The Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 Mutations

The Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 Mutations

Show other versions (1)

Noonan syndrome (NS) is one of several autosomal dominant “RASopathies” caused by mutations in components of the RAS-RAF-MEK-ERK MAPK pathway. Germ line mutations in RAF1 (encoding the serine-threonine kinase for MEK1/2) account for ~3-5% of NS, and unlike other NS alleles, RAF1 mutations that confe...

Full description

Bibliographic Details
Main Author: Wu, Xue
Other Authors: Neel, Benjamin
Language:en_ca
Published: 2013
Subjects:
Noonan syndrome
signal transduction
RAS/ERK pathway
mouse model
0307
Online Access:http://hdl.handle.net/1807/65516
id ndltd-TORONTO-oai-tspace.library.utoronto.ca-1807-65516
record_format oai_dc
spelling ndltd-TORONTO-oai-tspace.library.utoronto.ca-1807-655162014-06-24T04:14:21ZThe Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 MutationsWu, XueNoonan syndromesignal transductionRAS/ERK pathwaymouse model0307Noonan syndrome (NS) is one of several autosomal dominant “RASopathies” caused by mutations in components of the RAS-RAF-MEK-ERK MAPK pathway. Germ line mutations in RAF1 (encoding the serine-threonine kinase for MEK1/2) account for ~3-5% of NS, and unlike other NS alleles, RAF1 mutations that confer increased kinase activity are highly associated with hypertrophic cardiomyopathy (HCM). Notably, some NS-associated RAF1 mutations show normal or decreased kinase activity. To explore the pathogenesis of such mutations, I generated “knock-in” mice that express kinase-activating (L613V) or -impaired (D486N) Raf1 mutants, respectively. Knock-in mice expressing the kinase-activated allele Raf1L613V developed typical NS features (short stature, facial dysmorphia, haematological abnormalities), as well as HCM. As expected, agonist-evoked Mek/Erk activation was enhanced in multiple cell types expressing Raf1L613V. Moreover, postnatal Mek inhibition normalized the growth, facial, and cardiac defects in L613V/+ mice, showing that enhanced Mek/Erk activation by Raf1 mutant is critical for evoking NS phenotypes. D486N/+ female mice exhibited a mild growth defect. Male and female D486N/D486N mice developed concentric cardiac hypertrophy and incompletely penetrant, but severe, growth defects. Remarkably, Mek/Erk activation was enhanced in Raf1D486N-expressing cells compared with controls. In both mouse and human cells, RAF1D486N, as well as other kinase-impaired RAF1 mutants, show increased heterodimerization with BRAF, which is necessary and sufficient to promote increased MEK/ERK activation. Furthermore, kinase-activating RAF1 mutants also require heterodimerization to enhance MEK/ERK activation. Our results suggest that increased heterodimerization ability is the common pathogenic mechanism for NS-associated RAF1 mutations.Neel, Benjamin2013-062014-06-20T17:19:12ZNO_RESTRICTION2014-06-20T17:19:12Z2014-06-20Thesishttp://hdl.handle.net/1807/65516en_ca
collection NDLTD
language en_ca
sources NDLTD
topic Noonan syndrome
signal transduction
RAS/ERK pathway
mouse model
0307
spellingShingle Noonan syndrome
signal transduction
RAS/ERK pathway
mouse model
0307
Wu, Xue
The Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 Mutations
description Noonan syndrome (NS) is one of several autosomal dominant “RASopathies” caused by mutations in components of the RAS-RAF-MEK-ERK MAPK pathway. Germ line mutations in RAF1 (encoding the serine-threonine kinase for MEK1/2) account for ~3-5% of NS, and unlike other NS alleles, RAF1 mutations that confer increased kinase activity are highly associated with hypertrophic cardiomyopathy (HCM). Notably, some NS-associated RAF1 mutations show normal or decreased kinase activity. To explore the pathogenesis of such mutations, I generated “knock-in” mice that express kinase-activating (L613V) or -impaired (D486N) Raf1 mutants, respectively. Knock-in mice expressing the kinase-activated allele Raf1L613V developed typical NS features (short stature, facial dysmorphia, haematological abnormalities), as well as HCM. As expected, agonist-evoked Mek/Erk activation was enhanced in multiple cell types expressing Raf1L613V. Moreover, postnatal Mek inhibition normalized the growth, facial, and cardiac defects in L613V/+ mice, showing that enhanced Mek/Erk activation by Raf1 mutant is critical for evoking NS phenotypes. D486N/+ female mice exhibited a mild growth defect. Male and female D486N/D486N mice developed concentric cardiac hypertrophy and incompletely penetrant, but severe, growth defects. Remarkably, Mek/Erk activation was enhanced in Raf1D486N-expressing cells compared with controls. In both mouse and human cells, RAF1D486N, as well as other kinase-impaired RAF1 mutants, show increased heterodimerization with BRAF, which is necessary and sufficient to promote increased MEK/ERK activation. Furthermore, kinase-activating RAF1 mutants also require heterodimerization to enhance MEK/ERK activation. Our results suggest that increased heterodimerization ability is the common pathogenic mechanism for NS-associated RAF1 mutations.
author2 Neel, Benjamin
author_facet Neel, Benjamin
Wu, Xue
author Wu, Xue
author_sort Wu, Xue
title The Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 Mutations
title_short The Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 Mutations
title_full The Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 Mutations
title_fullStr The Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 Mutations
title_full_unstemmed The Molecular Pathogenesis of Noonan Syndrome-Associated RAF1 Mutations
title_sort molecular pathogenesis of noonan syndrome-associated raf1 mutations
publishDate 2013
url http://hdl.handle.net/1807/65516
work_keys_str_mv AT wuxue themolecularpathogenesisofnoonansyndromeassociatedraf1mutations
AT wuxue molecularpathogenesisofnoonansyndromeassociatedraf1mutations
_version_ 1716704755681591296

Similar Items