Your search keyword '"Grimi, Beatrice"' showing total 27 results

1. Fetoplacental mosaicism: potential implications for false-positive and false-negative noninvasive prenatal screening results

Author

Grati, Francesca R., Malvestiti, Francesca, Ferreira, Jose C.P.B., Bajaj, Komal, Gaetani, Elisa, Agrati, Cristina, Grimi, Beatrice, Dulcetti, Francesca, Ruggeri, Anna M., De Toffol, Simona, Maggi, Federico, Wapner, Ronald, Gross, Susan, and Simoni, Giuseppe

Published

2014

2. Implications of fetoplacental mosaicism on cell‐free DNA testing for sex chromosome aneuploidies

Author

Grati, Francesca Romana, Bajaj, Komal, Zanatta, Valentina, Malvestiti, Francesca, Malvestiti, Barbara, Marcato, Livia, Grimi, Beatrice, Maggi, Federico, Simoni, Giuseppe, Gross, Susan J., and Ferreira, Jose

Published

2017

3. Interpreting mosaicism in chorionic villi: results of a monocentric series of 1001 mosaics in chorionic villi with follow-up amniocentesis

Author

Malvestiti, Francesca, Agrati, Cristina, Grimi, Beatrice, Pompilii, Eva, Izzi, Claudia, Martinoni, Lorenza, Gaetani, Elisa, Liuti, Maria Rosaria, Trotta, Anna, Maggi, Federico, Simoni, Giuseppe, and Grati, Francesca Romana

Published

2015

4. The type of feto-placental aneuploidy detected by cfDNA testing may influence the choice of confirmatory diagnostic procedure†

Author

Grati, Francesca Romana, Bajaj, Komal, Malvestiti, Francesca, Agrati, Cristina, Grimi, Beatrice, Malvestiti, Barbara, Pompilii, Eva, Maggi, Federico, Gross, Susan, Simoni, Giuseppe, and Ferreira, Jose Carlos P.

Published

2015

5. Increased risk after noninvasive prenatal screening on cell-free DNA circulating in maternal blood: does a new indication for invasive prenatal diagnosis require new criteria for confirmatory cytogenetic analysis?

Author

Grati, Francesca Romana, Malvestiti, Francesca, Grimi, Beatrice, Liuti, Rosaria, Agrati, Cristina, Gaetani, Elisa, Milani, Silvia, Martinoni, Lorenza, Zanatta, Valentina, Gallazzi, Gloria, Maggi, Federico, and Simoni, Giuseppe

Published

2015

6. De novo small supernumerary marker chromosomes detected on 143 000 consecutive prenatal diagnoses: chromosomal distribution, frequencies, and characterization combining molecular cytogenetics approaches

Author

Malvestiti, Francesca, De Toffol, Simona, Grimi, Beatrice, Chinetti, Sara, Marcato, Livia, Agrati, Cristina, Di Meco, Anna Maria, Frascoli, Giuditta, Trotta, Anna, Malvestiti, Barbara, Ruggeri, Anna, Dulcetti, Francesca, Maggi, Federico, Simoni, Giuseppe, and Grati, Francesca Romana

Published

2014

7. Performance of conventional cytogenetic analysis on chorionic villi when only one cell layer, cytotrophoblast or mesenchyme alone, is analyzed

Author

Grati, Francesca Romana, primary, Malvestiti, Francesca, additional, Gallazzi, Gloria, additional, Saragozza, Silvia, additional, Grimi, Beatrice, additional, Agrati, Cristina, additional, Branca, Lara, additional, Palumbo, Federica, additional, Trotta, Anna, additional, Chinetti, Sara, additional, Simoni, Giuseppe, additional, Ferreira, Jose, additional, and Benn, Peter, additional

Published

2021

8. Misdiagnosis rate when conventional cytogenetic analysis on chorionic villi is performed on only one cell layer, cytotrophoblast or mesenchyme, alone

Author

Grati, Francesca Romana, primary, Malvestiti, Francesca, additional, Gallazzi, Gloria, additional, Saragozza, Silvia, additional, Grimi, Beatrice, additional, Agrati, Cristina, additional, Branca, Lara, additional, Palumbo, Federica, additional, Trotta, Anna, additional, Chinetti, Sara, additional, Simoni, Giuseppe, additional, Ferreira, Jose, additional, and Benn, Peter, additional

Published

2021

9. Response to “QF-PCR as a substitute for karyotyping of cytotrophoblast for the analysis of chorionic villi: advantages and limitations from a cytogenetic retrospective audit of 44 727 first-trimester prenatal diagnoses”

Author

Grati, Francesca R., Malvestiti, Francesca, Grimi, Beatrice, Gaetani, Elisa, Di Meco, Anna Maria, Trotta, Anna, Liuti, Rosaria, Chinetti, Sara, Dulcetti, Francesca, Ruggeri, Anna Maria, Agrati, Cristina, Frascoli, Giuditta, Milani, Silvia, De Toffol, Simona, Martinoni, Lorenza, Paganini, Silvia, Marcato, Livia, Maggi, Federico, and Simoni, Giuseppe

Published

2013

10. QF-PCR as a substitute for karyotyping of cytotrophoblast for the analysis of chorionic villi: advantages and limitations from a cytogenetic retrospective audit of 44,727 first-trimester prenatal diagnoses

Author

Grati, Francesca R., Malvestiti, Francesca, Grimi, Beatrice, Gaetani, Elisa, Meco, Anna Maria Di, Trotta, Anna, Liuti, Rosaria, Chinetti, Sara, Dulcetti, Francesca, Ruggeri, Anna Maria, Agrati, Cristina, Frascoli, Giuditta, Milani, Silvia, Toffol, Simona De, Martinoni, Lorenza, Paganini, Silvia, Marcato, Livia, Maggi, Federico, and Simoni, Giuseppe

Published

2013

11. CVS analysis by QF-PCR: Advantages and limitations from an experience of 41,197 firsttrimester cytogenetic diagnoses: 10-1

Author

Grati, Francesca Romana, Malvestiti, Francesca, Marcato, Livia, Grimi, Beatrice, Gaetani, Elisa, Meco, Anna Maria Di, Trotta, Anna, Liuti, Rosaria, Chinetti, Sara, Dulcetti, Francesca, Ruggeri, Anna Maria, Agrati, Cristina, Martinoni, Lorenza, Paganini, Silvia, Castoldi, Barbara, Negri, Beatrice, Maggi, Federico, and Simoni, Giuseppe

Published

2012

12. KaryoLite™ BoBs™ test for the genetic analysis of miscarriage products: An efficient and cost-effective workflow: 5-6

Author

Grati, Francesca Romana, Gomes, Denise Molina, Ganesamoorthy, Devika, Aboura, Azzedine, Marcato, Livia, Bru, Fabrice, Slater, Howard R, Dupont, Celine, Toffol, Simona De, Bouhanna, Philippe, Malvestiti, Francesca, Selva, Jacqueline, Ruggeri, Anna Maria, Grimi, Beatrice, Maggi, Federico, Blondeel, Eleonore, Simoni, Giuseppe, and Vialard, François

Published

2012

13. Prenatal BACs-on-BeadsTM: the prospective experience of five prenatal diagnosis laboratories

Author

Vialard, François, Simoni, Giuseppe, Gomes, Denise Molina, Abourra, Azzedine, Toffol, Simona De, Bru, Fabrice, Martinez Romero, Maria Carmen, Nitsch, Lucio, Bouhanna, Philippe, Marcato, Livia, Popowski, Thomas, Grimi, Beatrice, Martínez-Conejero, Jose Antonio, Benzacken, B., Genesio, Rita, and Grati, Francesca R.

Published

2012

14. Prenatal diagnosis of del(4)(q27q31.23), due to a maternal balanced complex chromosome rearrangement, characterized by array-CGH

Author

Malvestiti, Francesca, De Toffol, Simona, Chinetti, Sara, Grimi, Beatrice, Favero, Giancarlo, Borsatti, Alessandro, Maggi, Federico, Simoni, Giuseppe, and Grati, Francesca Romana

Published

2010

15. Pure Monosomy and Pure Trisomy of 13q21.2–31.1 Consequent to a Familial Insertional Translocation: Exclusion of PCDH9 As the Responsible Gene for Autosomal Dominant Auditory Neuropathy (AUNAL)

Author

Grati, Francesca R., Lesperance, Marci M., De Toffol, Simona, Chinetti, Sara, Selicorni, Angelo, Emery, Sarah, Grimi, Beatrice, Dulcetti, Francesca, Malvestiti, Barbara, Taylor, Joseph, Milani, Silvia, Ruggeri, Anna M., Maggi, Federico, and Simoni, Giuseppe

Published

2009

16. eP486 - Misdiagnosis rate when conventional cytogenetic analysis on chorionic villi is performed on only one cell layer, cytotrophoblast or mesenchyme, alone

Author

Grati, Francesca Romana, Malvestiti, Francesca, Gallazzi, Gloria, Saragozza, Silvia, Grimi, Beatrice, Agrati, Cristina, Branca, Lara, Palumbo, Federica, Trotta, Anna, Chinetti, Sara, Simoni, Giuseppe, Ferreira, Jose, and Benn, Peter

Published

2021

17. Recombinant Chromosome 4 from a Familial Pericentric Inversion: Prenatal and Adulthood Wolf-Hirschhorn Phenotypes

Author

Malvestiti, Francesca, Benedicenti, Francesco, De Toffol, Simona, Chinetti, Sara, Höller, Adelheid, Grimi, Beatrice, Fichtel, Gertrud, Braghetto, Monica, Agrati, Cristina, Bonaparte, Eleonora, Maggi, Federico, Simoni, Giuseppe, and Grati, Francesca Romana

Subjects

Article Subject

Abstract

Pericentric inversion of chromosome 4 can give rise to recombinant chromosomes by duplication or deletion of 4p. We report on a familial case of Wolf-Hirschhorn Syndrome characterized by GTG-banding karyotypes, FISH, and array CGH analysis, caused by a recombinant chromosome 4 with terminal 4p16.3 deletion and terminal 4q35.2 duplication. This is an aneusomy due to a recombination which occurred during the meiosis of heterozygote carrier of cryptic pericentric inversion. We also describe the adulthood and prenatal phenotypes associated with the recombinant chromosome 4.

Published

2013

18. In this Issue

Author

Grati, Francesca R., primary, Malvestiti, Francesca, additional, Ferreira, Jose C.P.B., additional, Bajaj, Komal, additional, Gaetani, Elisa, additional, Agrati, Cristina, additional, Grimi, Beatrice, additional, Dulcetti, Francesca, additional, Ruggeri, Anna M., additional, De Toffol, Simona, additional, Maggi, Federico, additional, Wapner, Ronald, additional, Gross, Susan, additional, and Simoni, Giuseppe, additional

Published

2014

19. Pure monosomy and pure trisomy of 13q21.2???31.1 consequent to a familial insertional translocation: Exclusion of PCDH9 as the responsible gene for autosomal dominant auditory neuropathy (AUNA1)

Author

Division of Pediatric Otolaryngology, Department of Otolaryngology-Head and Neck Surgery, University of Michigan Health System, Ann Arbor, Michigan, Research and Development, Cytogenetics and Molecular Biology, TOMA Advanced Biomedical Assays S.p.A., Busto Arsizio, Varese, Italy ; TOMA, Advanced Biomedical Assays S.p.A., Via Ferrer 25/27, 21052 Busto Arsizio, VA, Italia., Research and Development, Cytogenetics and Molecular Biology, TOMA Advanced Biomedical Assays S.p.A., Busto Arsizio, Varese, Italy, I Clinica Pediatrica, Fondazione Policlinico Mangiagalli Regina Elena, Milan, Italy, Grati, Francesca R., Lesperance, Marci M., De Toffol, Simona, Chinetti, Sara, Selicorni, Angelo, Emery, Sarah, Grimi, Beatrice, Dulcetti, Francesca, Malvestiti, Barbara, Taylor, Joseph, Milani, Silvia, Ruggeri, Anna M., Maggi, Federico, Simoni, Giuseppe, Division of Pediatric Otolaryngology, Department of Otolaryngology-Head and Neck Surgery, University of Michigan Health System, Ann Arbor, Michigan, Research and Development, Cytogenetics and Molecular Biology, TOMA Advanced Biomedical Assays S.p.A., Busto Arsizio, Varese, Italy ; TOMA, Advanced Biomedical Assays S.p.A., Via Ferrer 25/27, 21052 Busto Arsizio, VA, Italia., Research and Development, Cytogenetics and Molecular Biology, TOMA Advanced Biomedical Assays S.p.A., Busto Arsizio, Varese, Italy, I Clinica Pediatrica, Fondazione Policlinico Mangiagalli Regina Elena, Milan, Italy, Grati, Francesca R., Lesperance, Marci M., De Toffol, Simona, Chinetti, Sara, Selicorni, Angelo, Emery, Sarah, Grimi, Beatrice, Dulcetti, Francesca, Malvestiti, Barbara, Taylor, Joseph, Milani, Silvia, Ruggeri, Anna M., Maggi, Federico, and Simoni, Giuseppe

Abstract

Insertional translocations (IT) are rare structural rearrangements. Offspring of IT balanced carriers are at high risk to have either pure partial trisomy or monosomy for the inserted segment as manifested by ???pure??? phenotypes. We describe an IT between chromosomes 3 and 13 segregating in a three-generation pedigree. Short tandem repeat (STR) segregation analysis and array-comparative genomic hybridization were used to define the IT as a 25.1 Mb segment spanning 13q21.2???q31.1. The phenotype of pure monosomy included deafness, duodenal stenosis, developmental and growth delay, vertebral anomalies, and facial dysmorphisms; the trisomy was manifested by only minor dysmorphisms. As the AUNA1 deafness locus on 13q14-21 overlaps the IT in the PCDH9 (protocadherin-9) gene region, PCDH9 was investigated as a candidate gene for deafness in both families. Genotyping of STRs and single nucleotide polymorphisms defined the AUNA1 breakpoint as 35 kb 5??? to PCDH9 , with a 2.4 Mb area of overlap with the IT. DNA sequencing of coding regions in the AUNA1 family and in the retained homologue chromosome in the monosomic patient revealed no mutations. We conclude that AUNA1 deafness does not share a common etiology with deafness associated with monosomy 13q21.2???q31.3; deafness may result from monosomy of PCHD9 or another gene in the IT, as has been demonstrated in contiguous gene deletion syndromes. Precise characterization of the breakpoints of the translocated region is useful to identify which genes may be contributing to the phenotype, either through haploinsufficiency or extra dosage effects, in order to define genotype???phenotype correlations. ?? 2009 Wiley-Liss, Inc.

Published

2009

20. Prenatal detection by subtelomeric FISH and MLPA of unbalanced meiotic recombinants resulting from parental pericentric inversions

Author

Grati, Francesca R., Chinetti, Sara, Malgara, Roberta, Rognoni, Giulia, Grimi, Beatrice, De Toffol, Simona, Milani, Silvia, Dulcetti, Francesca, Frascoli, Giuditta, Di Meco, Anna Maria, Liuti, Rosaria, Trotta, Anna, Coffa, Jordy, Maggi, Federico, and Simoni, Giuseppe

Published

2008

21. Chromosome abnormalities investigated by non‐invasive prenatal testing account for approximately 50% of fetal unbalances associated with relevant clinical phenotypes

Author

Grati, Francesca Romana, primary, Barlocco, Andrea, additional, Grimi, Beatrice, additional, Milani, Silvia, additional, Frascoli, Giuditta, additional, Di Meco, Anna Maria, additional, Liuti, Rosaria, additional, Trotta, Anna, additional, Chinetti, Sara, additional, Dulcetti, Francesca, additional, Ruggeri, Anna Maria, additional, De Toffol, Simona, additional, Clementi, Maurizio, additional, Maggi, Federico, additional, and Simoni, Giuseppe, additional

Published

2010

22. Confirmation of mosaicism and uniparental disomy in amniocytes, after detection of mosaic chromosome abnormalities in chorionic villi

Author

Grati, Francesca R, primary, Grimi, Beatrice, additional, Frascoli, Giuditia, additional, Di Meco, Anna Maria, additional, Liuti, Rosaria, additional, Milani, Silvia, additional, Trotta, Anna, additional, Dulcetti, Francesca, additional, Grosso, Enrico, additional, Miozzo, Monica, additional, Maggi, Federico, additional, and Simoni, Giuseppe, additional

Published

2006

23. Prenatal search for UPD 14 and UPD 15 in 83 cases of familial andde novo heterologous Robertsonian translocations

Author

Ruggeri, Anna, primary, Dulcetti, Francesca, additional, Miozzo, Monica, additional, Grati, Francesca R., additional, Grimi, Beatrice, additional, Bellato, Silvano, additional, Natacci, Federica, additional, Maggi, Federico, additional, and Simoni, Giuseppe, additional

Published

2004

24. Prenatal BACs-on-BeadsTM: the prospective experience of five prenatal diagnosis laboratories.

Author

Vialard, François, Simoni, Giuseppe, Gomes, Denise Molina, Abourra, Azzedine, Toffol, Simona De, Bru, Fabrice, Romero, Maria Carmen Martinez, Nitsch, Lucio, Bouhanna, Philippe, Marcato, Livia, Popowski, Thomas, Grimi, Beatrice, Martínez-Conejero, Jose Antonio, Benzacken, B., Genesio, Rita, and Grati, Francesca R.

Abstract

ABSTRACT Objective We previously reported on the validation of Prenatal BACs-on-BeadsTM on retrospectively selected and prospective prenatal samples. This bead-based multiplex assay detects chromosome 13, 18, 21 and X/Y aneuploidies and the nine most frequent microdeletion syndromes. We demonstrated that Prenatal BACs-on-BeadsTM is a new-generation, prenatal screening tool. Here, we describe the experience of five European prenatal diagnosis laboratories concerning the ongoing use of Prenatal BACs-on-BeadsTM. Methods Some 1653 samples were analyzed. All results were confirmed by conventional karyotyping or another appropriate technique. All indications for invasive prenatal diagnosis were included. Amniotic fluid and chorionic villus samples were analyzed in equivalent proportions. Results The failure rate was 3.3% and the overall abnormality detection rate was ~1/10. Eighty-five percent of the detected abnormalities were common aneuploidies. Eleven microdeletions and duplications were identified, thus giving an overall yield for microdeletion and microduplication detection of 1/145. Compared with QF-PCR, Prenatal BACs-on-BeadsTM provides an additional detection rate of ~1/250 for low-risk pregnancies. The false positive and negative rates were both <1%. Conclusion When associated with conventional karyotyping, the Prenatal BACs-on-BeadsTM assay combines a short turnaround time (typical of rapid aneuploidy detection tests) with valuable detection of the most frequent microdeletion syndromes that cannot be detected in cytogenetic analyses. © 2012 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2012

25. Prenatal search for UPD 14 and UPD 15 in 83 cases of familial and de novo heterologous Robertsonian translocations.

Author

Ruggeri, Anna, Dulcetti, Francesca, Miozzo, Monica, Grati, Francesca R., Grimi, Beatrice, Bellato, Silvano, Natacci, Federica, Maggi, Federico, and Simoni, Giuseppe

Abstract

Objectives The presence in the conceptus of a Robertsonian translocation predisposes to UPD formation, mainly by post-zygotic events of chromosome abnormality rescue. This is due to the increased risk of generating aneuploid zygotes because the rearranged chromosome and the respective homologues are prone to non-disjunction errors. Given this, carriers and karyotypically normal individuals conceived from a parent with a Robertsonian translocation are at risk for UPD. Abnormal phenotypes due to an imprinting effect have been found to be associated with UPD 14 and 15. The aim of the study was to refine, at the time of prenatal diagnosis, the risk for UPD 14 and 15 in a population with Robertsonian translocations involving these chromosomes. Methods Sixty-five cases of familial and de novo heterologous Robertsonian translocations involving chromosomes 14 and 15 and 18 fetuses with a normal karyotype, but conceived by a Robertsonian translocation carrier were prenatally studied to investigate the presence of UPD for chromosomes 14 and 15. Results Of the 65 Robertsonian translocation carriers, one fetus with a de novo der(14;21) showed maternal UPD 14. None of the 18 fetuses with a normal karyotype had UPD. Conclusion Our data, combined with other previous prenatal investigations provide a general risk estimate for UPD 14 and 15 of 0.6%. Nevertheless, combining our data and those previously reported, all three fetuses with UPD had a de novo Robertsonian translocation, thus suggesting a risk of UPD formation of about 3% for this specific group of translocation carriers. Copyright © 2004 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2004

26. Chromosome abnormalities investigated by noninvasive prenatal testing account for approximately 50 of fetal unbalances associated with relevant clinical phenotypesThe authors have no conflict of interests.How to cite this article: Grati FR, Barlocco A, Grimi B, Milani S, Frascoli G, Di Meco AM, Liuti R, Trotta A, Chinetti S, Dulcetti F, Ruggeri AM, De Toffol S, Clementi M, Maggi F, Simoni G. 2010. Chromosome abnormalities investigated by noninvasive prenatal testing account for approximately 50 of fetal unbalances associated with relevant clinical phenotypes. Am J Med Genet Part A 152A:1434–1442.

Author

Grati, Francesca Romana, Barlocco, Andrea, Grimi, Beatrice, Milani, Silvia, Frascoli, Giuditta, Di Meco, Anna Maria, Liuti, Rosaria, Trotta, Anna, Chinetti, Sara, Dulcetti, Francesca, Ruggeri, Anna Maria, De Toffol, Simona, Clementi, Maurizio, Maggi, Federico, and Simoni, Giuseppe

Abstract

During the past 20 years noninvasive screening tests have been increasingly utilized in prenatal diagnosis PD practice. Considerable effort has been exerted by multicenter consortia to evaluate the reliability of noninvasive screening tests in detecting those women with an increased risk of having a pregnancy affected by trisomies 21, 18, and 13, monosomy X, and triploidies. To what extent this group of abnormal karyotypes accounts for the total number of phenotypically relevant fetal chromosome abnormalities has, however, never been investigated. The present report is an attempt aimed to quantify this proportion. A retrospective analysis of a homogeneous survey of 115,128 consecutive invasive prenatal tests was undertaken. All cases were classified in accordance with the indication given for the invasive testing. Cytogenetic results regarding 96,416 karyotype analyses performed because of advanced maternal age ≥35 years or gestational anxiety <35 years were considered since these are the patients who usually undergo noninvasive screening tests. We calculated the number of cases T21, T18, T13, 45,X, and triploidy that would have been detected by prenatal screening on the basis of the published detection rate of the combined2 test or the quadruple test. Our findings indicate that the chromosomal abnormalities investigated by screening tests represent <50 of the fetal chromosomal abnormalities associated with an abnormal outcome ranging from intermediatetosevere in women <35 years 45.8 and 39.6 in the first and second trimesters, respectively, and sensitivity >50 in women ≥35 years 65.1 and 61.8, respectively. To conclude, approximately 50 of the phenotypically relevant abnormal karyotypes cannot be detected by noninvasive prenatal screening tests. © 2010 WileyLiss, Inc.

Published

2010

27. De novo small supernumerary marker chromosomes detected on 143,000 consecutive prenatal diagnoses: chromosomal distribution, frequencies, and characterization combining molecular cytogenetics approaches.

Author

Malvestiti F, De Toffol S, Grimi B, Chinetti S, Marcato L, Agrati C, Di Meco AM, Frascoli G, Trotta A, Malvestiti B, Ruggeri A, Dulcetti F, Maggi F, Simoni G, and Grati FR

Subjects

Adult, Chromosomes, Comparative Genomic Hybridization methods, Comparative Genomic Hybridization statistics & numerical data, Cytogenetic Analysis statistics & numerical data, Female, Genetic Markers, Humans, Incidence, Male, Pregnancy, Reproducibility of Results, Chromosome Aberrations statistics & numerical data, Cytogenetic Analysis methods, Mosaicism statistics & numerical data, Prenatal Diagnosis

Abstract

Objective: The risk of clinical consequences in prenatal cases with de novo small supernumerary marker chromosomes (sSMC), often in mosaic conditions, is not easy to predict, which results in difficulties in genetic counseling., Method: In this study, we evaluated the frequency, the chromosomal origin, and the clinical indication of 104 de novo sSMC detected in a monocenter survey on the basis of 143,000 consecutive prenatal diagnoses, and we assessed the reliability of molecular cytogenetics technologies for sSMC characterization., Results: We detected a de novo sSMC frequency of 0.072%. Its incidence in advanced maternal age group is statistically different from that found in maternal anxiety indication (<35 years old). A higher prevalence of mosaicism in chorionic villi sampling (CVS) than in amniotic fluids was also revealed related to confined placental mosaicisms. The risk of confirmation in amniotic fluids of mosaics previously revealed at CVS was 33.3%. No uniparental disomy conditions were found when imprinted chromosomes were involved in the occurrence of de novo sSMC. The majority of de novo sSMC were acrocentric derived-chromosomes, and a neocentromere formation was observed in one pregnancy., Conclusion: Our data support that array comparative genomic hybridization has improved sSMC characterization and demonstrate its utility in supporting genetic counseling. We propose a workflow for de novo sSMC characterization., (© 2014 John Wiley & Sons, Ltd.)

Published

2014