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Study Description

Long Interspsesed Element-1 (LINE1 or L1) encodes two proteins (ORF1p and ORF2p) required for its mobilization (i.e. retrotransposition) in the human genome. Human ORF2p, a 150kDa protein, has endonuclease (EN) and reverse transcriptase (RT) activities. L1 EN is classified as apurinic/apyrimidin-like endonuclease (APE) and is responsible for initiating target-site primer reverse transcription (TPRT) during the L1 retrotransposition cycle. During canonical TPRT, the L1 EN activity makes a single-strand endonucleolytic nick at a double-strand DNA target sequence in genomic DNA. The endonucleolytic nick is typically made at an L1 EN degnerate consensus cleavage sequence (5'-TTTT/A-3') exposing a free 3' hydroxy group that can be used as a primer by the ORF2p L1 RT activity to reverse transcribe the associated L1 RNA. Here, we characterized over 21,000 de novo engineered L1 retrotransposition events in HeLa cells to determine if L1 exhibits overt integration preferences in the human genome. Bru-seq of HeLa cells to determine actively transcribed regions of the genome was also performed. This Bru-seq data was used to determine if engineered L1 integration events preferentially integrate into transcribed regions of the genome, and to determine which strand during transcription may present itself as preferential during L1 retrotransposition.

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Publicly Available Data
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Molecular Data
TypeSourcePlatformNumber of Oligos/SNPsSNP Batch IdComment
Whole Genome Transcriptome Sequencing Illumina HiSeq 2500 N/A N/A
Amplicon Sequencing Pacific Biosciences Single Molecule Real Time Sequencing N/A N/A
Selected Publications
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Study Attribution
  • Principal Investigator
    • Moran, John V. PhD. University of Michigan, Ann Arbor, MI, USA.
  • Co-Investigator
    • Wilson, Thomas E. MD, PhD. University of Michigan, Ann Arbor, MI, USA.
  • Funding Source
    • GM060518. National Institutes of Health, Bethesda, MD, USA.
    • Howard Hughes Medical Institute. Howard Hughes Medical Institute, Chevy Chase, MD, USA.