studying the epigenomic regulation of repressing long terminal repeat (LTR) retrotransposons (RTs) in Oryza sativa. Results showed significant evidence of methylation spreading originating from the LTR-RT sequences, and the extent of spreading was dependent on five factors: 1) LTR-RT family, 2) time since the LTR-RT insertion, 3) recombination rate of the LTR-RT region, 4) level of LTR-RT sequence methylation, and 5) chromosomal location. Methylation spreading had negative effects by reducing host gene expression, but only on host genes with LTR-RT inserted in its introns. Our results also suggested high levels of LTR-RT methylationmight have a role in suppressing TE-mediated deleterious ectopic recombination. In the end, despite the methylation spreading, no strong epigenetic trade-off was detected and majority of LTR-RT may have only minor epigenetic effects on nearby host genes.

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