Your search keyword '"Valentina Cigna"' showing total 21 results

1. Incidental Detection of a Chromosomal Aberration by Array-CGH in an Early Prenatal Diagnosis for Monogenic Disease on Coelomic Fluid

Author

Margherita Vinciguerra, Filippo Leto, Filippo Cassarà, Viviana Tartaglia, Michela Malacarne, Domenico Coviello, Valentina Cigna, Emanuela Orlandi, Francesco Picciotto, Gaspare Cucinella, Emanuela Salzano, Maria Piccione, Aurelio Maggio, and Antonino Giambona

Subjects

prenatal diagnosis, array comparative genomic hybridization, coelocentesis, monosomy X, beta thalassemia, Science

Abstract

Background: Turner syndrome is a rare genetic condition in which a female is partly or completely missing an X chromosome. Signs and symptoms vary among those affected. In fetuses that survive at birth and without congenital malformations, the prognosis is usually positive, but it has high lethality in utero, especially in the first trimester of pregnancy. Methods: We report a case of monosomy X detected during a prenatal diagnosis for beta thalassemia on coelomic fluid (CF) at the VIII week of gestation. Beta globin gene analysis, whole genome amplification (WGA), quantitative fluorescent PCR and array comparative genomic hybridization (array-CGH) were performed on DNA extracted from CF. Results: A monoallelic pattern of all Short Tandem Repeats mapped on the X chromosome was found and array-CGH performed on WGA from a few fetal erythroblasts confirmed monosomy X. Conclusion: This report underlines the importance of an early prenatal diagnosis and the countless potentialities of array-CGH that could make definition of molecular karyotype possible from a few fetal cells, unlike conventional cytogenetic techniques that require a greater cellular content. This is the first report of a molecular karyotype obtained from two cells selected by micromanipulation of CF and defined at such an early gestational age.

Published

2022

2. Prenatal diagnosis of hemoglobinopathies: from fetoscopy to coelocentesis

Author

Gianfranca Damiani, Margherita Vinciguerra, Cristina Jakil, Monica Cannata, Filippo Cassarà, Francesco Picciotto, Giovanna Schillaci, Valentina Cigna, Disma Renda, Aldo Volpes, Francesca Sammartano, Samuela Milone, Adolfo Allegra, Cristina Passarello, Filippo Leto, and Antonino Giambona

Subjects

thalassemia, prenatal diagnosis, coelocentesis., Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Prenatal diagnosis of hemoglobinopathies involves the study of fetal material from blood, amniocytes, trophoblast coelomatic cells and fetal DNA in maternal circulation. Its first application dates back to the 70s and it involves globin chain synthesis analysis on fetal blood. In the 1980s molecular analysis was introduced as well as amniocentesis and chorionic villi sampling under high-resolution ultrasound imaging. The application of direct sequencing and polymerase chain reactionbased methodologies improved the DNA analysis procedures and reduced the sampling age for invasive prenatal diagnosis from 18 to 16- 11 weeks allowing fetal genotyping within the first trimester of pregnancy. In the last years, fetal material obtained at 7-8 weeks of gestation by coelocentesis and isolation of fetal cells has provided new platforms on which to develop diagnostic capabilities while non-invasive technologies using fetal DNA in maternal circulation are starting to develop.

Published

2014

3. Celocentesis for Early Prenatal Diagnosis in Couples at-Risk for β-Thalassemia and Sicilian (δβ)0-Thalassemia

Author

Antonino Giambona, Filippo Leto, Filippo Cassarà, Viviana Tartaglia, Rosario Campisi, Corrado Campisi, Valentina Cigna, Elena Mugavero, Gaspare Cucinella, Emanuela Orlandi, Francesco Picciotto, Aurelio Maggio, and Margherita Vinciguerra

Subjects

Biochemistry (medical), Clinical Biochemistry, Hematology, Genetics (clinical)

Published

2022

4. 5612571 EARLIER PRENATAL DIAGNOSIS OF HEMOGLOBINOPATHIES BY CELOCENTESIS

Author

Antonino Giambona, A.G., primary, Filippo Leto, F.L., additional, Filippo Cassara, F.C., additional, Viviana Tartaglia, V.T., additional, Valentina Cigna, V.C., additional, Gaspare Cucinella, G.C., additional, Emanuela Orlandi, E.O., additional, Francesco Picciotto, F.P., additional, Margherita Vinciguerra, M.V., additional, and Aurelio Maggio, A.M., additional

Published

2023

5. Early prenatal diagnosis of Hb Lepore Boston‐Washington and β‐thalassemia on fetal celomatic DNA

Author

Antonino Giambona, Filippo Leto, Filippo Cassarà, Viviana Tartaglia, Giuseppe Marchese, Emanuela Orlandi, Valentina Cigna, Francesco Picciotto, Aurelio Maggio, and Margherita Vinciguerra

Subjects

Fetus, Pregnancy, Hemoglobins, Abnormal, Prenatal Diagnosis, beta-Thalassemia, Biochemistry (medical), Clinical Biochemistry, Humans, Female, DNA, Hematology, General Medicine

Abstract

Analysis of fetal DNA in at risk couples for thalassemia is performed from fetal trophoblast or amniotic fluid cells. Although these procedures are in common use, the main limitation is essentially due to the late gestation week in which diagnosis is performed. The celomic cavity develops around 4 weeks of pregnancy within the extraembryonic mesoderm and contains embryonic erythroid precursor cells as a source of fetal DNA that can be used to perform invasive prenatal diagnosis.Celomatic fluids were obtained at 8 weeks of gestation in thirteen women with high-risk pregnancies. Twelve of these couples were at risk for Hb Lepore disease and β-thalassemia and one couple represented a rare case in which both parents were carriers of Hb Lepore Boston-Washington. Fetal cells were isolated by micromanipulator and nested polymerase chain reactions were performed.The analysis was successfully performed in all examined cases. Two fetuses were found to have a compound heterozygosity for β-thalassemia and Hb Lepore Boston-Washington, three fetuses were found to be carriers of β-thalassemia, three fetuses of Hb Lepore, five were found without parental mutations. The genotypic analysis, carried out both by amniocentesis and on abortive tissue or after birth, showed concordance with results obtained on fetal celomic DNA.Our results unequivocally show that fetal DNA can be obtained by nucleated fetal cells present in celomatic fluid and demonstrate for the first time that prenatal diagnosis of β-thalassemia and Hb Lepore may be feasible in an earlier time of pregnancy than other procedures.

Published

2022

6. Celomic Fluid: Laboratory Workflow for Prenatal Diagnosis of Monogenic Diseases

Author

Antonino Giambona, Margherita Vinciguerra, Filippo Leto, Filippo Cassarà, Viviana Tartaglia, Valentina Cigna, Emanuela Orlandi, Francesco Picciotto, Nourah H. Al Qahtani, Eman S. Alsulmi, Noor B. Almandil, Sayed AbdulAzeez, J. Francis Borgio, and Aurelio Maggio

Subjects

Pharmacology, Pregnancy Trimester, First, Fetus, Pregnancy, Prenatal Diagnosis, Genetics, Humans, Molecular Medicine, Female, DNA, General Medicine, Workflow

Abstract

Celomic fluid can be considered as an ultra-filtrate of maternal serum, containing a high protein concentration, urea, and many other molecules. It is an important transfer interface and a reservoir of nutrients for the embryo. Celomic fluid contains fetal cells that can be used for prenatal diagnosis of monogenic diseases in an earlier gestational period than villocentesis and amniocentesis.The purpose of this study was to evaluate the characteristics of celomic fluid and to establish a workflow laboratory procedure for very early prenatal diagnosis of monogenic diseases.Three hundred and eighty-five celomatic fluids were collected between the seventh and tenth week of gestation. We sampled 1 mL of celomic fluid in all cases. The embryo-fetal erythroid precursor cells were selected by the anti-CD71 microbead method or by a direct micromanipulator pick-up on the basis of their morphology. We amplified the extracted DNA using a nested polymerase chain reaction. Primers for short tandem repeat amplification were used to perform a quantitative fluorescent polymerase chain reaction evaluation to control maternal contamination.We observed maternal contamination in 95% of celomic fluids with a range between 5 and 100%. No fetal cells were observed in 0.78% of celomic fluids. The number of fetal cells ranged from a few units to several hundred. Isolation of embryo-fetal erythroblasts selected by the micromanipulator made diagnosis feasible in all cases.The selection of fetal cells by a micromanipulator and nested polymerase chain reaction analysis made celomatic fluid suitable for early prenatal diagnosis of monogenic disorders even in the presence of high maternal contamination and few fetal cells. The procedure reported in this study provides the opportunity for the use of celomic fluid sampled by celocentesis as an alternative to chorionic villi sampling and amniocentesis, to allow invasive prenatal diagnosis at a very early stage of pregnancy.

Published

2022

7. Incidental Detection of a Chromosomal Aberration by Array-CGH in an Early Prenatal Diagnosis for Monogenic Disease on Coelomic Fluid

Author

Margherita Vinciguerra, Filippo Leto, Filippo Cassarà, Viviana Tartaglia, Michela Malacarne, Domenico Coviello, Valentina Cigna, Emanuela Orlandi, Francesco Picciotto, Gaspare Cucinella, Emanuela Salzano, Maria Piccione, Aurelio Maggio, Antonino Giambona, Vinciguerra M., Leto F., Cassarà F., Tartaglia V., Malacarne M., Coviello D., Cigna V., Orlandi E., Picciotto F., Cucinella G., Salzano E., Piccione M., Maggio A., and Giambona A.

Subjects

Space and Planetary Science, Paleontology, prenatal diagnosis, array comparative genomic hybridization, coelocentesis, monosomy X, beta thalassemia, array comparative genomic hybridization, beta thalassemia, coelocentesis, monosomy X, prenatal diagnosis, General Biochemistry, Genetics and Molecular Biology, Ecology, Evolution, Behavior and Systematics

Abstract

Background: Turner syndrome is a rare genetic condition in which a female is partly or completely missing an X chromosome. Signs and symptoms vary among those affected. In fetuses that survive at birth and without congenital malformations, the prognosis is usually positive, but it has high lethality in utero, especially in the first trimester of pregnancy. Methods: We report a case of monosomy X detected during a prenatal diagnosis for beta thalassemia on coelomic fluid (CF) at the VIII week of gestation. Beta globin gene analysis, whole genome amplification (WGA), quantitative fluorescent PCR and array comparative genomic hybridization (array-CGH) were performed on DNA extracted from CF. Results: A monoallelic pattern of all Short Tandem Repeats mapped on the X chromosome was found and array-CGH performed on WGA from a few fetal erythroblasts confirmed monosomy X. Conclusion: This report underlines the importance of an early prenatal diagnosis and the countless potentialities of array-CGH that could make definition of molecular karyotype possible from a few fetal cells, unlike conventional cytogenetic techniques that require a greater cellular content. This is the first report of a molecular karyotype obtained from two cells selected by micromanipulation of CF and defined at such an early gestational age.

Published

2023

8. 5612571 EARLIER PRENATAL DIAGNOSIS OF HEMOGLOBINOPATHIES BY CELOCENTESIS

Author

A.G. Antonino Giambona, F.L. Filippo Leto, F.C. Filippo Cassara, V.T. Viviana Tartaglia, V.C. Valentina Cigna, G.C. Gaspare Cucinella, E.O. Emanuela Orlandi, F.P. Francesco Picciotto, M.V. Margherita Vinciguerra, and A.M. Aurelio Maggio

Subjects

Hematology

Published

2023

9. Early prenatal diagnosis of hemoglobinopathies by celocentesis is ready for use in routine clinical practice

Author

Antonino Giambona, Filippo Leto, Filippo Cassarà, Viviana Tartaglia, Giuseppe Marchese, Emanuela Orlandi, Valentina Cigna, Francesco Picciotto, Aurelio Maggio, and Margherita Vinciguerra

Subjects

Biochemistry (medical), Clinical Biochemistry, Hematology, General Medicine

Published

2022

10. Non-immune hydrops fetalis: Two case reports

Author

Clelia Lo Verso, Emanuela Orlandi, Valentina Cigna, Vincenzo Duca, Marianna Maranto, Gaspare Cucinella, Francesco Picciotto, Maranto M., Cigna V., Orlandi E., Cucinella G., Verso C.L., Duca V., and Picciotto F.

Subjects

Fetus, medicine.medical_specialty, Amniotic fluid, Heart disease, Obstetrics, business.industry, Anemia, Fetal transfusion, Fetal anemia, General Medicine, medicine.disease, Hydrops fetalis, Preterm cesarean section, Blood chemistry, Infectious disease (medical specialty), Case report, medicine, Etiology, business, Cordocentesis

Abstract

BACKGROUND Fetal hydrops is a serious condition difficult to manage, often with a poor prognosis, and it is characterized by the collection of fluid in the extravascular compartments. Before 1968, the most frequent cause was the maternal-fetal Rh incompatibility. Today, 90% of the cases are non-immune hydrops fetalis. Multiple fetal anatomic and functional disorders can cause non-immune hydrops fetalis and the pathogenesis is incompletely understood. Etiology varies from viral infections to heart disease, chromosomal abnormalities, hematological and autoimmune causes. CASE SUMMARY A 38-year-old pregnant woman has neck lymphoadenomegaly, fever, cough, tonsillar plaques at 14 wk of amenorrhea and a rash with widespread itching. At 27.5 wk a fetal ultrasound shows signs of severe anemia and hydrops. Cordo-centesis is performed with confirmation of severe fetal anemia and subsequent fetal transfusion. The karyotype is 46, XX, array-comparative genome hybridization (CGH) negative, and infectious tests are not conclusive. In the following days there is a progressive improvement of the indirect signs of fetal anemia. At 33.6 wk, for relapse of severe fetal anemia, further fetal transfusions are necessary and an urgent cesarean section is performed. On the day 12 of life, for the detection of anemia, the newborn is subjected to transfusion of concentrated red blood cells and begins treatment with erythropoietin. Later there is a normalization of blood chemistry values and the baby does not need new transfusions. A 29-year-old pregnant woman, with Sjogren's syndrome and positive Anti-Ro/SSA antibodies, is subjected to serial fetal ecocardio for branch block. At 26.5 wk there is a finding of fetal ascites. Infectious disease tests on amniotic fluid are negative as well as quantitative fluorescent polymerase chain reaction, Array CGH. At cordocentesis Hb is 1.3 mmol/L, consequently fetal transfusion is performed. Also in this case, due to continuous episodes of relapse of fetal anemia with consequent transfusions, at 29.4 wk a cesarean section is performed. On day 9 of life, a treatment with erythropoietin is started in the newborn, but the baby needs three blood transfusions. The search for autoantibodies in the baby found SS-A Ro60 positive, SSA-Ro52 positive and SS-B negative. The hemoglobin values normalized after the disappearance of maternal autoantibodies. CONCLUSION An attempt to determine the etiology of hydrops should be made at the time of diagnosis because the goal is to treat underlying cause, whenever possible. Even if the infectious examinations are not conclusive, but the pregnancy history is strongly suggestive of infection as in the first case, the infectious etiology must not be excluded. In the second case, instead, transplacental passage of maternal autoantibodies caused hydrops fetalis and severe anemia. Finally, obstetric management must be aimed at fetal support up to an optimal timing for delivery by evaluating risks and benefits to increase the chances of survival without sequelae.

Published

2021

11. Celocentesis for early prenatal diagnosis of hemoglobinopathy

Author

Valentina Cigna, Aurelio Maggio, Filippo Cassarà, Gianfranca Damiani, Filippo Leto, Kypros H. Nicolaides, Antonino Giambona, C Jakil, Francesco Picciotto, George Makrydimas, Giovanna Schillaci, Margherita Vinciguerra, and Manuela Orlandi

Subjects

Pregnancy, medicine.medical_specialty, Radiological and Ultrasound Technology, business.industry, Obstetrics, Obstetrics and Gynecology, Aneuploidy, Gestational age, Prenatal diagnosis, General Medicine, medicine.disease, Miscarriage, Hemoglobinopathy, Reproductive Medicine, Medicine, Gestation, Radiology, Nuclear Medicine and imaging, business, Live birth

Abstract

OBJECTIVE Celocentesis is an invasive technique that can provide prenatal diagnosis of single-gene disorders, from as early as 7 weeks' gestation. The objective of this study was to examine the safety of celocentesis. METHODS In this prospective study, celocentesis was performed for prenatal diagnosis of hemoglobinopathy in 402 singleton pregnancies in which both parents were carriers of β-thalassemia or sickle cell disease trait. We assessed procedure-related maternal discomfort or pain, success of sampling and obtaining results, pregnancy outcome and postnatal follow-up. RESULTS First, celocentesis was carried out at a median gestational age of 8.6 (range, 6.9-9.9) weeks and celomic fluid was successfully aspirated in 99.8% of cases. Second, 67% of women had no or only mild discomfort, 18% had moderate discomfort, 12% had mild-to-moderate pain and 3% had severe pain. Third, prenatal diagnosis from analysis of the celomic fluid was successful in 93.8% cases, and in the last 121 cases, it was always successful. Fourth, in all cases of successful sampling and analysis of celomic fluid, the diagnosis was concordant with results obtained from additional prenatal or postnatal testing. Fifth, in addition to diagnosis of hemoglobinopathy, quantitative fluorescence polymerase chain reaction analysis, which was performed to evaluate maternal contamination using several markers for chromosomes X, Y, 21, 18 and 13, led to the accurate diagnosis of chromosomal aneuploidy. Sixth, in all cases of an affected fetus diagnosed by celocentesis in which the parents chose termination of pregnancy, this was carried out

Published

2020

12. Very early prenatal diagnosis of Cockayne’s syndrome by coelocentesis

Author

Antonino Giambona, Margherita Vinciguerra, Filippo Leto, Filippo Cassarà, Gaspare Cucinella, Valentina Cigna, Emanuela Orlandi, Maria Piccione, Francesco Picciotto, Aurelio Maggio, Giambona A., Vinciguerra M., Leto F., Cassara F., Cucinella G., Cigna V., Orlandi E., Piccione M., Picciotto F., and Maggio A.

Subjects

ERCC6, Sex Factors, Pregnancy, Placenta, Prenatal diagnosis, Humans, Obstetrics and Gynecology, Female, Celocentesis, Cockayne’s syndrome, Coelomic fluid, CSB, DNA, Polymerase Chain Reaction, Foetal cell

Abstract

Cockayne’s syndrome (CS) is a rare autosomal recessive multisystem disease characterised by early severe progression of symptoms. This study reports the feasibility of earlier prenatal diagnosis of CS by coelocentesis at 8 weeks of gestation respect to amniocentesis or villocentesis. Three couples at risk for CS asked to perform prenatal diagnosis by coelocentesis. Coelomic fluid was aspired from coelomic cavity in four singleton pregnancy at 8weeks of gestation and 40 foetal cells were recovered by micromanipulator. Maternal DNA contamination was evaluated by quantitative fluorescent PCR (QF-PCR) and target regions of foetal DNA containing parental mutations of ERCC6 gene were amplified and sequenced. In all these cases, molecular analysis was possible. One foetus resulted affected of CS and the diagnosis was confirmed on placental tissue after voluntary abortion. In three cases, foetuses resulted carrier of a parental mutation and the results were confirmed after the birth. This study suggests that reliable prenatal diagnosis of CS could be performed using foetal cells present in coelomatic fluid in earlier pregnancy. Coelocentesis could be applied in prenatal diagnosis of CSs as well as for other monogenic diseases, at very early stage of pregnancy, if parental mutations are already known.Impact StatementWhat is already know on this subject? Previous studies utilising coelocentesis for prenatal determination of foetal sex reported variable success ranging from 58% to 95%, because of low total DNA content and presence of maternal cell contamination. This procedure has never been reported for early prenatal diagnosis at 8 weeks of gestation for rare genetically transmitted diseases such as Cockayne’s syndrome. What do the results of this study add? This study demonstrates that coelomic fluid sampling combined with well-standardised laboratory procedures can be applied for prenatal diagnosis at eight weeks of gestation for any rare monogenic disease if molecular defects are known. What are the implications of these findings for clinical practice and/or further research? The findings of this study in at risk couples for monogenic diseases investigated by coelocentesis demonstrate that embryo-foetal cell selection from CF allows reliable and early prenatal diagnosis of diseases. This technique is attractive to parents because it provides prenatal diagnosis of genetic disease at least 4 weeks earlier than what can be achieved by the traditional procedures reducing anxiety of parents and provides the option for medical termination of affected cases at 8–10 weeks’ gestation, which is less traumatic and safer than second-trimester surgical termination. Further research concerns the possibility to obtain foetal karyotype at eight weeks of gestation and the possibility of intrauterine corrective therapy.

Published

2022

13. Identification of embryo-fetal cells in celomic fluid using morphological and short-tandem repeats analysis

Author

Gianfranca Damiani, Adolfo Allegra, A Volpes, C Jakil, George Makrydimas, Giovanna Schillaci, Antonino Giambona, Filippo Leto, Cristina Passarello, Aurelio Maggio, Kypros H. Nicolaides, Valentina Cigna, and Giuseppe Stampone

Subjects

0301 basic medicine, Pregnancy, Fetus, 030219 obstetrics & reproductive medicine, Gestational sac, Obstetrics and Gynecology, Embryo, Prenatal diagnosis, Biology, medicine.disease, Andrology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, embryonic structures, Immunology, medicine, Gestation, Erythropoiesis, Yolk sac, Genetics (clinical)

Abstract

Objective The main problem to wide acceptability of celocentesis as earlier prenatal diagnosis is contamination of the sample by maternal cells. The objective of this study was to investigate the cellular composition of celomic fluid for morphological discrimination between maternal and embryo-fetal cells. Method Celomic fluids were aspired by ultrasound-guided transcervical celocentesis at 7-9 weeks’ gestation from singleton pregnancies before surgical termination for psychological reasons. DNA was extracted from celomic fluid cells showed the same morphology and quantitative fluorescentPCR assay was performed to evaluate their fetal or maternal origin. Results Six different types of non-hematological maternal and four different types of embryo-fetal cells were detected. The most common maternal cells were of epithelial origin. The majority of embryo-fetal cells were roundish with a nucleus located in an eccentric position near the wall. These cells were considered to be erythroblasts, probably derived from the yolk sac that serves as the initial site of erythropoiesis. Conclusions The combined use of morphology and DNA analysis make it possible to select and isolate embryo-fetal cells, even when maternal contamination is high. This development provides the opportunity for the use of celocentesis for early prenatal diagnosis of genetic diseases and application of array-CGH. This article is protected by copyright. All rights reserved.

Published

2016

14. Embryo-fetal erythroid cell selection from celomic fluid allows earlier prenatal diagnosis of hemoglobinopathies

Author

Giovanna Schillaci, Antonino Giambona, Cristina Passarello, C Jakil, Valentina Cigna, Filippo Leto, Gianfranca Damiani, Aurelio Maggio, George Makrydimas, Kypros H. Nicolaides, Francesco Picciotto, and Disma Renda

Subjects

0301 basic medicine, Fetus, Pregnancy, Pathology, medicine.medical_specialty, 030219 obstetrics & reproductive medicine, Obstetrics and Gynecology, Prenatal diagnosis, Embryo, Biology, medicine.disease, Andrology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, embryonic structures, medicine, Erythroid cell, Gestation, Maternal contamination, Genetics (clinical), Selection (genetic algorithm)

Abstract

Objective Celocentesis, which involves aspiration of celomic fluid at 7–9 weeks' gestation, can potentially provide early prenatal diagnosis of single-gene disorders. The main barrier to wide acceptability of this technique is contamination of the sample by maternal cells. This problem can be overcome through selection of embryo-fetal erythroid precursors, which are found in celomatic fluid. Method Embryo-fetal erythroid precursors were selected by an anti-CD71 MicroBeads method or by direct micromanipulator pickup of the cells selected on the basis of their morphology. Results In our series of 302 singleton pregnancies at high risk for hemoglobinopathies, Celocentesis provided a sample of celomic fluid in all cases. In 100 (33.1%) samples, maternal contamination was absent or very low ( 60%, and selection of embryo-fetal cells was achieved by micromanipulation. In all 302 cases, there was concordance between DNA obtained from celomic fluid samples and fetal or newborn DNA. Conclusions Celocentesis can be a reliable procedure for earlier prenatal diagnosis of fetal monogenic diseases. © 2016 John Wiley & Sons, Ltd.

Published

2016

15. Fetal aneuploidy diagnosed at celocentesis for early prenatal diagnosis of congenital hemoglobinopathies

Author

Cristina Passarello, Francesco Picciotto, Giovanna Schillaci, Gianfranca Damiani, Margherita Vinciguerra, Salvatrice A. Lauricella, Aurelio Maggio, George Makrydimas, Kypros H. Nicolaides, Filippo Leto, Antonino Giambona, and Valentina Cigna

Subjects

0301 basic medicine, Adult, medicine.medical_specialty, Trisomy 13 Syndrome, Aneuploidy, Chorionic villus sampling, Prenatal diagnosis, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, medicine, Humans, Fetus, 030219 obstetrics & reproductive medicine, medicine.diagnostic_test, Obstetrics, business.industry, Obstetrics and Gynecology, General Medicine, medicine.disease, Triploidy, Hemoglobinopathies, Pregnancy Trimester, First, 030104 developmental biology, medicine.anatomical_structure, Amniocentesis, Chorionic villi, Feasibility Studies, Female, Down Syndrome, Trisomy, business

Abstract

INTRODUCTION Currently, prenatal diagnosis of genetic disorders requires chorionic villus sampling or amniocentesis carried out after 11 and 16 weeks of gestation, respectively. Celocentesis is a procedure for prenatal diagnosis that could be used from as early as 7 weeks. The present investigation evaluated the feasibility of performing diagnosis for monogenic diseases using celomic fluid containing cells of fetal origin. MATERIAL AND METHODS Analysis consisted of 489 singleton pregnancies undergoing celocentesis for the prenatal diagnosis of hemoglobinopathies (n = 367) or before surgical termination of pregnancy for social indications (n = 122). Embryo-fetal cells were isolated from celomic fluid using CD71 antibodies or by micromanipulation. Quantitative fluorescent polymerase chain reaction of short tandem repeat sequences of chromosomes 13, 18, 21, X and Y were used to determine the presence of maternal DNA. RESULTS 357/489 (73%) of celomic fluid samples were contaminated with maternal cells. In two cases, diagnosis was not possible due to the high contamination of celomic fluid. Eighty-seven (23.8%) fetuses were affected by hemoglobinopathies and, in five cases, chromosomal aneuploidies were found, including three cases of trisomy 21, one of trisomy 13 and one of triploidy. In all cases, the diagnosis of hemoglobinopathies and chromosomal abnormalities was confirmed by molecular and traditional cytogenetic analysis after amniocentesis, chorionic villus or placental tissue collection following pregnancy termination. CONCLUSIONS The findings of this study demonstrate that embryo-fetal cell selection from celomic fluid allows reliable and early prenatal diagnosis of hemoglobinopathies and can give more information on any fetal aneuploidy following the control of maternal contamination by quantitative fluorescent-PCR.

Published

2017

16. Identification of embryo-fetal cells in celomic fluid using morphological and short-tandem repeats analysis

Author

Antonino, Giambona, Filippo, Leto, Gianfranca, Damiani, Cristina, Jakil, Valentina, Cigna, Giovanna, Schillaci, Giuseppe, Stampone, Aldo, Volpes, Adolfo, Allegra, Kypros H, Nicolaides, George, Makrydimas, Cristina, Passarello, and Aurelio, Maggio

Subjects

Comparative Genomic Hybridization, Gestational Age, DNA, Embryo, Mammalian, Polymerase Chain Reaction, Fluorescence, Body Fluids, Pregnancy Trimester, First, Fetus, Gestational Sac, Pregnancy, Prenatal Diagnosis, Humans, Female, Microsatellite Repeats

Abstract

The main problem to wide acceptability of celocentesis as earlier prenatal diagnosis is contamination of the sample by maternal cells. The objective of this study was to investigate the cellular composition of celomic fluid for morphological discrimination between maternal and embryo-fetal cells.Celomic fluids were aspired by ultrasound-guided transcervical celocentesis at 7-9 weeks' gestation from singleton pregnancies before surgical termination for psychological reasons. DNA extracted from celomic fluid cells showed the same morphology, and quantitative fluorescent polymerase chain reaction (PCR) assay was performed to evaluate their fetal or maternal origin.Six different types of non-hematological maternal and four different types of embryo-fetal cells were detected. The most common maternal cells were of epithelial origin. The majority of embryo-fetal cells were roundish with a nucleus located in an eccentric position near the wall. These cells were considered to be erythroblasts, probably derived from the yolk sac that serves as the initial site of erythropoiesis.The combined use of morphology and DNA analysis makes it possible to select and isolate embryo-fetal cells, even when maternal contamination is high. This development provides the opportunity for the use of celocentesis for early prenatal diagnosis of genetic diseases and application of array comparative genomic hybridization. © 2016 John WileySons, Ltd.

Published

2016

17. Embryo-fetal erythroid cell selection from celomic fluid allows earlier prenatal diagnosis of hemoglobinopathies

Author

Antonino, Giambona, Gianfranca, Damiani, Filippo, Leto, Cristina, Jakil, Disma, Renda, Valentina, Cigna, Giovanna, Schillaci, Francesco, Picciotto, Kypros H, Nicolaides, Cristina, Passarello, George, Makrydimas, and Aurelio, Maggio

Subjects

Pregnancy Trimester, First, Erythroid Cells, Pregnancy, Prenatal Diagnosis, beta-Thalassemia, Humans, Female, Microscopy, Phase-Contrast, Anemia, Sickle Cell, Biomarkers

Abstract

Celocentesis, which involves aspiration of celomic fluid at 7-9 weeks' gestation, can potentially provide early prenatal diagnosis of single-gene disorders. The main barrier to wide acceptability of this technique is contamination of the sample by maternal cells. This problem can be overcome through selection of embryo-fetal erythroid precursors, which are found in celomatic fluid.Embryo-fetal erythroid precursors were selected by an anti-CD71 MicroBeads method or by direct micromanipulator pickup of the cells selected on the basis of their morphology.In our series of 302 singleton pregnancies at high risk for hemoglobinopathies, Celocentesis provided a sample of celomic fluid in all cases. In 100 (33.1%) samples, maternal contamination was absent or very low (5%), and unambiguous results were obtained without the need for any preliminary procedures. In 160 (53%) cases, the contamination was between 5% and 60%, and selection of embryo-fetal erythroid precursors was successfully achieved by anti-CD71 MicroBeads. In 42 (13.9%) cases, the contamination was60%, and selection of embryo-fetal cells was achieved by micromanipulation. In all 302 cases, there was concordance between DNA obtained from celomic fluid samples and fetal or newborn DNA.Celocentesis can be a reliable procedure for earlier prenatal diagnosis of fetal monogenic diseases.

Published

2015

18. Non-mosaic Tetrasomy Yp by Complex Isodicentric Rearrangement of the Y Chromosome: Prenatal Diagnosis with Cordocentesis in a Fetus with Abnormal Obstetric Ultrasound

Author

Salvatrice A. Lauricella, V. Consiglio, Helenia C. Cuttaia, Martina Busè, Valentina Cigna, Maria Piccione, and Giovanna Schillaci

Subjects

Gynecology, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Clinodactyly, Polydactyly, medicine.diagnostic_test, business.industry, Prenatal diagnosis, Karyotype, Y chromosome, medicine.disease, Testis determining factor, Tetrasomy, Medicine, medicine.symptom, business, Fluorescence in situ hybridization

Abstract

Tetrasomy Y is a very rare event, especially when it is present in a complete form. It is determined by complex rearrangement of the Y chromosome. Clinical features include psychomotor delay, skeletal abnormalities and facial dysmorphism. We report on a case of prenatal diagnosis of non-mosaic tetrasomy Yp, performed by karyotype and fluorescence in situ hybridization (FISH) on fetal blood. These analyses showed the presence of two isodicentric Y, with two copies of SRY and one copy of DXZ1 (XCEN) in each one. Karyotype was characterized as 47; X, Isodicentric (Y) (pter→q12::q12→pter) x2 (SRYx4). Cytogenetic studies were performed after detection of abnormal prenatal ultrasound, showing severe intrauterine growth restriction (symmetric IUGR), hydropic placenta, mild cerebellar hypoplasia, microretrognathia, hyperechogenic bowel with slight distension, dilation of recto-sigmoid tract, ambiguous genitalia, clinodactyly of the right fifth finger, suspected polydactyly. It was not possible to make a clear genotypephenotype correlation because a pregnancy interruption was performed.

Published

2015

19. Prenatal diagnosis of hemoglobinopathies: from fetoscopy to coelocentesis

Author

Cristina Passarello, C Jakil, Disma Renda, A Volpes, Monica Cannata, Filippo Cassarà, Filippo Leto, Gianfranca Damiani, Francesco Picciotto, Antonino Giambona, Giovanna Schillaci, Francesca Sammartano, Samuela Milone, Margherita Vinciguerra, Valentina Cigna, and Adolfo Allegra

Subjects

Gynecology, thalassemia, Fetus, medicine.medical_specialty, Pregnancy, prenatal diagnosis, medicine.diagnostic_test, business.industry, Obstetrics, Chorionic villus sampling, Prenatal diagnosis, medicine.disease, Fetoscopy, Cell-free fetal DNA, embryonic structures, medicine, Amniocentesis, coelocentesis, thalassemia, prenatal diagnosis, coelocentesis, Diseases of the blood and blood-forming organs, RC633-647.5, business, Genotyping

Abstract

Prenatal diagnosis of hemoglobinopathies involves the study of fetal material from blood, amniocytes, trophoblast coelomatic cells and fetal DNA in maternal circulation. Its first application dates back to the 70s and it involves globin chain synthesis analysis on fetal blood. In the 1980s molecular analysis was introduced as well as amniocentesis and chorionic villi sampling under high-resolution ultrasound imaging. The application of direct sequencing and polymerase chain reactionbased methodologies improved the DNA analysis procedures and reduced the sampling age for invasive prenatal diagnosis from 18 to 16–11 weeks allowing fetal genotyping within the first trimester of pregnancy. In the last years, fetal material obtained at 7–8 weeks of gestation by coelocentesis and isolation of fetal cells has provided new platforms on which to develop diagnostic capabilities while non-invasive technologies using fetal DNA in maternal circulation are starting to develop.

Published

2014

20. Earlier Antenatal Diagnosis of Hemoglobinopathies By Coelocentesis

Author

Rosario Di Maggio, Cristina Yakil, Angela Vitrano, Antonino Giambona, Aurelio Maggio, Giovanna Schillaci, Massimiliano Sacco, Valentina Cigna, Cristina Passarello, Gianfranca Damiani, and Filippo Leto

Subjects

Gynecology, medicine.medical_specialty, Fetus, Pregnancy, Amniotic fluid, medicine.diagnostic_test, business.industry, Obstetrics, Immunology, Gestational sac, Chorionic villus sampling, Prenatal diagnosis, Cell Biology, Hematology, medicine.disease, Biochemistry, medicine.anatomical_structure, Amniocentesis, medicine, Gestation, business

Abstract

In countries with a high prevalence of hemoglobinopathy carriers, the only realistic approach to control the birth of new patients with thalassemia major or sickle cell disease is population screening in combination with invasive prenatal diagnosis[1]. In the early 1990's, molecular definition of the thalassemia defects, development of procedures for their detection by DNA analysis and introduction of amniotic fluid sampling (amniocentesis) or chorionic villus sampling (CVS) led to early prenatal diagnosis at 16 and 11 weeks, respectively [2]. An alternative technique for earlier diagnosis is celocentesis [3]. At the end of week 4 of gestation, the developing exocoelomic cavity (ECC) splits the extra-embryonic mesoderm into two layers, the somatic mesoderm lining the trophoblast and the splanchnic mesoderm covering the secondary yolk sac and the embryo. The ECC is the largest anatomical space inside the gestational sac between 5 and 9 weeks of gestation and is surrounded by celomic fluid (CF), which contains cells of fetal origin [4-5]. This fluid can be sampled by a technique that involves the ultrasound-guided insertion of a needle through the vagina from as early as 7 weeks of gestation. Previous studies utilizing coelocentesis for prenatal determination of single-gene defects reported variable success ranging from 58 to 95% because of presence of maternal cell contamination (MCC) [6]. In this work we demostred as this problem can be overcome through the identification of embryo-fetal erythroid precursors presented in the coelomatic fluid and their specific selection. 302 couples from different regions of Italy, at risk for ß thalassemia or sickle cell disease asked for prenatal diagnosis by coelocentesis that was carried out at between 6+6 and 9+2 weeks' gestation. Coelomic fluid samples with no or very low (5% maternal contamination, two different procedures were used to isolate embryo-fetal cells: the first technique involved positive selection of embryo-fetal erythroid precursors by anti-CD71 MicroBeads (160 samples), the second procedure was through the use of a micromanipulator (42 samples). In 68/300 (22.6%) cases the fetus was affected by ß-thalass/ß-thalassemia and 66 women chosen to terminate the pregnancy. Two families decided to continue the pregnancy for ethical reasons despite the documented presence of an affected fetus. The antenatal diagnosis was confirmed in all 66 cases by molecular analysis of placental tissue after termination (Table 1). In 232/300 (77.4%) cases the fetus was diagnosed as being normal or a carrier for ß-thalassemia or sicke cell disease. The results obtained after coelocentesis were confirmed by amniocentesis or postnatally. In two case (0.66%) was no obtained a reliable diagnosis because no fetal cells were found (Table 1). The findings of this study in a large number of pregnancies investigated by coelocentesis, demonstrate that embryo-fetal erytroid cell selection from coelomatic fluid allows reliable and earlier prenatal diagnosis of hemoglobinopathies. This technique is attractive to parents because it provides prenatal diagnosis of genetic disease at least 4 weeks earlier respect to traditional procedures reducing anxiety of parents and from a clinical point of view this procedure would allow women to undergo medical TOP at 8-10 weeks of gestation which is less traumatic and safer than second trimester surgical TOP. Table 1. Overall results of prenatal diagnosis of hemoglobinopathies by coelocentesis. Number of coelocentesis effectuated 302 Results of Prenatal diagnosis: Affected 68 Carrier of hemoglobinopathies 161 Non Affected 71 diagnosis not reiable 2 Control post coelocentesis: Placental tissue after termination 66 CVS or amniocentesis 153 Postnatal test 61 Awaiting 20 Coelocentesis diagnostic errors 0 Disclosures No relevant conflicts of interest to declare.

Published

2015

21. Prenatal diagnosis of a variant of the azygos venous system

Author

Rossella Conti, Clelia Lo Verso, Gianfranca Damiani, Vincenzo Duca, Valentina Cigna, and Laura Lo Verso

Subjects

medicine.medical_specialty, Intercostal veins, Hemiazygos vein, Short Report, Prenatal diagnosis, 030218 nuclear medicine & medical imaging, Vascular anomaly, 03 medical and health sciences, Accessory hemiazygos vein, 0302 clinical medicine, Superior vena cava, medicine, Vein, Multidisciplinary, Azygos vein, business.industry, Variants, Mediastinum, Anatomy, medicine.disease, medicine.anatomical_structure, medicine.vein, 030220 oncology & carcinogenesis, cardiovascular system, Radiology, business

Abstract

Background The azygos venous system consists of the azygos vein on the right side and the hemiazygos and accessory hemiazygos on the left side. The azygos vein runs through the abdominal cavity along the right side of the vertebral bodies, in a cranial direction, passes through the diaphragm and reaches the mediastinum, where it forms the arch of the azygos which flows into the superior vena cava. Along its course, the azygos vein communicates with the intercostal veins on the right, the hemiazygos vein that collects blood from the left lower intercostal veins, and accessory hemiazygos vein that drains into the left upper intercostal veins. The last two, at the level of the seventh thoracic vertebra, unite and end in the azygos vein. The accessory hemiazygos vein is normally included in the length between T4 and T8. The embryological origin of the accessory hemiazygos vein is the result of an expansion in the direction of the cranial hemiazygos vein, which comes from the left upper sovracardinale vein (Dudiak et al. in Semin Roentgenol 24(1):47–55, 1989; Radiographics 11(2):233–246, 1991; Webb et al. in Am J Roentgenol 139(1):157–161, 1982). Findings This case report describes a rare variant of azygos vein system identified in prenatal diagnosis and confirmed by postnatal ultrasonography. Conclusions The observation of the patient has excluded hemodynamic alterations associated with vascular anomaly.