TY - JOUR
T1 - Polymorphism analysis of the huntingtin gene in italian families affected with huntington disease
AU - Novelletto, Andrea
AU - Persichetti, Francesca
AU - Sabbadini, Guglielmo
AU - Mandich, Paola
AU - Bellone, Emilia
AU - Ajmar, Franco
AU - Squitieri, F.
AU - Campanella, G.
AU - Bozza, Angela
AU - Macdonald, Marcy E.
AU - Gusella, James F.
AU - Frontali, Marina
N1 - Funding Information:
We gratefully acknowledge Prof. L.Terrenato for his continuous support and advice. We also thank Prof. F.Ferro-Milone, Drs G.Bargagli, M.Pavone and F.Perini for providing some of the samples. This work was partially supported by CNR grants 93.00031.PF99 to A.N. and 'Progetto Finalizzato Ingegneria Genetica' to F.A., and by grants of 'Telethon Italia1 to P.M. and A.N.
PY - 1994/7
Y1 - 1994/7
N2 - Two sources of variation in the huntingtin gene, the length of the CCG-rich segment downstream to the (CAG)n stretch undergoing expansion in Huntington disease (HD) and the deletion of 3 bp at codon positions 2642-2645(Δ2642), were analysed on the normal and HD chromosomes of 80 Italian families affected with HD. No instances of meiotic instability of the CCG-rich segment were detected. A strong linkage disequilibrium was found between the HD mutation and alleles at both polymorphic regions: CCG-rich length alleles different from 176 bp are underrepresented while Δ2642 is overrepresented on HD chromosomes. The presence of such alleles on HD chromosomes does not affect age at onset of the disease. Normal chromosomes displayed a non-random association, shorter (CAG)n segments being preferentially followed by longer CCG-rich segments. Finally, the finding, among normal subjects, of carriers of variants on both chromosomes denotes that variation at either of the two polymorphisms does not impair the function of the huntingtin gene product.
AB - Two sources of variation in the huntingtin gene, the length of the CCG-rich segment downstream to the (CAG)n stretch undergoing expansion in Huntington disease (HD) and the deletion of 3 bp at codon positions 2642-2645(Δ2642), were analysed on the normal and HD chromosomes of 80 Italian families affected with HD. No instances of meiotic instability of the CCG-rich segment were detected. A strong linkage disequilibrium was found between the HD mutation and alleles at both polymorphic regions: CCG-rich length alleles different from 176 bp are underrepresented while Δ2642 is overrepresented on HD chromosomes. The presence of such alleles on HD chromosomes does not affect age at onset of the disease. Normal chromosomes displayed a non-random association, shorter (CAG)n segments being preferentially followed by longer CCG-rich segments. Finally, the finding, among normal subjects, of carriers of variants on both chromosomes denotes that variation at either of the two polymorphisms does not impair the function of the huntingtin gene product.
UR - http://www.scopus.com/inward/record.url?scp=0028332346&partnerID=8YFLogxK
U2 - 10.1093/hmg/3.7.1129
DO - 10.1093/hmg/3.7.1129
M3 - Article
SN - 0964-6906
VL - 3
SP - 1129
EP - 1132
JO - Human Molecular Genetics
JF - Human Molecular Genetics
IS - 7
ER -