on May 25, 2006
Published online before print May 25, 2006, doi: 10.1161/01.STR.0000226624.93519.78
| |||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Submitted on January 16, 2006
From the Department of Neurology (T.W., S.H., P.B., M.-L.A., T.B., C.G.-G.), University of Heidelberg, Germany; the Department of Neurology (B.E., O.B.), City Hospital Minden, Germany; the Department of Neurology (A.P.), University of Brescia, Italy; the Department of Dermatology (I.H.), University of Heidelberg, Germany; the Department of Neurology (J.J.M.), Sanatorio Allende, Cordoba, Argentina; the Neurological Clinic and Stroke Unit (S.E., P.L.), University Hospital Basel, Switzerland; and the Department of Neurological Rehabilitation (T.B.), Schmieder-Kliniken Heidelberg, Germany. * To whom correspondence should be addressed. E-mail: Caspar_Grond-Ginsbach{at}med.uni-heidelberg.de.
Background and Purpose--Cervical artery dissections (CAD) can be associated with connective tissue aberrations in skin biopsies. The analysis of healthy relatives of patients suggested that the connective tissue phenotype is familial with an autosomal dominant inheritance. Methods--We performed genetic linkage studies in 3 families of patients with CAD. Connective tissue phenotypes for the patients and all family members were assessed by electron microscopic study of skin biopsies. A genome-wide linkage analysis of 1 family (1 patient with 8 healthy relatives) indicated 2 candidate loci. Three genes were subsequently studied by sequence analysis. Part of the genome was also studied by linkage analysis in 2 further families. Results--The genome-wide scan in a single family suggested linkage between the hypothetical mutation causing the connective tissue phenotype and informative genetic markers on chromosome 15q24 (logarithm of the odds score: Z = +2.1). A second possible candidate locus (Z=+1.9) was found on chromosome 10q26. Sequence analysis of 3 candidate genes in the suggestive locus (chondroitin sulfate proteoglycan4 [CSPG4], lysyl oxidase-like1 [LOXL1] and fibroblast growth factor receptor2 [FGFR2]) did not lead to the identification of a mutation responsible for connective tissue alterations. In 2 additional smaller families the loci on chromosome 15q24 and 10q26 were excluded by linkage analysis. Conclusions--Linkage analysis of a large family with CAD-associated connective tissue alterations suggested the presence of a candidate locus on chromosome 15q2 or on chromosome 10q26. Sequence analysis did not lead to the identification of a mutated candidate gene in 1 of these loci. The study of 2 additional pedigrees indicated locus heterogeneity for the connective tissue phenotype of CAD patients.
Revised on April 11, 2006
Accepted on April 21, 2006
Genetic Analysis of Familial Connective Tissue Alterations Associated With Cervical Artery Dissections Suggests Locus Heterogeneity
Tina Wiest PhD;
Key words: cerebrovascular disorder • cervical artery dissection • genetic linkage analysis
This article has been cited by other articles:
 |
|
 |
|
  S. Debette and H. S. Markus The Genetics of Cervical Artery Dissection: A Systematic Review Stroke, June 1, 2009; 40(6): e459 - e466. [Abstract] [Full Text] [PDF]
|
|
|
|
|
|
J. J. Martin, I. Hausser, P. Lyrer, O. Busse, R. Schwarz, R. Schneider, T. Brandt, M. Kloss, M. Schwaninger, S. Engelter, et al. Familial Cervical Artery Dissections: Clinical, Morphologic, and Genetic Studies Stroke, December 1, 2006; 37(12): 2924 - 2929. [Abstract] [Full Text] [PDF]
|
|