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  • Further insights from structural mass spectrometry into endocytosis adaptor protein assemblies.

Further insights from structural mass spectrometry into endocytosis adaptor protein assemblies.

International journal of mass spectrometry (2020-11-28)
Johannes Heidemann, Knut Kölbel, Albert Konijnenberg, Jeroen Van Dyck, Maria Garcia-Alai, Rob Meijers, Frank Sobott, Charlotte Uetrecht
ABSTRACT

As a fundament in many biologically relevant processes, endocytosis in its different guises has been arousing interest for decades and still does so. This is true for the actual transport and its initiation alike. In clathrin-mediated endocytosis, a comparatively well understood endocytic pathway, a set of adaptor proteins bind specific lipids in the plasma membrane, subsequently assemble and thus form a crucial bridge from clathrin to actin for the ongoing process. These adaptor proteins are highly interesting themselves and the subject of this manuscript. Using many of the instruments that are available now in the mass spectrometry toolbox, we added some facets to the picture of how these minimal assemblies may look, how they form, and what influences the structure. Especially, lipids in the adaptor protein complexes result in reduced charging of a normal sized complex due to their specific binding position. The results further support our structural model of a double ring structure with interfacial lipids.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
Alcohol Dehydrogenase from Saccharomyces cerevisiae, ≥300 units/mg protein, lyophilized powder (contains buffer salts), Mw 141-151 kDa
Sigma-Aldrich
Pyruvate Kinase from rabbit muscle, Type III, lyophilized powder, 350-600 units/mg protein
Sigma-Aldrich
Concanavalin A from Canavalia ensiformis (Jack bean), Type IV, lyophilized powder
Sigma-Aldrich
L-Glutamic Dehydrogenase from bovine liver, Type III, lyophilized powder, ≥20 units/mg protein