Structural And Biochemical Studies Confirming The Mechanism Of Action Of Asciminib, An Agent Specifically Targeting The Abl Myristoyl Pocket (Stamp)

Peter Schuld,Stephan Grzesiek, Johannes Schlotte, Judith M Habazettl,Wolfgang Jahnke,Louise Barys,Sandra W Cowan-Jacob,Alice Loo, Andrea Wiget,Paul W. Manley

BLOOD(2020)

引用 5|浏览25
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摘要
Tyrosine kinase inhibitors (TKIs) that inhibit the transphosphorylation activity of the BCR-ABL1 oncoprotein by binding the ATP-binding site of the catalytic domain of protein kinases are well established as being effective drugs for the treatments of chronic myeloid leukemia (CML). However, the off-target kinase activities of these non-specific TKIs are associated with adverse events that can limit their suitability for the treatment of patients and can negatively impact quality of life. Therefore, a new drug combining high efficacy with minimal side-effects could provide substantial therapeutic advantages.
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