Abstract
CRM1 is a nuclear export receptor that has been intensively targeted over the last decade for the development of antitumor and antiviral drugs. Structural analysis of several inhibitor compounds bound to CRM1 revealed that their mechanism of action relies on the covalent modification of a critical cysteine residue (Cys528 in the human receptor) located in the nuclear export signal-binding cleft. This study presents the crystal structure of human CRM1, covalently modified by 2-mercaptoethanol on Cys528, in complex with RanGTP at 2.58Å resolution. The results demonstrate that buffer components can interfere with the characterization of cysteine-dependent inhibitor compounds.
Author supplied keywords
Cite
CITATION STYLE
Shaikhqasem, A., Schmitt, K., Valeriusb, O., & Ficnera, R. (2021). Crystal structure of human CRM1, covalently modified by 2-mercaptoethanol on Cys528, in complex with RanGTP. Acta Crystallographica Section F: Structural Biology Communications, 77, 70–78. https://doi.org/10.1107/S2053230X2100203X
Register to see more suggestions
Mendeley helps you to discover research relevant for your work.
