Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.

Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.

For the development of efficient anti-cancer therapeutics against the HER receptor family it is indispensable to understand the mechanistic model of the HER receptor activation upon ligand binding. Due to its high complexity the binding mode of Heregulin 1 beta (HRG1β) with its receptor HER3 is so f...

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Main Authors: Carmen Peess, Leopold von Proff, Sabine Goller, Karl Andersson, Michael Gerg, Magnus Malmqvist, Birgit Bossenmaier, Michael Schräml
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4319926?pdf=render
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spelling doaj-e2fc1ca19e7f42cc9ebfc36ca9b8d4f92020-11-25T01:01:52ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01102e011687010.1371/journal.pone.0116870Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.Carmen PeessLeopold von ProffSabine GollerKarl AnderssonMichael GergMagnus MalmqvistBirgit BossenmaierMichael SchrämlFor the development of efficient anti-cancer therapeutics against the HER receptor family it is indispensable to understand the mechanistic model of the HER receptor activation upon ligand binding. Due to its high complexity the binding mode of Heregulin 1 beta (HRG1β) with its receptor HER3 is so far not understood. Analysis of the interaction of HRG1β with surface immobilized HER3 extracellular domain by time-resolved Surface Plasmon Resonance (SPR) was so far not interpretable using any regular analysis method as the interaction was highly complex. Here, we show that Interaction Map (IM) made it possible to shed light on this interaction. IM allowed deciphering the rate limiting kinetic contributions from complex SPR sensorgrams and thereby enabling the extraction of discrete kinetic rate components from the apparently heterogeneous interactions. We could resolve details from the complex avidity-driven binding mode of HRG1β with HER3 by using a combination of SPR and IM data. Our findings contribute to the general understanding that a major conformational change of HER3 during its activation is induced by a complex sequential HRG1β docking mode.http://europepmc.org/articles/PMC4319926?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Carmen Peess
Leopold von Proff
Sabine Goller
Karl Andersson
Michael Gerg
Magnus Malmqvist
Birgit Bossenmaier
Michael Schräml
spellingShingle Carmen Peess
Leopold von Proff
Sabine Goller
Karl Andersson
Michael Gerg
Magnus Malmqvist
Birgit Bossenmaier
Michael Schräml
Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.
PLoS ONE
author_facet Carmen Peess
Leopold von Proff
Sabine Goller
Karl Andersson
Michael Gerg
Magnus Malmqvist
Birgit Bossenmaier
Michael Schräml
author_sort Carmen Peess
title Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.
title_short Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.
title_full Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.
title_fullStr Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.
title_full_unstemmed Deciphering the stepwise binding mode of HRG1β to HER3 by surface plasmon resonance and interaction map.
title_sort deciphering the stepwise binding mode of hrg1β to her3 by surface plasmon resonance and interaction map.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description For the development of efficient anti-cancer therapeutics against the HER receptor family it is indispensable to understand the mechanistic model of the HER receptor activation upon ligand binding. Due to its high complexity the binding mode of Heregulin 1 beta (HRG1β) with its receptor HER3 is so far not understood. Analysis of the interaction of HRG1β with surface immobilized HER3 extracellular domain by time-resolved Surface Plasmon Resonance (SPR) was so far not interpretable using any regular analysis method as the interaction was highly complex. Here, we show that Interaction Map (IM) made it possible to shed light on this interaction. IM allowed deciphering the rate limiting kinetic contributions from complex SPR sensorgrams and thereby enabling the extraction of discrete kinetic rate components from the apparently heterogeneous interactions. We could resolve details from the complex avidity-driven binding mode of HRG1β with HER3 by using a combination of SPR and IM data. Our findings contribute to the general understanding that a major conformational change of HER3 during its activation is induced by a complex sequential HRG1β docking mode.
url http://europepmc.org/articles/PMC4319926?pdf=render
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