Molecular characterization of 39 de novo sSMC: contribution to prognosis and genetic counselling, a prospective study.

6533b853fe1ef96bd12ace00

RESEARCH PRODUCT

Molecular characterization of 39 de novo sSMC: contribution to prognosis and genetic counselling, a prospective study.

N. Lemeur G. Bourrouillou Véronique Satre Muriel Payet Anouck Schneider B. Quilichini Thierry Rousseau A. Liquier Jacques Puechberty François Vialard S. Fert Ferrer D. Molina Gomes S. Amblard Patrick Callier Martine Doco-fenzy H. Stora Marie-pierre Cordier Nathalie Marle Brigitte Simon-bouy Joris Andrieux Laurence Faivre A. L. Mosca Azzedine Aboura Florence Fellmann F. Girard-lemaire Danielle Martinet Pascal Chambon A. Delaye Damien Sanlaville M. Becker Elisabeth Flori C. Rangon Sébastien Jacquemont Anne Bazin V. Kremer Eva Pipiras R. Molignier F. Mugneret Géraldine Joly-helas Serge Aho A. Vigouroux-castera Anne-claude Tabet

subject

Adult Genetic Markers Risk Euchromatin Karyotype Context (language use)Prenatal diagnosis Single-nucleotide polymorphism Genetic Counseling Biology Polymorphism Single Nucleotide Young Adult Pregnancy Prenatal Diagnosis Genetics medicine SNP Humans Genetic Predisposition to Disease Prospective Studies Genetics (clinical)Genetic Association Studies In Situ Hybridization Fluorescence Genetics Chromosome Aberrations Comparative Genomic Hybridization medicine.diagnostic_test Karyotype Middle Aged Prognosis Molecular biology Female France Switzerland SNP array Fluorescence in situ hybridization Genome-Wide Association Study

description

Small supernumerary marker chromosomes (sSMCs) are structurally abnormal chromosomes that cannot be characterized by karyotype. In many prenatal cases of de novo sSMC, the outcome of pregnancy is difficult to predict because the euchromatin content is unclear. This study aimed to determine the presence or absence of euchromatin material of 39 de novo prenatally ascertained sSMC by array-comparative genomic hybridization (array-CGH) or single nucleotide polymorphism (SNP) array. Cases were prospectively ascertained from the study of 65,000 prenatal samples [0.060%; 95% confidence interval (CI), 0.042-0.082]. Array-CGH showed that 22 markers were derived from non-acrocentric markers (56.4%) and 7 from acrocentic markers (18%). The 10 additional cases remained unidentified (25.6%), but 7 of 10 could be further identified using fluorescence in situ hybridization; 69% of de novo sSMC contained euchromatin material, 95.4% of which for non-acrocentric markers. Some sSMC containing euchromatin had a normal phenotype (31% for non-acrocentric and 75% for acrocentric markers). Statistical differences between normal and abnormal phenotypes were shown for the size of the euchromatin material (more or less than 1 Mb, p = 0.0006) and number of genes (more or less than 10, p = 0.0009). This study is the largest to date and shows the utility of array-CGH or SNP array in the detection and characterization of de novo sSMC in a prenatal context.

year	journal	country	edition	language
2012-11-27	Clinical genetics

10.1111/cge.12138 https://pubmed.ncbi.nlm.nih.gov/23489061