Publications by authors named "Jared R Stees"

Super-enhancers (SEs) mediate high transcription levels of target genes. Previous studies have shown that SEs recruit transcription complexes and generate enhancer RNAs (eRNAs). We characterized transcription at the human and murine β-globin locus control region (LCR) SE.

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Zinc finger proteins are the most common among families of DNA-binding transcription factors. Designer transcription factors generated by the fusion of engineered zinc finger DNA-binding domains (ZF-DBDs) to effector domains have been valuable tools for the modulation of gene expression and for targeted genome editing. However, ZF-DBDs without effector domains have also been shown to effectively modulate gene expression by competing with sequence-specific DNA-binding transcription factors.

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Reactivation of γ-globin expression has been shown to ameliorate disease phenotypes associated with mutations in the adult β-globin gene, including sickle cell disease. Specific mutations in the promoter of the γ-globin genes are known to prevent repression of the genes in the adult and thus lead to hereditary persistence of fetal hemoglobin. One such hereditary persistence of fetal hemoglobin is associated with a sequence located 567 bp upstream of the Gγ-globin gene which assembles a GATA-containing repressor complex.

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Article Synopsis
  • Enhancers and promoters help regulate RNA polymerase activity by forming stable protein complexes, known as enhanceosomes, at specific gene loci.
  • Research on the mouse β-globin gene locus using the MAPit method revealed that a specific DNA element (MARE) shows high occupancy during the differentiation of certain cells, indicating strong binding of proteins in that region.
  • Targeting an artificial DNA-binding domain to this MARE site reduced binding of proteins necessary for transcription, underscoring its role in recruiting transcription complexes during cell differentiation, without impacting other globin genes.
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