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Structural Dynamics Associated with Intermediate Formation in an Archetypal Conformational Disease

In conformational diseases, native protein conformers convert to pathological intermediates that polymerize. Structural characterization of these key intermediates is challenging. They are unstable and minimally populated in dynamic equilibria that may be perturbed by many analytical techniques. We...

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Autores principales: Nyon, Mun Peak, Segu, Lakshmi, Cabrita, Lisa D., Lévy, Géraldine R., Kirkpatrick, John, Roussel, Benoit D., Patschull, Anathe O.M., Barrett, Tracey E., Ekeowa, Ugo I., Kerr, Richard, Waudby, Christopher A., Kalsheker, Noor, Hill, Marian, Thalassinos, Konstantinos, Lomas, David A., Christodoulou, John, Gooptu, Bibek
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3314904/
https://www.ncbi.nlm.nih.gov/pubmed/22405009
http://dx.doi.org/10.1016/j.str.2012.01.012
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author Nyon, Mun Peak
Segu, Lakshmi
Cabrita, Lisa D.
Lévy, Géraldine R.
Kirkpatrick, John
Roussel, Benoit D.
Patschull, Anathe O.M.
Barrett, Tracey E.
Ekeowa, Ugo I.
Kerr, Richard
Waudby, Christopher A.
Kalsheker, Noor
Hill, Marian
Thalassinos, Konstantinos
Lomas, David A.
Christodoulou, John
Gooptu, Bibek
author_facet Nyon, Mun Peak
Segu, Lakshmi
Cabrita, Lisa D.
Lévy, Géraldine R.
Kirkpatrick, John
Roussel, Benoit D.
Patschull, Anathe O.M.
Barrett, Tracey E.
Ekeowa, Ugo I.
Kerr, Richard
Waudby, Christopher A.
Kalsheker, Noor
Hill, Marian
Thalassinos, Konstantinos
Lomas, David A.
Christodoulou, John
Gooptu, Bibek
author_sort Nyon, Mun Peak
collection PubMed
description In conformational diseases, native protein conformers convert to pathological intermediates that polymerize. Structural characterization of these key intermediates is challenging. They are unstable and minimally populated in dynamic equilibria that may be perturbed by many analytical techniques. We have characterized a forme fruste deficiency variant of α(1)-antitrypsin (Lys154Asn) that forms polymers recapitulating the conformer-specific neo-epitope observed in polymers that form in vivo. Lys154Asn α(1)-antitrypsin populates an intermediate ensemble along the polymerization pathway at physiological temperatures. Nuclear magnetic resonance spectroscopy was used to report the structural and dynamic changes associated with this. Our data highlight an interaction network likely to regulate conformational change and do not support the recent contention that the disease-relevant intermediate is substantially unfolded. Conformational disease intermediates may best be defined using powerful but minimally perturbing techniques, mild disease mutants, and physiological conditions.
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spelling pubmed-33149042012-04-11 Structural Dynamics Associated with Intermediate Formation in an Archetypal Conformational Disease Nyon, Mun Peak Segu, Lakshmi Cabrita, Lisa D. Lévy, Géraldine R. Kirkpatrick, John Roussel, Benoit D. Patschull, Anathe O.M. Barrett, Tracey E. Ekeowa, Ugo I. Kerr, Richard Waudby, Christopher A. Kalsheker, Noor Hill, Marian Thalassinos, Konstantinos Lomas, David A. Christodoulou, John Gooptu, Bibek Structure Article In conformational diseases, native protein conformers convert to pathological intermediates that polymerize. Structural characterization of these key intermediates is challenging. They are unstable and minimally populated in dynamic equilibria that may be perturbed by many analytical techniques. We have characterized a forme fruste deficiency variant of α(1)-antitrypsin (Lys154Asn) that forms polymers recapitulating the conformer-specific neo-epitope observed in polymers that form in vivo. Lys154Asn α(1)-antitrypsin populates an intermediate ensemble along the polymerization pathway at physiological temperatures. Nuclear magnetic resonance spectroscopy was used to report the structural and dynamic changes associated with this. Our data highlight an interaction network likely to regulate conformational change and do not support the recent contention that the disease-relevant intermediate is substantially unfolded. Conformational disease intermediates may best be defined using powerful but minimally perturbing techniques, mild disease mutants, and physiological conditions. Cell Press 2012-03-07 /pmc/articles/PMC3314904/ /pubmed/22405009 http://dx.doi.org/10.1016/j.str.2012.01.012 Text en © 2012 ELL & Excerpta Medica. https://creativecommons.org/licenses/by/3.0/ Open Access under CC BY 3.0 (https://creativecommons.org/licenses/by/3.0/) license
spellingShingle Article
Nyon, Mun Peak
Segu, Lakshmi
Cabrita, Lisa D.
Lévy, Géraldine R.
Kirkpatrick, John
Roussel, Benoit D.
Patschull, Anathe O.M.
Barrett, Tracey E.
Ekeowa, Ugo I.
Kerr, Richard
Waudby, Christopher A.
Kalsheker, Noor
Hill, Marian
Thalassinos, Konstantinos
Lomas, David A.
Christodoulou, John
Gooptu, Bibek
Structural Dynamics Associated with Intermediate Formation in an Archetypal Conformational Disease
title Structural Dynamics Associated with Intermediate Formation in an Archetypal Conformational Disease
title_full Structural Dynamics Associated with Intermediate Formation in an Archetypal Conformational Disease
title_fullStr Structural Dynamics Associated with Intermediate Formation in an Archetypal Conformational Disease
title_full_unstemmed Structural Dynamics Associated with Intermediate Formation in an Archetypal Conformational Disease
title_short Structural Dynamics Associated with Intermediate Formation in an Archetypal Conformational Disease
title_sort structural dynamics associated with intermediate formation in an archetypal conformational disease
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3314904/
https://www.ncbi.nlm.nih.gov/pubmed/22405009
http://dx.doi.org/10.1016/j.str.2012.01.012
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