Genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen

BACKGROUND: The phenotypic heterogeneity of sickle cell disease is likely the result of multiple genetic factors and their interaction with the sickle mutation. High transcranial doppler (TCD) velocities define a subgroup of children with sickle cell disease who are at increased risk for developing...

Descripción completa

Detalles Bibliográficos
Autores principales: Adams, Gaye T, Snieder, Harold, McKie, Virgil C, Clair, Betsy, Brambilla, Donald, Adams, Robert J, Kutlar, Ferdane, Kutlar, Abdullah
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2003
Materias:
Study Protocol
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC183831/
https://www.ncbi.nlm.nih.gov/pubmed/12871600
http://dx.doi.org/10.1186/1471-2350-4-6
_version_ 1782120878050377728
author Adams, Gaye T
Snieder, Harold
McKie, Virgil C
Clair, Betsy
Brambilla, Donald
Adams, Robert J
Kutlar, Ferdane
Kutlar, Abdullah
author_facet Adams, Gaye T
Snieder, Harold
McKie, Virgil C
Clair, Betsy
Brambilla, Donald
Adams, Robert J
Kutlar, Ferdane
Kutlar, Abdullah
author_sort Adams, Gaye T
collection PubMed
description BACKGROUND: The phenotypic heterogeneity of sickle cell disease is likely the result of multiple genetic factors and their interaction with the sickle mutation. High transcranial doppler (TCD) velocities define a subgroup of children with sickle cell disease who are at increased risk for developing ischemic stroke. The genetic factors leading to the development of a high TCD velocity (i.e. cerebrovascular disease) and ultimately to stroke are not well characterized. METHODS: We have designed a case-control association study to elucidate the role of genetic polymorphisms as risk factors for cerebrovascular disease as measured by a high TCD velocity in children with sickle cell disease. The study will consist of two parts: a candidate gene study and a genomewide screen and will be performed in 230 cases and 400 controls. Cases will include 130 patients (TCD ≥ 200 cm/s) randomized in the Stroke Prevention Trial in Sickle Cell Anemia (STOP) study as well as 100 other patients found to have high TCD in STOP II screening. Four hundred sickle cell disease patients with a normal TCD velocity (TCD < 170 cm/s) will be controls. The candidate gene study will involve the analysis of 28 genetic polymorphisms in 20 candidate genes. The polymorphisms include mutations in coagulation factor genes (Factor V, Prothrombin, Fibrinogen, Factor VII, Factor XIII, PAI-1), platelet activation/function (GpIIb/IIIa, GpIb IX-V, GpIa/IIa), vascular reactivity (ACE), endothelial cell function (MTHFR, thrombomodulin, VCAM-1, E-Selectin, L-Selectin, P-Selectin, ICAM-1), inflammation (TNFα), lipid metabolism (Apo A1, Apo E), and cell adhesion (VCAM-1, E-Selectin, L-Selectin, P-Selectin, ICAM-1). We will perform a genomewide screen of validated single nucleotide polymorphisms (SNPs) in pooled DNA samples from 230 cases and 400 controls to study the possible association of additional polymorphisms with the high-risk phenotype. High-throughput SNP genotyping will be performed through MALDI-TOF technology using Sequenom's MassARRAY™ system. DISCUSSION: It is expected that this study will yield important information on genetic risk factors for the cerebrovascular disease phenotype in sickle cell disease by clarifying the role of candidate genes in the development of high TCD. The genomewide screen for a large number of SNPs may uncover the association of novel polymorphisms with cerebrovascular disease and stroke in sickle cell disease.
format Text
id pubmed-183831
institution National Center for Biotechnology Information
language English
publishDate 2003
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-1838312003-08-27 Genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen Adams, Gaye T Snieder, Harold McKie, Virgil C Clair, Betsy Brambilla, Donald Adams, Robert J Kutlar, Ferdane Kutlar, Abdullah BMC Med Genet Study Protocol BACKGROUND: The phenotypic heterogeneity of sickle cell disease is likely the result of multiple genetic factors and their interaction with the sickle mutation. High transcranial doppler (TCD) velocities define a subgroup of children with sickle cell disease who are at increased risk for developing ischemic stroke. The genetic factors leading to the development of a high TCD velocity (i.e. cerebrovascular disease) and ultimately to stroke are not well characterized. METHODS: We have designed a case-control association study to elucidate the role of genetic polymorphisms as risk factors for cerebrovascular disease as measured by a high TCD velocity in children with sickle cell disease. The study will consist of two parts: a candidate gene study and a genomewide screen and will be performed in 230 cases and 400 controls. Cases will include 130 patients (TCD ≥ 200 cm/s) randomized in the Stroke Prevention Trial in Sickle Cell Anemia (STOP) study as well as 100 other patients found to have high TCD in STOP II screening. Four hundred sickle cell disease patients with a normal TCD velocity (TCD < 170 cm/s) will be controls. The candidate gene study will involve the analysis of 28 genetic polymorphisms in 20 candidate genes. The polymorphisms include mutations in coagulation factor genes (Factor V, Prothrombin, Fibrinogen, Factor VII, Factor XIII, PAI-1), platelet activation/function (GpIIb/IIIa, GpIb IX-V, GpIa/IIa), vascular reactivity (ACE), endothelial cell function (MTHFR, thrombomodulin, VCAM-1, E-Selectin, L-Selectin, P-Selectin, ICAM-1), inflammation (TNFα), lipid metabolism (Apo A1, Apo E), and cell adhesion (VCAM-1, E-Selectin, L-Selectin, P-Selectin, ICAM-1). We will perform a genomewide screen of validated single nucleotide polymorphisms (SNPs) in pooled DNA samples from 230 cases and 400 controls to study the possible association of additional polymorphisms with the high-risk phenotype. High-throughput SNP genotyping will be performed through MALDI-TOF technology using Sequenom's MassARRAY™ system. DISCUSSION: It is expected that this study will yield important information on genetic risk factors for the cerebrovascular disease phenotype in sickle cell disease by clarifying the role of candidate genes in the development of high TCD. The genomewide screen for a large number of SNPs may uncover the association of novel polymorphisms with cerebrovascular disease and stroke in sickle cell disease. BioMed Central 2003-07-18 /pmc/articles/PMC183831/ /pubmed/12871600 http://dx.doi.org/10.1186/1471-2350-4-6 Text en Copyright © 2003 Adams et al; licensee BioMed Central Ltd. This is an Open Access article: verbatim copying and redistribution of this article are permitted in all media for any purpose, provided this notice is preserved along with the article's original URL.
spellingShingle Study Protocol
Adams, Gaye T
Snieder, Harold
McKie, Virgil C
Clair, Betsy
Brambilla, Donald
Adams, Robert J
Kutlar, Ferdane
Kutlar, Abdullah
Genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen
title Genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen
title_full Genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen
title_fullStr Genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen
title_full_unstemmed Genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen
title_short Genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen
title_sort genetic risk factors for cerebrovascular disease in children with sickle cell disease: design of a case-control association study and genomewide screen
topic Study Protocol
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC183831/
https://www.ncbi.nlm.nih.gov/pubmed/12871600
http://dx.doi.org/10.1186/1471-2350-4-6
work_keys_str_mv AT adamsgayet geneticriskfactorsforcerebrovasculardiseaseinchildrenwithsicklecelldiseasedesignofacasecontrolassociationstudyandgenomewidescreen
AT sniederharold geneticriskfactorsforcerebrovasculardiseaseinchildrenwithsicklecelldiseasedesignofacasecontrolassociationstudyandgenomewidescreen
AT mckievirgilc geneticriskfactorsforcerebrovasculardiseaseinchildrenwithsicklecelldiseasedesignofacasecontrolassociationstudyandgenomewidescreen
AT clairbetsy geneticriskfactorsforcerebrovasculardiseaseinchildrenwithsicklecelldiseasedesignofacasecontrolassociationstudyandgenomewidescreen
AT brambilladonald geneticriskfactorsforcerebrovasculardiseaseinchildrenwithsicklecelldiseasedesignofacasecontrolassociationstudyandgenomewidescreen
AT adamsrobertj geneticriskfactorsforcerebrovasculardiseaseinchildrenwithsicklecelldiseasedesignofacasecontrolassociationstudyandgenomewidescreen
AT kutlarferdane geneticriskfactorsforcerebrovasculardiseaseinchildrenwithsicklecelldiseasedesignofacasecontrolassociationstudyandgenomewidescreen
AT kutlarabdullah geneticriskfactorsforcerebrovasculardiseaseinchildrenwithsicklecelldiseasedesignofacasecontrolassociationstudyandgenomewidescreen

Ejemplares similares