Advancing multimer analysis of von Willebrand factor by single-molecule AFM imaging

The formation of hemostatic plugs at sites of vascular injury crucially involves the multimeric glycoprotein von Willebrand factor (VWF). VWF multimers are linear chains of N-terminally linked dimers. The latter are formed from monomers via formation of the C-terminal disulfide bonds Cys2771-Cys2773...

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Autores principales: Löf, Achim, König, Gesa, Schneppenheim, Sonja, Schneppenheim, Reinhard, Benoit, Martin, Budde, Ulrich, Müller, Jochen P., Brehm, Maria A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6333368/
https://www.ncbi.nlm.nih.gov/pubmed/30645640
http://dx.doi.org/10.1371/journal.pone.0210963
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author Löf, Achim
König, Gesa
Schneppenheim, Sonja
Schneppenheim, Reinhard
Benoit, Martin
Budde, Ulrich
Müller, Jochen P.
Brehm, Maria A.
author_facet Löf, Achim
König, Gesa
Schneppenheim, Sonja
Schneppenheim, Reinhard
Benoit, Martin
Budde, Ulrich
Müller, Jochen P.
Brehm, Maria A.
author_sort Löf, Achim
collection PubMed
description The formation of hemostatic plugs at sites of vascular injury crucially involves the multimeric glycoprotein von Willebrand factor (VWF). VWF multimers are linear chains of N-terminally linked dimers. The latter are formed from monomers via formation of the C-terminal disulfide bonds Cys2771-Cys2773’, Cys2773-Cys2771’, and Cys2811-Cys2811’. Mutations in VWF that impair multimerization can lead to subtype 2A of the bleeding disorder von Willebrand Disease (VWD). Commonly, the multimer size distribution of VWF is assessed by electrophoretic multimer analysis. Here, we present atomic force microscopy (AFM) imaging as a method to determine the size distribution of VWF variants by direct visualization at the single-molecule level. We first validated our approach by investigating recombinant wildtype VWF and a previously studied mutant (p.Cys1099Tyr) that impairs N-terminal multimerization. We obtained excellent quantitative agreement with results from earlier studies and with electrophoretic multimer analysis. We then imaged specific mutants that are known to exhibit disturbed C-terminal dimerization. For the mutants p.Cys2771Arg and p.Cys2773Arg, we found the majority of monomers (87 ± 5% and 73 ± 4%, respectively) not to be C-terminally dimerized. While these results confirm that Cys2771 and Cys2773 are crucial for dimerization, they additionally provide quantitative information on the mutants’ different abilities to form alternative C-terminal disulfides for residual dimerization. We further mutated Cys2811 to Ala and found that only 23 ± 3% of monomers are not C-terminally dimerized, indicating that Cys2811 is structurally less important for dimerization. Furthermore, for mutants p.Cys2771Arg, p.Cys2773Arg, and p.Cys2811Ala we found ‘even-numbered’ non-native multimers, i.e. multimers with monomers attached on both termini; a multimer species that cannot be distinguished from native multimers by conventional multimer analysis. Summarizing, we demonstrate that AFM imaging can provide unique insights into VWF processing defects at the single-molecule level that cannot be gained from established methods of multimer analysis.
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spelling pubmed-63333682019-01-31 Advancing multimer analysis of von Willebrand factor by single-molecule AFM imaging Löf, Achim König, Gesa Schneppenheim, Sonja Schneppenheim, Reinhard Benoit, Martin Budde, Ulrich Müller, Jochen P. Brehm, Maria A. PLoS One Research Article The formation of hemostatic plugs at sites of vascular injury crucially involves the multimeric glycoprotein von Willebrand factor (VWF). VWF multimers are linear chains of N-terminally linked dimers. The latter are formed from monomers via formation of the C-terminal disulfide bonds Cys2771-Cys2773’, Cys2773-Cys2771’, and Cys2811-Cys2811’. Mutations in VWF that impair multimerization can lead to subtype 2A of the bleeding disorder von Willebrand Disease (VWD). Commonly, the multimer size distribution of VWF is assessed by electrophoretic multimer analysis. Here, we present atomic force microscopy (AFM) imaging as a method to determine the size distribution of VWF variants by direct visualization at the single-molecule level. We first validated our approach by investigating recombinant wildtype VWF and a previously studied mutant (p.Cys1099Tyr) that impairs N-terminal multimerization. We obtained excellent quantitative agreement with results from earlier studies and with electrophoretic multimer analysis. We then imaged specific mutants that are known to exhibit disturbed C-terminal dimerization. For the mutants p.Cys2771Arg and p.Cys2773Arg, we found the majority of monomers (87 ± 5% and 73 ± 4%, respectively) not to be C-terminally dimerized. While these results confirm that Cys2771 and Cys2773 are crucial for dimerization, they additionally provide quantitative information on the mutants’ different abilities to form alternative C-terminal disulfides for residual dimerization. We further mutated Cys2811 to Ala and found that only 23 ± 3% of monomers are not C-terminally dimerized, indicating that Cys2811 is structurally less important for dimerization. Furthermore, for mutants p.Cys2771Arg, p.Cys2773Arg, and p.Cys2811Ala we found ‘even-numbered’ non-native multimers, i.e. multimers with monomers attached on both termini; a multimer species that cannot be distinguished from native multimers by conventional multimer analysis. Summarizing, we demonstrate that AFM imaging can provide unique insights into VWF processing defects at the single-molecule level that cannot be gained from established methods of multimer analysis. Public Library of Science 2019-01-15 /pmc/articles/PMC6333368/ /pubmed/30645640 http://dx.doi.org/10.1371/journal.pone.0210963 Text en © 2019 Löf et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Löf, Achim
König, Gesa
Schneppenheim, Sonja
Schneppenheim, Reinhard
Benoit, Martin
Budde, Ulrich
Müller, Jochen P.
Brehm, Maria A.
Advancing multimer analysis of von Willebrand factor by single-molecule AFM imaging
title Advancing multimer analysis of von Willebrand factor by single-molecule AFM imaging
title_full Advancing multimer analysis of von Willebrand factor by single-molecule AFM imaging
title_fullStr Advancing multimer analysis of von Willebrand factor by single-molecule AFM imaging
title_full_unstemmed Advancing multimer analysis of von Willebrand factor by single-molecule AFM imaging
title_short Advancing multimer analysis of von Willebrand factor by single-molecule AFM imaging
title_sort advancing multimer analysis of von willebrand factor by single-molecule afm imaging
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6333368/
https://www.ncbi.nlm.nih.gov/pubmed/30645640
http://dx.doi.org/10.1371/journal.pone.0210963
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