AI Article Synopsis

  • The study investigates how γ-retrovirus vectors with long terminal repeats (LTRs) can activate oncogenes and contribute to leukemia in gene therapy, emphasizing the importance of understanding the molecular components of LTRs for safer gene transfer.
  • The research focuses on the negative control region (NCR) of the LTR, which is conserved among mammalian γ-retroviruses and is believed to influence gene transcription and potentially oncogenesis in hematopoietic cells.
  • Findings from in vitro assays indicate that the NCR is essential for immortalization of murine bone marrow cells, suggesting that targeted research on the NCR could help better understand its role in insertional oncogenesis linked to γ-retroviral vectors.

Article Abstract

Integrating vectors based on γ-retroviruses and containing full-length long terminal repeats (LTRs) have been associated with activation of oncogene expression and leukemogenesis in human gene therapy trials. Identification of the specific molecular elements of the LTRs that have a role in insertional oncogenesis events is important as it can lead to the development of safer gene transfer vectors. The negative control region (NCR) of the LTR is a particularly well-conserved sequence among mammalian γ-retroviruses with demonstrated regulatory activity of gene transcription in hematopoietic cells, which led us to hypothesize that this region may have a role in insertional oncogenesis after γ-retroviral vector (GV)-mediated gene transfer into hematopoietic progenitors. We used an in vitro assay of murine bone marrow cell immortalization to compare the immortalization capabilities of a series of GVs carrying murine leukemia virus (MLV) LTR deletion mutants. Compared with GV carrying the full-length MLV LTR, deletion of the complete LTR enhancer sequence showed significant reduction of immortalization rates. However, the use of a mutant LTR deleted of the enhancer sequence, with exception of the NCR, did not affect immortalization. Importantly, the inclusion of an LTR mutant devoid only of the NCR did show significant reduction of immortalization rates compared with the full LTR sequence. Therefore, our data point to the NCR as a key element for immortalization and justify additional studies to evaluate its specific role in MLV-mediated insertional oncogenesis.

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http://dx.doi.org/10.1038/gt.2016.51DOI Listing

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