Molecular analysis and test of linkage between the FMR-I gene and infantile autism in multiplex families

Hallmayer, J; Pintado, E; Lotspeich, L; Spiker, D; Kraemer, H C; Lee Wong, D; Lin, A; Herbert, J; Cavalli-Sforza, L L; Ciaranello, R D

Title: Molecular analysis and test of linkage between the FMR-I gene and infantile autism in multiplex families

Journal Article · Tue Nov 01 00:00:00 EST 1994 · American Journal of Human Genetics

OSTI ID:56843

Hallmayer, J; Pintado, E; Lotspeich, L; Spiker, D; Kraemer, H C; Lee Wong, D; Lin, A; Herbert, J; Cavalli-Sforza, L L; Ciaranello, R D ^[1]

Stanford Univ., CA (United States); and others

Approximately 2%-5% of autistic children show cytogenetic evidence of the fragile X syndrome. This report tests whether infantile autism in multiplex autism families arises from an unusual manifestion of the fragile X syndrome. This could arise either by expansion of the (CGG)n trinucleotide repeat in FMR-1 or from a mutation elsewhere in the gene. We studied 35 families that met stringent criteria for multiplex autism. Amplification of the trinucleotide repeat and analysis of methylation status were performed in 79 autistic children and in 31 of their unaffected siblings by Southern blot analysis. No examples of amplified repeats were seen in the autistic or control children or in their parents or grandparents. We next examined the hypothesis that there was a mutation elsewhere in the FMR-1 gene, by linkage analysis in 32 of these families. We tested four different dominant models and a recessive model. Linkage to FMR-1 could be excluded (lod score between -24 and -62) in all models by using probes DXS548, FRAXAC1, and FRAXAC2 and the CGG repeat itself. Tests for heterogeneity in this sample were negative, and the occurrence of positive lod scores in this data set could be attributed to chance. Analysis of the data by the affected-sib method also did not show evidence for linkage of any marker to autism. These results enable us to reject the hypothesis that multiplex autism arises from expansion of the (CGG)n trinucleotide repeat in FMR-1. Further, because the overall lod scores for all probes in all models tested were highly negative, linkage to FMR-1 can also be ruled out in multiplex autistic families. 35 refs., 2 figs., 5 tabs.

Cite

Export

Save

OSTI ID:: 56843

Journal Information:: American Journal of Human Genetics, Vol. 55, Issue 5; Other Information: PBD: Nov 1994

Country of Publication:: United States

Language:: English

Similar Records

Reverse mutations in fragile X syndrome

Journal Article · Thu Sep 01 00:00:00 EDT 1994 · American Journal of Human Genetics · OSTI ID:56843

Brown, W T; Nolin, S; Houck, G E

Evidence for high-risk haplotypes and (CGG)n expansion in fragile X syndrome in the Hellenic population of Greece and Cyprus

Journal Article · Fri Jul 12 00:00:00 EDT 1996 · American Journal of Medical Genetics · OSTI ID:56843

Syrrou, M; Georgiou, I; Pagoulatos, G

Lack of expansion of triplet repeats in the FMR1, FRAXE, and FRAXF loci in male multiplex families with autism and pervasive developmental disorders

Journal Article · Fri Aug 09 00:00:00 EDT 1996 · American Journal of Medical Genetics · OSTI ID:56843

Holden, J J.A.; Julien-Inalsingh, C; Wing, M

Related Subjects

55 BIOLOGY AND MEDICINE
BASIC STUDIES
HUMAN POPULATIONS
HEREDITARY DISEASES
MENTAL DISORDERS
GENES
GENE MUTATIONS
GENETIC MAPPING
HUMAN X CHROMOSOME
CHROMOSOMAL ABERRATIONS
PHENOTYPE
NUCLEOTIDES
INFANTS
STATISTICAL MODELS

Title: Molecular analysis and test of linkage between the FMR-I gene and infantile autism in multiplex families

Citation Formats

Similar Records

Related Subjects