In this Rube Goldberg contraption, leukemic cells are entered at the “Start” arrow, treated with an azanuceloside analog, and emerge as normal neutrophils. Along the way, a variety of epigenetic targets and DNA damage and repair pathways are encountered. Klco et al illustrate that despite state-of-the-art genomic technology, the mechanisms accounting for the clinical activity of DNMT inhibitors in myeloid leukemias remain complex and unclear.

In this Rube Goldberg contraption, leukemic cells are entered at the “Start” arrow, treated with an azanuceloside analog, and emerge as normal neutrophils. Along the way, a variety of epigenetic targets and DNA damage and repair pathways are encountered. Klco et al illustrate that despite state-of-the-art genomic technology, the mechanisms accounting for the clinical activity of DNMT inhibitors in myeloid leukemias remain complex and unclear.

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