Cryptic Extensibility in von Willebrand Factor Revealed by Molecular Nanodissection

Author:

Csányi Mária Csilla1,Sziklai Dominik1ORCID,Feller Tímea2,Hársfalvi Jolán1,Kellermayer Miklós13

Affiliation:

1. Institute of Biophysics and Radiation Biology, Semmelweis University, Tűzoltó u. 37-47, H1094 Budapest, Hungary

2. Discovery and Translational Science Department, Leeds Institute of Cardiovascular and Metabolic Medicine, University of Leeds, Leeds LS29JT, UK

3. HUNREN-SE Biophysical Virology Group, Tűzoltó Str. 37-47, H1094 Budapest, Hungary

Abstract

Von Willebrand factor (VWF) is a multimer with a variable number of protomers, each of which is a head-to-head dimer of two multi-domain monomers. VWF responds to shear through the unfolding and extension of distinct domains, thereby mediating platelet adhesion and aggregation to the injured blood vessel wall. VWF's C1-6 segment uncoils and then the A2 domain unfolds and extends in a hierarchical and sequential manner. However, it is unclear whether there is any reservoir of further extensibility. Here, we explored the presence of cryptic extensibility in VWF by nanodissecting individual, pre-stretched multimers with atomic force microscopy (AFM). The AFM cantilever tip was pressed into the surface and moved in a direction perpendicular to the VWF axis. It was possible to pull out protein loops from VWF, which resulted in a mean contour length gain of 217 nm. In some cases, the loop became cleaved, and a gap was present along the contour. Frequently, small nodules appeared in the loops, indicating that parts of the nanodissected VWF segment remained folded. After analyzing the nodal structure, we conclude that the cryptic extensibility lies within the C1-6 and A1-3 regions. Cryptic extensibility may play a role in maintaining VWF’s functionality in extreme shear conditions.

Funder

Hungarian National Research, Development and Innovation Office

European Union

Publisher

MDPI AG

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