Involvement of the Same TNFR1 Residue in Mendelian and Multifactorial Inflammatory Disorders

OBJECTIVES: TNFRSF1A is involved in an autosomal dominant autoinflammatory disorder called TNFR-associated periodic syndrome (TRAPS). Most TNFRSF1A mutations are missense changes and, apart from those affecting conserved cysteines, their deleterious effect remains often questionable. This is especia...

Descripción completa

Detalles Bibliográficos
Autores principales: Jéru, Isabelle, Charmion, Serge, Cochet, Emmanuelle, Copin, Bruno, Duquesnoy, Philippe, Garcia, Maria Teresa Mitjavila, Le Borgne, Gaëlle, Cathebras, Pascal, Gaillat, Jacques, Karabina, Sonia, Dodé, Catherine, Lohse, Peter, Hentgen, Véronique, Amselem, Serge
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3722142/
https://www.ncbi.nlm.nih.gov/pubmed/23894535
http://dx.doi.org/10.1371/journal.pone.0069757
_version_ 1782278149704253440
author Jéru, Isabelle
Charmion, Serge
Cochet, Emmanuelle
Copin, Bruno
Duquesnoy, Philippe
Garcia, Maria Teresa Mitjavila
Le Borgne, Gaëlle
Cathebras, Pascal
Gaillat, Jacques
Karabina, Sonia
Dodé, Catherine
Lohse, Peter
Hentgen, Véronique
Amselem, Serge
author_facet Jéru, Isabelle
Charmion, Serge
Cochet, Emmanuelle
Copin, Bruno
Duquesnoy, Philippe
Garcia, Maria Teresa Mitjavila
Le Borgne, Gaëlle
Cathebras, Pascal
Gaillat, Jacques
Karabina, Sonia
Dodé, Catherine
Lohse, Peter
Hentgen, Véronique
Amselem, Serge
author_sort Jéru, Isabelle
collection PubMed
description OBJECTIVES: TNFRSF1A is involved in an autosomal dominant autoinflammatory disorder called TNFR-associated periodic syndrome (TRAPS). Most TNFRSF1A mutations are missense changes and, apart from those affecting conserved cysteines, their deleterious effect remains often questionable. This is especially true for the frequent R92Q mutation, which might not be responsible for TRAPS per se but represents a susceptibility factor to multifactorial inflammatory disorders. This study investigates TRAPS pathophysiology in a family exceptional by its size (13 members) and compares the consequences of several mutations affecting arginine 92. METHODS: TNFRSF1A screening was performed by PCR-sequencing. Comparison of the 3-dimensional structure and electrostatic properties of wild-type and mutated TNFR1 proteins was performed by in silico homology modeling. TNFR1 expression was assessed by FACS analysis, western blotting and ELISA in lysates and supernatants of HEK293T cells transiently expressing wild-type and mutated TNFR1. RESULTS: A TNFRSF1A heterozygous missense mutation, R92W (c.361C>T), was shown to perfectly segregate with typical TRAPS manifestations within the family investigated (p<5.10(−4)). It was associated with very high disease penetrance (0.9). Prediction of its impact on the protein structure revealed local conformational changes and alterations of the receptor electrostatic properties. R92W also impairs the TNFR1 expression at the cell surface and the levels of soluble receptor. Similar results were obtained with R92P, another mutation previously identified in a very small familial form with incomplete penetrance and variable expressivity. In contrast, TNFR1-R92Q behaves like the wild-type receptor. CONCLUSIONS: These data demonstrate the pathogenicity of a mutation affecting arginine 92, a residue whose involvement in inflammatory disorders is deeply debated. Combined with previous reports on arginine 92 mutations, this study discloses an unusual situation in which different amino acid substitutions at the same position in the protein are associated with a clinical spectrum bridging Mendelian to multifactorial conditions.
format Online
Article
Text
id pubmed-3722142
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-37221422013-07-26 Involvement of the Same TNFR1 Residue in Mendelian and Multifactorial Inflammatory Disorders Jéru, Isabelle Charmion, Serge Cochet, Emmanuelle Copin, Bruno Duquesnoy, Philippe Garcia, Maria Teresa Mitjavila Le Borgne, Gaëlle Cathebras, Pascal Gaillat, Jacques Karabina, Sonia Dodé, Catherine Lohse, Peter Hentgen, Véronique Amselem, Serge PLoS One Research Article OBJECTIVES: TNFRSF1A is involved in an autosomal dominant autoinflammatory disorder called TNFR-associated periodic syndrome (TRAPS). Most TNFRSF1A mutations are missense changes and, apart from those affecting conserved cysteines, their deleterious effect remains often questionable. This is especially true for the frequent R92Q mutation, which might not be responsible for TRAPS per se but represents a susceptibility factor to multifactorial inflammatory disorders. This study investigates TRAPS pathophysiology in a family exceptional by its size (13 members) and compares the consequences of several mutations affecting arginine 92. METHODS: TNFRSF1A screening was performed by PCR-sequencing. Comparison of the 3-dimensional structure and electrostatic properties of wild-type and mutated TNFR1 proteins was performed by in silico homology modeling. TNFR1 expression was assessed by FACS analysis, western blotting and ELISA in lysates and supernatants of HEK293T cells transiently expressing wild-type and mutated TNFR1. RESULTS: A TNFRSF1A heterozygous missense mutation, R92W (c.361C>T), was shown to perfectly segregate with typical TRAPS manifestations within the family investigated (p<5.10(−4)). It was associated with very high disease penetrance (0.9). Prediction of its impact on the protein structure revealed local conformational changes and alterations of the receptor electrostatic properties. R92W also impairs the TNFR1 expression at the cell surface and the levels of soluble receptor. Similar results were obtained with R92P, another mutation previously identified in a very small familial form with incomplete penetrance and variable expressivity. In contrast, TNFR1-R92Q behaves like the wild-type receptor. CONCLUSIONS: These data demonstrate the pathogenicity of a mutation affecting arginine 92, a residue whose involvement in inflammatory disorders is deeply debated. Combined with previous reports on arginine 92 mutations, this study discloses an unusual situation in which different amino acid substitutions at the same position in the protein are associated with a clinical spectrum bridging Mendelian to multifactorial conditions. Public Library of Science 2013-07-24 /pmc/articles/PMC3722142/ /pubmed/23894535 http://dx.doi.org/10.1371/journal.pone.0069757 Text en © 2013 Jéru 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Jéru, Isabelle
Charmion, Serge
Cochet, Emmanuelle
Copin, Bruno
Duquesnoy, Philippe
Garcia, Maria Teresa Mitjavila
Le Borgne, Gaëlle
Cathebras, Pascal
Gaillat, Jacques
Karabina, Sonia
Dodé, Catherine
Lohse, Peter
Hentgen, Véronique
Amselem, Serge
Involvement of the Same TNFR1 Residue in Mendelian and Multifactorial Inflammatory Disorders
title Involvement of the Same TNFR1 Residue in Mendelian and Multifactorial Inflammatory Disorders
title_full Involvement of the Same TNFR1 Residue in Mendelian and Multifactorial Inflammatory Disorders
title_fullStr Involvement of the Same TNFR1 Residue in Mendelian and Multifactorial Inflammatory Disorders
title_full_unstemmed Involvement of the Same TNFR1 Residue in Mendelian and Multifactorial Inflammatory Disorders
title_short Involvement of the Same TNFR1 Residue in Mendelian and Multifactorial Inflammatory Disorders
title_sort involvement of the same tnfr1 residue in mendelian and multifactorial inflammatory disorders
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3722142/
https://www.ncbi.nlm.nih.gov/pubmed/23894535
http://dx.doi.org/10.1371/journal.pone.0069757
work_keys_str_mv AT jeruisabelle involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT charmionserge involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT cochetemmanuelle involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT copinbruno involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT duquesnoyphilippe involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT garciamariateresamitjavila involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT leborgnegaelle involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT cathebraspascal involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT gaillatjacques involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT karabinasonia involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT dodecatherine involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT lohsepeter involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT hentgenveronique involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders
AT amselemserge involvementofthesametnfr1residueinmendelianandmultifactorialinflammatorydisorders

Ejemplares similares