Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 Pathogenic mutations associated with cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy differently affect Jagged1 binding and Notch3 activity via the RBP/JK signaling Pathway.

Literature DB >> 14714274

Pathogenic mutations associated with cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy differently affect Jagged1 binding and Notch3 activity via the RBP/JK signaling Pathway.

Anne Joutel¹, Marie Monet, Valérie Domenga, Florence Riant, Elisabeth Tournier-Lasserve.

Abstract

Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL) is an inherited vascular dementia characterized by the degeneration of smooth-muscle cells in small cerebral arteries. CADASIL is caused by mutations in NOTCH3, one of the four mammalian homologs to the Drosophila melanogaster NOTCH gene. Disease-associated mutations are distributed throughout the 34 epidermal growth factor-like repeats (EGFRs) that compose the extracellular domain of the Notch3 receptor and result in a loss or a gain of a cysteine residue in one of these EGFRs. In human adults, Notch3 expression is highly restricted to vascular smooth-muscle cells. In patients with CADASIL, there is an abnormal accumulation of Notch3 in the vessel. Molecular pathways linking NOTCH3 mutations to degeneration of vascular smooth-muscle cells are as yet poorly understood. In this study, we investigated the effect of CADASIL mutations on Notch3 activity. We studied five naturally occurring mutations: R90C and C212S, located in the previously identified mutational hotspot EGFR2-5; C428S, shown in this study to be located in the ligand-binding domain EGFR10-11; and C542Y and R1006C, located in EGFR13 and EGFR26, respectively. All five mutant proteins were correctly processed. The C428S and C542Y mutant receptors exhibited a significant reduction in Jagged1-induced transcriptional activity of a RBP/JK responsive luciferase reporter, relative to wild-type Notch3. Impaired signaling activity of these two mutants arose through different mechanisms; the C428S mutant lost its Jagged1-binding ability, whereas C542Y retained it but exhibited an impaired presentation to the cell surface. In contrast, the R90C, C212S, and R1006C mutants retained the ability to bind Jagged1 and were associated with apparently normal levels of signaling activity. We conclude that mutations in Notch3 differently affect Jagged1 binding and Notch3 signaling via the RBP/JK pathway.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：

Year: 2004 PMID： 14714274 PMCID： PMC1181931 DOI： 10.1086/381506

Source DB: PubMed Journal: Am J Hum Genet ISSN： 0002-9297 Impact factor: 11.025

33 in total

Review 1. Variations on the Notch pathway in neural development.

Authors: Nicholas J Justice; Yuh Nung Jan
Journal: Curr Opin Neurobiol Date: 2002-02 Impact factor: 6.627

2. CADASIL Notch3 mutant proteins localize to the cell surface and bind ligand.

Authors: Talin Haritunians; Jim Boulter; Carol Hicks; Jonathon Buhrman; Guy DiSibio; Carrie Shawber; Gerry Weinmaster; Donna Nofziger; Carolyn Schanen
Journal: Circ Res Date: 2002-03-22 Impact factor: 17.367

Review 3. Notch and presenilin: a proteolytic mechanism emerges.

Authors: M E Fortini
Journal: Curr Opin Cell Biol Date: 2001-10 Impact factor: 8.382

4. Diagnostic strategies in CADASIL.

Authors: H S Markus; R J Martin; M A Simpson; Y B Dong; N Ali; A H Crosby; J F Powell
Journal: Neurology Date: 2002-10-22 Impact factor: 9.910

5. Skin biopsy immunostaining with a Notch3 monoclonal antibody for CADASIL diagnosis.

Authors: A Joutel; P Favrole; P Labauge; H Chabriat; C Lescoat; F Andreux; V Domenga; M Cécillon; K Vahedi; A Ducros; F Cave-Riant; M G Bousser; E Tournier-Lasserve
Journal: Lancet Date: 2001-12-15 Impact factor: 79.321

6. Vascular expression of Notch pathway receptors and ligands is restricted to arterial vessels.

Authors: N Villa; L Walker; C E Lindsell; J Gasson; M L Iruela-Arispe; G Weinmaster
Journal: Mech Dev Date: 2001-10 Impact factor: 1.882

7. Phenotype of a homozygous CADASIL patient in comparison to 9 age-matched heterozygous patients with the same R133C Notch3 mutation.

Authors: S Tuominen; V Juvonen; K Amberla; T Jolma; J O Rinne; S Tuisku; T Kurki; R Marttila; M Pöyhönen; M L Savontaus; M Viitanen; H Kalimo
Journal: Stroke Date: 2001-08 Impact factor: 7.914

8. A novel proteolytic cleavage involved in Notch signaling: the role of the disintegrin-metalloprotease TACE.

Authors: C Brou; F Logeat; N Gupta; C Bessia; O LeBail; J R Doedens; A Cumano; P Roux; R A Black; A Israël
Journal: Mol Cell Date: 2000-02 Impact factor: 17.970

9. Diagnostic Notch3 sequence analysis in CADASIL: three new mutations in Dutch patients. Dutch CADASIL Research Group.

Authors: S A Oberstein; M D Ferrari; E Bakker; J van Gestel; A L Kneppers; R R Frants; M H Breuning; J Haan
Journal: Neurology Date: 1999-06-10 Impact factor: 9.910

10. C455R notch3 mutation in a Colombian CADASIL kindred with early onset of stroke.

Authors: J F Arboleda-Velasquez; F Lopera; E Lopez; M P Frosch; D Sepulveda-Falla; J E Gutierrez; S Vargas; M Medina; C Martinez De Arrieta; R V Lebo; S A Slaugenhaupt; R A Betensky; A Villegas; M Arcos-Burgos; D Rivera; J C Restrepo; K S Kosik
Journal: Neurology Date: 2002-07-23 Impact factor: 9.910

44 in total

Review 1. Genetic animal models of cerebral vasculopathies.

Authors: Jeong Hyun Lee; Brian J Bacskai; Cenk Ayata
Journal: Prog Mol Biol Transl Sci Date: 2012 Impact factor: 3.622

Review 2. Notch and disease: a growing field.

Authors: Angeliki Louvi; Spyros Artavanis-Tsakonas
Journal: Semin Cell Dev Biol Date: 2012-02-20 Impact factor: 7.727

10. Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy: a genetic cause of cerebral small vessel disease.

Authors: Jay Chol Choi
Journal: J Clin Neurol Date: 2010-03-26 Impact factor: 3.077

Pathogenic mutations associated with cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy differently affect Jagged1 binding and Notch3 activity via the RBP/JK signaling Pathway.

Review 1. Variations on the Notch pathway in neural development.

2. CADASIL Notch3 mutant proteins localize to the cell surface and bind ligand.

Review 3. Notch and presenilin: a proteolytic mechanism emerges.

4. Diagnostic strategies in CADASIL.

5. Skin biopsy immunostaining with a Notch3 monoclonal antibody for CADASIL diagnosis.

6. Vascular expression of Notch pathway receptors and ligands is restricted to arterial vessels.

7. Phenotype of a homozygous CADASIL patient in comparison to 9 age-matched heterozygous patients with the same R133C Notch3 mutation.

8. A novel proteolytic cleavage involved in Notch signaling: the role of the disintegrin-metalloprotease TACE.

9. Diagnostic Notch3 sequence analysis in CADASIL: three new mutations in Dutch patients. Dutch CADASIL Research Group.

10. C455R notch3 mutation in a Colombian CADASIL kindred with early onset of stroke.

Review 1. Genetic animal models of cerebral vasculopathies.

Review 2. Notch and disease: a growing field.

Review 3. CADASIL: experimental insights from animal models.

4. YB-1 acts as a ligand for Notch-3 receptors and modulates receptor activation.

Review 5. An overview of notch signaling in adult tissue renewal and maintenance.

Review 6. Integration of Drosophila and Human Genetics to Understand Notch Signaling Related Diseases.

7. Functional analysis of a recurrent missense mutation in Notch3 in CADASIL.

8. Distinct phenotypic and functional features of CADASIL mutations in the Notch3 ligand binding domain.

9. Notch3 is a major regulator of vascular tone in cerebral and tail resistance arteries.

10. Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy: a genetic cause of cerebral small vessel disease.