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MLL leukemia induction by genome editing of human CD34+ hematopoietic cells

Blood. 2015; 
Corina Buechele , Erin H. Breese , Dominik Schneidawind , Chiou-Hong Lin , Johan Jeong , Jesus Duque-Afonso , Stephen H. K. Wong , Kevin S. Smith , Robert S. Negrin , Matthew Porteus , Michael L. Cleary
Products/Services Used Details Operation
Gene Synthesis The knock-in DNA templates contained MLL homology arms (∼700 bp) flanking the TALEN cleavage site, fusion partner complementary DNA (cDNA) sequences, an internal ribosomal entry site (IRES), a fluorescent marker gene coding NeonGreen, and a polyA tail (nucleotide sequences provided in supplemental Figure 1, see supplemental Data available at the Blood Web site).22  The constructs were synthesized commercially (GenScript USA Inc). Get A Quote

摘要

Chromosomal rearrangements involving the mixed-lineage leukemia (MLL) gene occur in primary and treatment-related leukemias and confer a poor prognosis. Studies based primarily on mouse models have substantially advanced our understanding of MLL leukemia pathogenesis, but often use supraphysiological oncogene expression with uncertain implications for human leukemia. Genome editing using site-specific nucleases provides a powerful new technology for gene modification to potentially model human disease, however, this approach has not been used to re-create acute leukemia in human cells of origin comparable to disease observed in patients. We applied transcription activator-like effector nuclease–mediated gen... More

关键词

cd34 antigens, genome editing, leukemia, oncogenes, mice, leukemia, acute, transplantation