Monobodies as enabling tools for structural and mechanistic biology

Monobodies, built with the scaffold of the fibronectin type III domain, are among the most well-established synthetic binding proteins. They promote crystallization of challenging molecular systems. They have strong tendency to bind to functional sites and thus serve as drug-like molecules that perturb the biological functions of their targets. Monobodies lack disulfide bonds and thus they are particularly suited as genetically encoded reagents to be used intracellularly. This article reviews recent monobody-enabled studies that reveal new structures, molecular mechanisms and potential therapeutic opportunities. A systematic analysis of the crystal structures of monobody-target complexes suggests important attributes that make monobodies effective crystallization chaperones.

Monobodies as enabling tools for structural and mechanistic biology

Advancing first principle-based molecular dynamics of biological systems with machine learning

Applying Peptide and Protein Synthesis to Study Post-translational Modifications in Epigenetics and Beyond

Scanning Probe Microscopy Characterization of Organic Self-Assembled Monolayers

Scanning Probe Microscopy Characterization of Organic Self-Assembled Monolayers

Applying Peptide and Protein Synthesis to Study Post-translational Modifications in Epigenetics and Beyond

Advancing first principle-based molecular dynamics of biological systems with machine learning