Biophysical analysis of a lethal laminin alpha-1 mutation reveals altered self-interaction

Trushar R. Patel; Denise Nikodemus; Tabot M.d. Besong; Raphael Reuten; Markus Meier; Stephen E. Harding; Donald J. Winzor; Manuel Koch; Jörg Stetefeld

doi:10.1016/j.matbio.2015.06.005

Biophysical analysis of a lethal laminin alpha-1 mutation reveals altered self-interaction

Trushar R. Patel, Denise Nikodemus, Tabot M.d. Besong, Raphael Reuten, Markus Meier, Stephen E. Harding, Donald J. Winzor, Manuel Koch, Jörg Stetefeld

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Abstract

Laminins are key basement membrane molecules that influence several biological activities and are linked to a number of diseases. They are secreted as heterotrimeric proteins consisting of one α, one β, and one γ chain, followed by their assembly into a polymer-like sheet at the basement membrane. Using sedimentation velocity, dynamic light scattering, and surface plasmon resonance experiments, we studied self-association of three laminin (LM) N-terminal fragments α-1 (hLM α-1 N), α-5 (hLM α-5 N) and β-3 (hLM β-3 N) originating from the short arms of the human laminin αβγ heterotrimer. Corresponding studies of the hLM α-1 N C49S mutant, equivalent to the larval lethal C56S mutant in zebrafish, have shown that this mutation causes enhanced self-association behavior, an observation that provides a plausible explanation for the inability of laminin bearing this mutation to fulfill functional roles in vivo, and hence for the deleterious pathological consequences of the mutation on lens function.

Original language	English
Journal	Matrix Biology
Early online date	26 Jul 2015
DOIs	https://doi.org/10.1016/j.matbio.2015.06.005
Publication status	E-pub ahead of print - 26 Jul 2015

Keywords

Analytical ultracentrifugation
CD spectroscopy
Dynamic light scattering
Extracellular matrix
Laminin short arms
Protein self-association
Surface plasmon resonance

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.matbio.2015.06.005

Patel_et_al_Biophysical_analysis_lethal_laminin_Matrix_Biology_2015
Eligibility for repository: checked 07/10/2015
Accepted author manuscript, 527 KBLicence: Creative Commons: Attribution-NonCommercial-NoDerivs (CC BY-NC-ND)

http://linkinghub.elsevier.com/retrieve/pii/S0945053X15001237

Cite this

@article{3e891b8dc7ae4e4c9262e451f5dfedfe,

title = "Biophysical analysis of a lethal laminin alpha-1 mutation reveals altered self-interaction",

abstract = "Laminins are key basement membrane molecules that influence several biological activities and are linked to a number of diseases. They are secreted as heterotrimeric proteins consisting of one α, one β, and one γ chain, followed by their assembly into a polymer-like sheet at the basement membrane. Using sedimentation velocity, dynamic light scattering, and surface plasmon resonance experiments, we studied self-association of three laminin (LM) N-terminal fragments α-1 (hLM α-1 N), α-5 (hLM α-5 N) and β-3 (hLM β-3 N) originating from the short arms of the human laminin αβγ heterotrimer. Corresponding studies of the hLM α-1 N C49S mutant, equivalent to the larval lethal C56S mutant in zebrafish, have shown that this mutation causes enhanced self-association behavior, an observation that provides a plausible explanation for the inability of laminin bearing this mutation to fulfill functional roles in vivo, and hence for the deleterious pathological consequences of the mutation on lens function.",

keywords = "Analytical ultracentrifugation, CD spectroscopy, Dynamic light scattering, Extracellular matrix, Laminin short arms, Protein self-association, Surface plasmon resonance",

author = "Patel, {Trushar R.} and Denise Nikodemus and Besong, {Tabot M.d.} and Raphael Reuten and Markus Meier and Harding, {Stephen E.} and Winzor, {Donald J.} and Manuel Koch and J{\"o}rg Stetefeld",

year = "2015",

month = jul,

day = "26",

doi = "10.1016/j.matbio.2015.06.005",

language = "English",

journal = "Matrix Biology",

issn = "0945-053X",

publisher = "Elsevier",

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T1 - Biophysical analysis of a lethal laminin alpha-1 mutation reveals altered self-interaction

AU - Patel, Trushar R.

AU - Nikodemus, Denise

AU - Besong, Tabot M.d.

AU - Reuten, Raphael

AU - Meier, Markus

AU - Harding, Stephen E.

AU - Winzor, Donald J.

AU - Koch, Manuel

AU - Stetefeld, Jörg

PY - 2015/7/26

Y1 - 2015/7/26

N2 - Laminins are key basement membrane molecules that influence several biological activities and are linked to a number of diseases. They are secreted as heterotrimeric proteins consisting of one α, one β, and one γ chain, followed by their assembly into a polymer-like sheet at the basement membrane. Using sedimentation velocity, dynamic light scattering, and surface plasmon resonance experiments, we studied self-association of three laminin (LM) N-terminal fragments α-1 (hLM α-1 N), α-5 (hLM α-5 N) and β-3 (hLM β-3 N) originating from the short arms of the human laminin αβγ heterotrimer. Corresponding studies of the hLM α-1 N C49S mutant, equivalent to the larval lethal C56S mutant in zebrafish, have shown that this mutation causes enhanced self-association behavior, an observation that provides a plausible explanation for the inability of laminin bearing this mutation to fulfill functional roles in vivo, and hence for the deleterious pathological consequences of the mutation on lens function.

AB - Laminins are key basement membrane molecules that influence several biological activities and are linked to a number of diseases. They are secreted as heterotrimeric proteins consisting of one α, one β, and one γ chain, followed by their assembly into a polymer-like sheet at the basement membrane. Using sedimentation velocity, dynamic light scattering, and surface plasmon resonance experiments, we studied self-association of three laminin (LM) N-terminal fragments α-1 (hLM α-1 N), α-5 (hLM α-5 N) and β-3 (hLM β-3 N) originating from the short arms of the human laminin αβγ heterotrimer. Corresponding studies of the hLM α-1 N C49S mutant, equivalent to the larval lethal C56S mutant in zebrafish, have shown that this mutation causes enhanced self-association behavior, an observation that provides a plausible explanation for the inability of laminin bearing this mutation to fulfill functional roles in vivo, and hence for the deleterious pathological consequences of the mutation on lens function.

KW - Analytical ultracentrifugation

KW - CD spectroscopy

KW - Dynamic light scattering

KW - Extracellular matrix

KW - Laminin short arms

KW - Protein self-association

KW - Surface plasmon resonance

U2 - 10.1016/j.matbio.2015.06.005

DO - 10.1016/j.matbio.2015.06.005

M3 - Article

SN - 0945-053X

JO - Matrix Biology

JF - Matrix Biology

ER -

Biophysical analysis of a lethal laminin alpha-1 mutation reveals altered self-interaction

Abstract

Keywords

UN SDGs

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