Publication | Open Access
Structure-function analysis of the RNA helicase maleless
48
Citations
36
References
2007
Year
Rna Helicase MalelessChromatinDosage Compensation ComplexSystems BiologyChromatin RemodelingProtein FoldingGeneticsX ChromosomeNatural SciencesRna BiologyMolecular BiologyGene RegulationRna Structure PredictionGene ExpressionMedicineStructural BiologyChromatin Function
Loss of function of the RNA helicase maleless (MLE) in Drosophila melanogaster leads to male-specific lethality due to a failure of X chromosome dosage compensation. MLE is presumably involved in incorporating the non-coding roX RNA into the dosage compensation complex (DCC), which is an essential but poorly understood requirement for faithful targeting of the complex to the X chromosome. Sequence comparison predicts several RNA-binding domains in MLE but their properties have not been experimentally verified. We evaluated the RNA-binding characteristics of these conserved motifs and their contributions to RNA-stimulated ATPase activity, to helicase activity, as well as to the targeting of MLE to the nucleus and to the X chromosome territory. We find that RB2 is the dominant, conditional RNA-binding module, which is indispensable for ATPase and helicase activity whereas the N-terminal RB1 motif does not bind RNA, but is involved in targeting MLE to the X chromosome. The C-terminal domain containing a glycine-rich heptad repeat adds potential dimerization and RNA-binding surfaces which are not required for helicase activity.
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