Molecular analysis of 53 fragile X families with the probe StB12.3

Puissant, H; Malinge, M C; Larget-Piet, A; Larget-Piet, L; Martin, D; Chauveau, P; Odent, S; Lemarec, B; Plessis, G; Parent, Ph

doi:10.1002/ajmg.1320530413

Title: Molecular analysis of 53 fragile X families with the probe StB12.3

Journal Article · Thu Dec 01 00:00:00 EST 1994 · American Journal of Medical Genetics

DOI:https://doi.org/10.1002/ajmg.1320530413· OSTI ID:61998

Puissant, H; Malinge, M C; Larget-Piet, A; Larget-Piet, L ^[1]; Martin, D ^[2]; Chauveau, P ^[3]; Odent, S; Lemarec, B ^[4]; Plessis, G ^[5]; Parent, Ph ^[6]

Unite de Genetique CHU d`Angers (France)
Genetique Medicale CHR Le Mans (France)
Genetique Medicale CHR Le Havre (France)
Genetique Medicale CHU Rennes (France)
Genetique Medicale CHU de Caen (France)
Genetique Medicale CHU de Brest (France)

Fifty-three pedigrees with the fragile X syndrome have been studied for amplification of the CGG repeat sequence adjacent to the CpG island in the FMR1 gene. Probe StB12.3 allowed direct detection of affected males, carrier females, normal transmitting males, as well as prenatal diagnosis. Comparison of our molecular data with our previous linkage data from 38 families indicates the effectiveness of direct DNA analysis. A total of 325 individuals were studied and no new mutation was found. All daughters of males with a premutation had a premutation. When the mother had a full mutation no children had a premutation. In premutated mothers, the size of the premutation seems to be a determining factor for the transition to the full mutation. All affected males had a full mutation or mosaicism and only 42% of the females with a full mutation were mentally impaired. Analysis of large families over 3 generations illustrated clearly the Sherman paradox. Furthermore, the analysis of these families is in reasonable agreement with the multiallelic model of Morton and Macpherson. Mosaic cases in the offspring of the mothers with a full mutation suggest a maternal germinal mosaicism. Then an abnormal methylation and a somatic heterogeneity established in very early steps of embryogenesis could explain these cases. 17 refs.

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Sponsoring Organization:: USDOE

OSTI ID:: 61998

Journal Information:: American Journal of Medical Genetics, Vol. 53, Issue 4; Other Information: PBD: 1 Dec 1994

Country of Publication:: United States

Language:: English

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Related Subjects

55 BIOLOGY AND MEDICINE
BASIC STUDIES
GENES
METHYLATION
HUMAN X CHROMOSOME
GENE MUTATIONS
GENE AMPLIFICATION
SIZE
DNA
PROBES
PATIENTS
MOSAICISM
MENTAL DISORDERS
HEREDITARY DISEASES
GENETICS

Title: Molecular analysis of 53 fragile X families with the probe StB12.3

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