AI Article Synopsis
- * Researchers created a new series of irreversible menin inhibitors, with compound 37 being the standout candidate, showing selectivity and potency against leukemic cells expressing MLL fusion proteins.
- * Compound 37 works through a unique mechanism by reducing menin protein levels and downregulating its gene transcription, potentially overcoming resistance to current menin inhibitors and demonstrating promising effects in further studies.
Article Abstract
The interaction between menin and MLL1 protein plays an important role in AML with MLL rearrangement and NPM1 mutation. Blocking the formation of menin-MLL complex can inhibit proliferation and induce differentiation in these cancer subtypes. In development of anticancer drugs, irreversible inhibitors are gaining spotlight as they may have better activities than the reversible analogs. Therefore, we designed and developed a novel series of covalent menin inhibitors. Among these compounds, 37 emerges as a selective and potent inhibitor of MLL fusion protein-expressing leukemic cells. The cellular study indicates 37 has a distinct mechanism of action, in both reducing menin protein levels and downregulating MEN1 transcription. This effect of 37 is not involved in proteasomal degradation, and may directly affect the synthesis of menin protein, which offers a significant advantage in addressing acquired resistance to menin inhibitors. Further study showed that compound 37 has prolonged anti-leukemic action and exhibits promising in vivo efficacy, making it a valuable probe for further menin-MLL interaction studies.
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| http://dx.doi.org/10.1016/j.ejmech.2024.116918 | DOI Listing |
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