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1. Disease onset in familial and sporadic multiple sclerosis in Argentina

Author

Rojas, J.I., Patrucco, L., MIguez, J., Sinay, V., Cassara, F. Pagani, Cáceres, F., Liguori, N. Fernandez, Saladino, M.L., Deri, N., Jaacks, G., Marcilla, M. Parada, Arrigoni, M.I., Correale, J., Fiol, M., Ysrraelit, M.C., Carrá, A., Curbelo, M.C., Martinez, A., Steinberg, J., Bestoso, S., Hryb, J.P., Di Pace, J.L., Perassolo, M.B., Carnero Contentti, E., Caride, A., Lopez, P.A., Martinez, C., Reich, E., and Cristiano, E.

Published
2016
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4. Reply

Author

Makrydimas, G., primary, Damiani, G., additional, Jakil, C., additional, Cigna, V., additional, Orlandi, M., additional, Picciotto, F., additional, Schillaci, G., additional, Cassarà, F., additional, Vinciguerra, M., additional, Leto, F., additional, Giambona, A., additional, Maggio, A., additional, and Nicolaides, K. H., additional

Published
2020
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5. Celocentesis for early prenatal diagnosis of hemoglobinopathy

Author

Makrydimas, G., primary, Damiani, G., additional, Jakil, C., additional, Cigna, V., additional, Orlandi, M., additional, Picciotto, F., additional, Schillaci, G., additional, Cassarà, F., additional, Vinciguerra, M., additional, Leto, F., additional, Giambona, A., additional, Maggio, A., additional, and Nicolaides, K. H., additional

Published
2020
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6. Gender ratio trends over time in multiple sclerosis patients from Argentina

Author

Rojas, J.I., Patrucco, L., MIguez, J., Sinay, V., Cassara, F. Pagani, Cáceres, F., Liguori, N. Fernandez, Saladino, M.L., Deri, N., Jaacks, G., Marcilla, M. Parada, Arrigoni, M.I., Correale, J., Fiol, M., Ysrraelit, M.C., Carrá, A., Curbelo, M.C., Martinez, A., Steinberg, J., Bestoso, S., Hryb, J.P., Di Pace, J.L., Perassolo, M.B., Contentti, E. Carnero, Caride, A., Lopez, P.A., Martinez, C., Reich, E., Giunta, D., and Cristiano, E.

Published
2017
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11. Management of chronic viral hepatitis in patients with thalassemia: Recommendations from an international panel

Author

Di Marco, V. Capra, M. Angelucci, E. Borgna-Pignatti, C. Telfer, P. Harmatz, P. Kattamis, A. Prossamariti, L. Filosa, A. Rund, D. Gamberini, M.R. Cianciulli, P. De Montalembert, M. Gagliardotto, F. Foster, G. Grangè, J.D. Cassarà, F. Iacono, A. Cappellini, M.D. Brittenham, G.M. Prati, D. Pietrangelo, A. Craxì, A. Maggio, A.

Abstract

Chelation therapy with new drugs prevents cardiac damage and improves the survival of thalassemia patients. Liver diseases have emerged as a critical clinical issue. Chronic liver diseases play an important role in the prognosis of thalassemia patients because of the high frequency of viral infections and important role of the liver in regulating iron metabolism. Accurate assessment of liver iron overload is required to tailor iron chelation therapy. The diagnosis of hepatitis B virus- or hepatitis C virus-related chronic hepatitis is required to detect patients who have a high risk of developing liver complications and who may benefit by antiviral therapy. Moreover, clinical management of chronic liver disease in thalassemia patients is a team management issue requiring a multidisciplinary approach. The purposes of this paper are to summarize the knowledge on the epidemiology and the risks of transmission of viral infections, to analyze invasive and noninvasive methods for the diagnosis of chronic liver disease, to report the knowledge on clinical course of chronic viral hepatitis, and to suggest the management of antiviral therapy in thalassemia patients with chronic hepatitis B or C virus or cirrhosis. © 2010 by The American Society of Hematology.

Published
2010

12. 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

13. Nonsense-mediated decay mechanism is a possible modifying factor of clinical outcome in nonsense cd39 beta thalassemia genotype

Author

Disma Renda, Maria Concetta Renda, Antonino Giambona, Giuseppina Calvaruso, G. Fiorentino, Paolo Rigano, Emanuela Fecarotta, Massimo Attanasio, Angela Vitrano, Filippo Cassarà, Angela Piazza, Aurelio Maggio, Renda, MC, Vitrano, A, Attanasio, M, Fecarotta, E, Piazza, A, Giambona, A, Fiorentino, G, Renda, D, Rigano, P, Calvaruso, G, Cassarà, F, and Maggio, A

Subjects
Pediatrics, medicine.medical_specialty, media_common.quotation_subject, Nonsense-mediated decay, Nonsense, Beta thalassemia, Biology, nonsense-mediated mRNA decay, beta-thalassemia, clinical outcame, beta-globin gene mutations, medicine.disease, Gastroenterology, nonsense-mediated mRNA decay, beta-thalassemia, beta-globin gene mutations, nonsense-mediated mRNA decay, beta-thalassemia, clinical outcame, beta-globin gene mutations, Internal medicine, Genotype, medicine, Diseases of the blood and blood-forming organs, RC633-647.5, media_common
Abstract

Nonsense-mediated mRNA decay (NMD) is a surveillance system to prevent the synthesis of non-functional proteins. In β-thalassemia, NMD may have a role in clinical outcome. An example of premature translation stop codons appearing for the first time is the β-globin cd39 mutation; when homozygous, this results in a severe phenotype. The aim of this study was to determine whether the homozygous nonsense cd39 may have a milder phenotype in comparison with IVS1,nt110/cd39 genotype. Genotypes have been identified from a cohort of 568 patients affected by β-thalassemia. These genotypes were compared with those found in 577 affected fetuses detected among 2292 prenatal diagnoses. The nine most common genotypes, each with an incidence rate of 1.5% or over, and together accounting for 80% of genotype frequencies, underwent statistical analysis. Genotype prevalence was calculated within the overall group. Results are expressed as proportions with 95% confidence intervals; P≤0.05 was considered statistically significant. A binomial distribution was assumed for each group; z-tests were used to compare genotype frequencies observed in the patient group with frequencies in the affected fetus group. In the absence of selecting factors, prevalence of these two genotypes was compared between a cohort of 568 β-thalassemia patients (PTS) and 577 affected fetuses (FOET) detected during the same period. IVS1,nt110/cd39 was significantly more prevalent in FOET than PTS (P是一种预防非功能性蛋白质合成的监控系统。在β地中海贫血中,NMD可能对临床结果有影响。第一次出现的过早终止密码子(PTC)为β珠蛋白cd39突变;若为纯合子,则会导致严重的表型。本研究旨在确定与IVS1,nt110/cd39基因型相比,纯合子无义cd39能否有更轻度的表型。目前已确定568名β地中海贫血患者的基因型,并与从2292个产前诊断中检测出的577名地中海贫血胎儿的基因型相比较。对9个最常见基因型进行统计分析,每个基因型的发生率均为1.5%或以上,共占基因型频率的80%。在整个组中计算基因型分布情况,其结果以95%置信区间表示;若P≤0.05,则具有统计意义。各组均假定成一个二项分布;Z测试适用于比较患者组的基因型频率和地中海贫血胎儿的基因型频率。 若没有选择因子,则比较568名β地中海贫血患者(PTS)和同一时期所检测到的577个地中海贫血胎儿(FOET)这两组基因型的发生率。IVS1,nt110/cd39在FOET中的发生率明显高于PTS(P

Published
2012

14. Iron Chelation Therapy in thalassaemia major: a sistematic review with meta-analyses of 1520 patients included on randomized clinical trials

Author

Adriana Ceci, John C. Wood, Giuseppina Aloj, Angela Vitrano, Antonis Kattamis, Maria Domenica Cappellini, John B. Porter, Aurelio Maggio, Paul Harmatz, Christian Gluud, Luciano Prossomariti, Suthat Fucharoen, Aldo Filosa, Filippo Cassarà, Fedele Bonifazi, Paolo Cianciulli, Robert W. Grady, Angela Iacono, Maggio, A, Filosa, A, Vitrano, A, Aloj, G, Kattamis, A, Ceci, A, Fucharoen, S, Cianciulli, P, Grady, RW, Prossomariti, L, Porter, JB, Iacono, A, Cappellini, MD, Bonifazi, F, Cassarà, F, Harmatz, P, Wood, J, and Gluud, C

Subjects
medicine.medical_specialty, Pyridones, Iron, MEDLINE, Thalassemia, Siderophores, Deferoxamine, Iron Chelating Agents, Chelation, treatment, thalassaemia, clinical trials, iron overload, meta-analysis, Benzoates, Gastroenterology, law.invention, chemistry.chemical_compound, Randomized controlled trial, law, Internal medicine, medicine, Humans, Ventricular Function, Deferiprone, Molecular Biology, Randomized Controlled Trials as Topic, Ejection fraction, business.industry, Myocardium, beta-Thalassemia, Deferasirox, Beta thalassemia, Cell Biology, Hematology, Triazoles, medicine.disease, Chelation Therapy, Surgery, Treatment Outcome, Liver, chemistry, Meta-analysis, Ferritins, Molecular Medicine, Drug Therapy, Combination, business, medicine.drug
Abstract

The effectiveness of deferoxamine (DFO), deferiprone (DFP), or deferasirox (DFX) in thalassemia major was assessed. Outcomes were reported as means±SD, mean differences with 95% CI, or standardized mean differences. Statistical heterogeneity was tested using χ2 (Q) and I2. Sources of bias and Grading of Recommendations Assessment, Development and Evaluation system (GRADE) were considered. Overall, 1520 patients were included. Only 7.4% of trials were free of bias. Overall measurements suggest low trial quality (GRADE). The meta-analysis suggests lower final liver iron concentrations during associated versus monotherapy treatment (p

Published
2011

15. Hepatocellular carcinoma in patients with thalassaemia syndromes: clinical characteristics and outcome in a long term single centre experience

Author

Gaetano Restivo Pantalone, Disma Renda, Veronica Di Salvo, Angela Vitrano, Franco Valenza, Antonino Giangreco, Filippo Cassarà, Aurelio Maggio, Fabio D’Amato, Elvira Bevacqua, Paolo Rigano, Restivo Pantalone, G, Renda, D, Valenza, F, D'Amato, F, Vitrano, A, Cassarà, F, Rigano, P, Di Salvo, V, Giangreco, A, Bevacqua, E, and Maggio, A

Subjects
Adult, Male, Pediatrics, medicine.medical_specialty, Carcinoma, Hepatocellular, Iron Overload, Cirrhosis, Thalassemia, Carcinoma, Humans, Medicine, Aged, business.industry, Liver Neoplasms, Transfusion Reaction, Cancer, Hematology, Hepatitis C, Hepatitis C, Chronic, Middle Aged, Prognosis, medicine.disease, Surgery, Hemoglobinopathy, Hepatocellular carcinoma, Thalassaemia, hepatocellular carcinoma, iron overload, cirrhosis, hepatitis C, Female, business, Liver cancer
Published
2010

16. Prenatal Diagnosis of Cystic Fibrosis by Celocentesis.

Author

Giambona A, Vinciguerra M, Leto F, Cassarà F, Marchese G, Cigna V, Orlandi E, Mugavero ME, Cucinella G, Maggio A, Termini L, Makrydimas G, D'Alcamo E, and Picciotto F

Subjects
Humans, Female, Pregnancy, Adult, beta-Thalassemia genetics, beta-Thalassemia diagnosis, Fetus, Cystic Fibrosis genetics, Cystic Fibrosis diagnosis, Prenatal Diagnosis methods, Cystic Fibrosis Transmembrane Conductance Regulator genetics
Abstract

Celocentesis is a new sampling tool for prenatal diagnosis available from 7 weeks in case of couples at risk for genetic diseases. In this study, we reported the feasibility of earlier prenatal diagnosis by celocentesis in four cases of cystic fibrosis and one case of cystic fibrosis and β-thalassemia co-inherited in the same fetus. Celomic fluids were aspired from the celomic cavity between 8 +2 and 9 +3 weeks of gestation and fetal cells were picked up by micromanipulator. Maternal DNA contamination was tested and target regions of fetal DNA containing parental pathogenetic variants of CFTR and HBB genes were amplified and sequenced. Four of the five fetuses resulted as being affected by cystic fibrosis and, in all cases, the women decided to interrupt the pregnancy. In the other case, the fetus presented a healthy carrier of cystic fibrosis. The results were confirmed in three cases on placental tissue. In one case, no abortive tissue was obtained. In the last case, the woman refused the prenatal diagnosis to confirm the celocentesis data; the pregnancy is ongoing without complications. This procedure provides prenatal diagnosis of monogenic diseases at least four weeks earlier than traditional procedures, reducing the anxiety of patients and providing the option for medical termination of the affected fetus at 8-10 weeks of gestation, which is less traumatic and safer than surgical termination in the second trimester.

Published
2024
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18. Incidental Detection of a Chromosomal Aberration by Array-CGH in an Early Prenatal Diagnosis for Monogenic Disease on Coelomic Fluid.

Author

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

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

Author

Giambona A, Leto F, Cassarà F, Tartaglia V, Campisi R, Campisi C, Cigna V, Mugavero E, Cucinella G, Orlandi E, Picciotto F, Maggio A, and Vinciguerra M

Subjects
Female, Humans, Pregnancy, Prenatal Diagnosis, Early Diagnosis, Fetus, beta-Thalassemia, Thalassemia
Abstract

The procedures commonly used for prenatal diagnosis (PND) of thalassemia are villocentesis or amniocentesis, respectively, at the 11th and 16th weeks of gestation. Their main limitation is essentially due to the late gestation week in which diagnosis is performed. The celomic cavity is accessible between the 7th and 9th weeks of gestation and it has been demonstrated that it contains embryonic erythroid precursor cells as a source of fetal DNA for earlier invasive PND of thalassemia and other monogenic diseases. In this study, we report the use of celomatic fluids obtained from nine women with high-risk pregnancies for Sicilian (δβ) 0 -thalassemia [(δβ) 0 -thal] deletion (NG_000007.3: g.64336_77738del13403) and β-thalassemia (β-thal). Fetal cells were isolated by a micromanipulator, and nested polymerase chain reaction (PCR) and short tandem repeats (STRs) analysis were performed. Prenatal diagnosis was successfully performed in all examined cases. One fetus was a compound heterozygote for (δβ) 0 - and β-thal, three fetuses were found to be carriers of β-thal, four fetuses carriers of a Sicilian δβ deletion, and one fetus without parental mutations. Accidentally, a rare case of paternal triploidy was observed. 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 the celomatic fluid and demonstrate, for the first time, that PND of Sicilian (δβ) 0 -thal and β-thal is feasible at an earlier time in pregnancy than other procedures.

Published
2022
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20. Early prenatal diagnosis of Hb Lepore Boston-Washington and β-thalassemia on fetal celomatic DNA.

Author

Giambona A, Leto F, Cassarà F, Tartaglia V, Marchese G, Orlandi E, Cigna V, Picciotto F, Maggio A, and Vinciguerra M

Subjects
DNA genetics, Female, Fetus chemistry, Humans, Pregnancy, Prenatal Diagnosis methods, Hemoglobins, Abnormal genetics, beta-Thalassemia diagnosis, beta-Thalassemia genetics
Abstract

Introduction: 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., Methods: 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., Results: 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., Conclusion: 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., (© 2022 John Wiley & Sons Ltd.)

Published
2022
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21. Very early prenatal diagnosis of Cockayne's syndrome by coelocentesis.

Author

Giambona A, Vinciguerra M, Leto F, Cassarà F, Cucinella G, Cigna V, Orlandi E, Piccione M, Picciotto F, and Maggio A

Subjects
DNA analysis, Female, Humans, Polymerase Chain Reaction methods, Pregnancy, Sex Factors, Placenta chemistry, Prenatal Diagnosis methods
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 8 weeks 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 Statement What 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
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22. Celomic Fluid: Laboratory Workflow for Prenatal Diagnosis of Monogenic Diseases.

Author

Giambona A, Vinciguerra M, Leto F, Cassarà F, Tartaglia V, Cigna V, Orlandi E, Picciotto F, Al Qahtani NH, Alsulmi ES, Almandil NB, AbdulAzeez S, Borgio JF, and Maggio A

Subjects
DNA, Female, Humans, Pregnancy, Pregnancy Trimester, First, Workflow, Fetus, Prenatal Diagnosis methods
Abstract

Background: 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., Objective: 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., Methods: 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., Results: 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., Conclusions: 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., (© 2022. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published
2022
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23. Double Heterozygosity for Hb Durham-N.C. ( HBB : c.344T>C) [β114(G16)Leu→Pro] and the IVS-I-110 ( HBB : c.93-21G>A) Causing a Severe β-Thalassemia Phenotype.

Author

Cannata M, Cassarà F, Vinciguerra M, Licari P, Passarello C, Leto F, Lo Pinto C, Pitrolo L, Ganci R, Maggio A, and Giambona A

Subjects
Biomarkers, DNA Mutational Analysis, Erythrocyte Indices, Female, Humans, Infant, beta-Thalassemia blood, Alleles, Amino Acid Substitution, Heterozygote, Mutation, Phenotype, beta-Globins genetics, beta-Thalassemia diagnosis, beta-Thalassemia genetics
Abstract

The evaluation of a 10-month-old girl of Sicilian origin with a clinical phenotype of severe thalassemia led to the identification of two β-globin gene defects, a β-thalassemia (β-thal), mutation at IVS-I-110 ( HBB : c.93-21G>A) and a variant hemoglobin (Hb) mutation at codon 114 ( HBB : c.344T>C) on the other allele, reported as Hb Durham-N.C. (also known as Hb Brescia) [β114(G16)Leu→Pro] in the HbVar database. A very low Hb level (Hb 3.5 g/dL), microcytosis [mean corpuscular volume (MCV) 63.2 fL] and hypocromia [mean corpuscular Hb (MCH) 19.6 pg], increased red blood cell (RBC) distribution width (RDW) (36.0%), higher reticulocytes (6.2%), anisocytosis, poikilocytosis, hypocromia, basophilic stippling and inclusion body formation, were present in the affected subject. Analysis of other family components showed the presence of HBB : c.93-21G>A defect in the mother and in her brother, while Hb Durham-N.C. was absent in all other relatives, thus, this mutation has arisen as a de novo defect. This is the first case described as a severe thalassemic phenotype in a compound heterozygote carrier of this unstable Hb and a common β-thalassemic allele. The important information gained from this case is that a rare dominant or recessive mutation may arise in every individual, even if this is a very rare event.

Published
2019
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24. Co-inheritance of HBB:c.-106G > C, a rare single nucleotide variation at position -56 relative to transcription initiation site, with other known mutations in the globin clusters.

Author

Vinciguerra M, Passarello C, Cassarà F, Leto F, Cannata M, Ferro E, Anzà D, Calvaruso G, Maggio A, and Giambona A

Subjects
Hemoglobinopathies blood, Hemoglobinopathies genetics, Humans, Italy, Multigene Family, Pedigree, Phenotype, Sequence Analysis, DNA, Alleles, Genotype, Inheritance Patterns, Mutation, Polymorphism, Single Nucleotide, Transcription Initiation Site, beta-Globins genetics
Abstract

Objectives: We performed molecular analysis to evaluate clinical implications of a rare nucleotide change, particularly when co-inherited with other known mutations in the globin clusters, in order to conduct an appropriate genetic counselling., Methods: Complete blood cell counts and high-performance liquid chromatography were the routine first level analysis for patients referred to our Hospital Center in Palermo to undergo the screening test for haemoglobinopathies. Sequencing analysis was the selected method for the phenotypic characterization, especially in case of new or very rare mutations in globin genes., Results: We report data of a rare single nucleotide variation at position -56 relative to transcription initiation site (NM_000518.4(HBB):c.-106G > C), identified in ten patients of Italian origin during the screening programme of the 'Sicilian population'. It was found in simple heterozygosity (n = 8), in association with beta haemoglobin variant Hb S (n = 1) and in heterozygosity with beta-thalassaemic allele IVS-I-1 G->A [(HBB):c.92 + 1G > A] and ααα anti3.7 rearrangement (n = 1)., Discussion: Heterozygous subjects for this substitution showed normal haematological and electrophoretic features. Heterozygotes for this mutation and other defect in globin genes showed the classical phenotype of a healthy carrier, therefore it can be considered a benign variant that does not alter the production and function of haemoglobin., Conclusion: This is another example of rare or new nucleotide variations whose identification and characterization is crucial in order to carry out appropriate genetic counselling to a potential risk couple.

Published
2018
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25. Longitudinal changes in LIC and other parameters in patients receiving different chelation regimens: Data from LICNET.

Author

Vitrano A, Sacco M, Rosso R, Quota A, Fiorino D, Oliva E, Gerardi C, Roccamo G, Spadola V, Filosa A, Tesé L, Calvaruso G, Pitrolo L, Mistretta L, Cassarà F, Di Maggio R, and Maggio A

Subjects
Adolescent, Adult, Aged, Biomarkers blood, Chelation Therapy, Child, Cross-Sectional Studies, Female, Ferritins blood, Humans, Iron Chelating Agents therapeutic use, Iron Overload diagnostic imaging, Iron Overload etiology, Liver diagnostic imaging, Liver drug effects, Magnetic Resonance Imaging methods, Male, Middle Aged, Young Adult, Iron metabolism, Iron Overload metabolism, Iron Overload pathology, Liver metabolism, Liver pathology
Abstract

Objectives: The liver remains the primary site of iron storage, with liver iron concentration (LIC) being a strong surrogate of total body iron. MRI-R2 can accurately measure LIC. The LICNET (Liver Iron Cutino Network) was established to diagnostics of liver iron overload by MRI-R2 subjects with hemochromatosis in hematological disorders. The aims of the study were to look at variation in LIC measurements during time across different chelation regimens., Methods: This was a cross-sectional study of 130 patients attending 9 Italian centers participating in the LICNET. LIC comparisons over time (T 0 and T 1 ) were made using t test and/or Wilcoxon test., Results: LIC significantly decreased from MRI1 to MRI2 although at high variance (median change -0.8 mg Fe/g dw, range: -29.0 to 33.0; P = .011) and 7.7% of patients shifted from LIC values of high risk (>15 mg Fe/g dw) to an intermediate-risk category (7-15 mg Fe/g dw). Median change in LIC and correlation with serum ferritin levels (SF), during different chelation regimens, is reported., Conclusions: These findings suggest as longitudinal variation in the LIC is possible, across all chelation regimens. It confirms as SF levels not always can be used for estimating changes in LIC., (© 2017 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2018
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26. Phenotypic evaluations of HBB :c.93-23T>C, a nucleotide substitution in the IVS I nt 108 of β-globin gene.

Author

Vinciguerra M, Cassarà F, Cannata M, Renda D, Calvaruso G, Leto F, Passarello C, Maggio A, and Giambona A

Abstract

Background: Thalassaemia and variant haemoglobin are the most common severe monogenic disorders worldwide., Aims: To develop prenatal diagnosis programmes for the prevention of the most important haemoglobin disorders and identify healthy carriers of thalassaemia., Methods: Sequencing analysis was used to obtain complete data on gene structure and to correlate specific phenotypic expression with mutations, especially for new or very rare mutations in globin genes., Results: A rare single nucleotide variation, HBB :c.93-23T>C, located in nucleotide 108 of the first intervening sequence of the HBB gene, was identified. This variation was previously reported but its clinical significance was not known. Six heterozygous patients had this nucleotide variation and eight further cases co-inherited it together with other defects in the globin genes. Heterozygous subjects for this substitution showed normal haematological and electrophoretic features, whereas subjects who were compound heterozygotes for this mutation and another defect in globin genes showed the classic phenotype of a healthy carrier., Conclusion: This nucleotide can be considered a single nucleotide polymorphism and not a thalassaemic mutation that reduces the production of haemoglobin. This is another example of a very rare nucleotide variation. Knowledge of this is important so that appropriate genetic counselling can be carried out of a couple potentially at risk, where one of the partners is a carrier of β-thalassaemia and the other is carrier of a nucleotide variation., Competing Interests: Competing interests: None declared., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2017. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published
2017
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27. HBB: c.316-125A>G and HBB: c.316-42delC: Phenotypic Evaluations of Two Rare Changes in the Second Intron of the HBB Gene.

Author

Vinciguerra M, Cannata M, Cassarà F, Passarello C, Leto F, Calvaruso G, Renda D, Maggio A, and Giambona A

Subjects
Adult, Female, Humans, Male, Middle Aged, Pregnancy, Sicily, Hemoglobins genetics, Introns genetics, Multigene Family, Point Mutation, Polymorphism, Single Nucleotide
Abstract

We report two very rare changes in the second intron of the HBB gene, a substitution at nucleotide (nt) 726 [IVS-II-726 (A>G) (β + ), NM_000518, HBB: c.316-125A>G] and a deletion of a cytosine at nt 809 [IVS-II-809 (-C) (β), NM_000518, HBB: c.316-42delC] identified during the screening program for hemoglobinopathies in the resident Sicilian population. The purpose of this study was to evaluate the clinical implication of these rare changes, particularly in coinheritance with known mutations in the globin clusters, in order to conduct an appropriate genetic counseling for at-risk couples. Molecular analysis detected the first rare nt substitution in two cases in simple heterozygosity and in two cases in association with other known mutations on globin genes, while the deletion was identified in a pregnant woman, carrier of β-thal, and in her fetus at prenatal diagnosis (PND) for hemoglobinopathies. The present study emphasizes the importance of sharing the observed changes in the globin gene cluster, especially in the case of new or rare undefined mutations, in order to facilitate the determination of their phenotypic expression and possible interactions with known molecular defects.

Published
2017
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28. Phenotypic Evaluation of a Novel Nucleotide Substitution (HBD: c.442T>C) on the δ-Globin Gene.

Author

Cassarà F, Vinciguerra M, Cannata M, Marchese G, Passarello C, Leto F, Maggio A, and Giambona A

Subjects
Adult, Amino Acid Substitution, Erythrocyte Indices, Female, Hemoglobinopathies blood, Humans, Male, Phenotype, Sequence Analysis, DNA, beta-Thalassemia, Alleles, Hemoglobinopathies diagnosis, Hemoglobinopathies genetics, Hemoglobins, Abnormal genetics, Mutation, delta-Globins genetics
Abstract

HBD: c.442T>C is a new mutation at the stop codon (TGA>CGA) of the δ-globin gene, which produces a new codon for arginine. This substitution causes a 51 nucleotides longer open reading frame determining the synthesis of a potential larger δ subunit, which is a probable target of mechanisms for the degradation of aberrant proteins as well as the defective synthesized mRNA molecules, and may also be rapidly degraded by a variety of RNA surveillance pathways. We identified this molecular defect in four patients: three women with a reduced HbA 2 level and a 37-year-old male showing the typical phenotype of an α-thalassemia (α-thal) carrier with reduced values of red cell indices and normal HbA 2 level (2.5%). The mutation on the δ-globin gene was found to have been coinherited with a β-globin gene defect leading to a normalized HbA 2 level. These data support the necessity of investigating these cases at a molecular level, particularly if the partner is also a β-thalassemia (β-thal) carrier. The present data emphasizes the importance of a careful evaluation of correlation between genotypes resulting from DNA analysis and phenotypes, especially in cases of atypical hematological parameters, in order to carry out an adequate diagnostic process finalized to appropriate genetic counseling.

Published
2017
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29. Real-life experience with liver iron concentration R2 MRI measurement in patients with hemoglobinopathies: baseline data from LICNET.

Author

Vitrano A, Calvaruso G, Tesé L, Gioia F, Cassarà F, Campisi S, Butera F, Commendatore V, Rizzo M, Santoro V, Cigna V, Quota A, Bagnato S, Argento C, Fidone C, Schembari D, Gerardi C, Barbiera F, Bellisssima G, Giugno G, Polizzi G, Rosso R, Abbate G, Caruso V, Chiodi E, Gamberini MR, Giorgi B, Putti MC, Filosa A, De Ritis MR, Oliva E, Arcadi N, Fustaneo M, Mistretta L, Di Maggio R, Sacco M, Veronica DS, Giangreco A, and Maggio A

Subjects
Adolescent, Adult, Aged, Alanine Transaminase blood, Biomarkers, Child, Comorbidity, Cross-Sectional Studies, Female, Ferritins blood, Hemoglobinopathies diagnosis, Humans, Iron Chelating Agents therapeutic use, Iron Overload drug therapy, Male, Middle Aged, Young Adult, Hemoglobinopathies complications, Iron metabolism, Iron Overload diagnosis, Iron Overload etiology, Liver metabolism, Liver pathology, Magnetic Resonance Imaging methods
Abstract

Background: Real-life data on the use of R2 MRI for the assessment of liver iron concentration (LIC) remain limited., Methods: We conducted a cross-sectional analysis on 363 patients (mean age 35.6 yr, 44.1% men) with hemoglobinopathies (204 β-thalassemia major [TM], 102 β-thalassemia intermedia [TI], and 57 sickle cell disease [SCD]) that were evaluated with R2 MRI as part of LICNET, an MRI network of 13 Italian treatment centers., Results: The mean LIC was 7.8 mg/g (median: 4.0), with high LIC (>7 mg/g) noted in both transfused (TM, TI 37%; SCD 38%) and non-transfused (TI 20%) patients. Ferritin levels correlated with LIC in both transfused (TM, TI, SCD) and non-transfused (TI) patients (P < 0.001), although lower values predicted high LIC in non-transfused patients (1900 vs. 650 ng/mL in TM vs. non-transfused TI). A correlation between LIC and ALT levels was only noted in HCV-negative patients (rs = 0.316, P < 0.001). The proportion of patients with high LIC was significantly different between iron chelators used (P = 0.023), with the lowest proportion in deferasirox (30%) and highest in deferiprone (53%)-treated patients., Conclusions: High LIC values persist in subgroups of patients with hemoglobinopathy, warranting closer monitoring and management optimization, even for non-transfused patients with relatively low ferritin levels., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2016
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30. Coinheritance of a Rare Nucleotide Substitution on the β-Globin Gene and Other Known Mutations in the Globin Clusters: Management in Genetic Counseling.

Author

Vinciguerra M, Passarello C, Leto F, Crivello A, Fustaneo M, Cassarà F, Cannata M, Maggio A, and Giambona A

Subjects
DNA Mutational Analysis, Genetic Counseling, Hemoglobin A2, Hemoglobin, Sickle genetics, Hemoglobins, Abnormal genetics, Humans, Introns genetics, Mutation, Phenotype, Registries, beta-Thalassemia genetics, Multigene Family genetics, beta-Globins genetics
Abstract

A large number of methods for DNA analysis are available to identify defects in globin genes associated with hemoglobin (Hb) disorders. In this study, we report a rare nucleotide (nt) substitution on the β-globin gene, nt 781 in the second intron [IVS-II-781 (C > G); HBB: c.316-70C > G], identified in four patients. This nt substitution was previously described only as a personal communication to the HbVar database and indicated as a β(0) or β(+) mutation. The purpose of this study was to evaluate the clinical implication of this nt change, particularly when coinherited with severe β-thalassemia (β-thal), in order to be able to conduct appropriate genetic counseling. Genetic studies were performed on two subjects, one carried Hb S [β6(A3)Glu→Val; HBB: c.20A > T], and the other carried IVS-I-110 (G > A) (HBB: c.93-21G > A). All these subjects showed this new β nt substitution in association with Hb A2' (or Hb B2) [δ16(A13)Gly→Arg; HBD: c.49G > C]. Another 16 samples, carrying the same δ variant as the probands, were processed by β-globin gene sequencing in order to better understand the correlation between this Hb variant and the rare nt substitution reported in this study. The present investigation emphasizes the importance of sharing the observed nt changes in the globin gene cluster, especially in the case of new or rare undefined mutations, in order to facilitate the determination of their phenotypic expression, the possible interactions with known molecular defects and to formulate appropriate genetic counseling for at-risk couples.

Published
2016
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31. Hb San Cataldo [β144(HC1)Lys→Thr; HBB: C.434A > C]: A New Hemoglobin Variant with Increased Affinity for Oxygen.

Author

Vinciguerra M, Passarello C, Cassarà F, Leto F, Cannata M, Crivello A, Di Salvo V, Maggio A, and Giambona A

Subjects
2,3-Diphosphoglycerate, Diagnosis, Differential, Female, Hemoglobinopathies genetics, Heterozygote, Humans, Middle Aged, Polycythemia Vera etiology, Hemoglobins, Abnormal genetics, Mutation, Missense, Oxygen metabolism, Polycythemia Vera genetics
Abstract

A 59-year-old Italian woman came to our center for revaluation of a previous diagnosis of polycythemia vera. The patient presented with a lifelong history of polycythemia, no increase in white blood cells (WBCs) and platelets, and a negative bone marrow biopsy. Analysis of hemoglobin (Hb) fractions showed an abnormal fast moving Hb component. We aimed to determine if this variant was the cause of polycythemia in this patient. A complete blood count (CBC) was performed by an automated cell counter and Hb fractions were determined by high performance liquid chromatography (HPLC). Standard stability tests and oxygen affinity evaluation were also performed. Genomic DNA was extracted from peripheral blood leukocytes using the phenol chloroform method and the entire β-globin gene was analyzed by direct sequencing. At the hematological level, no anemia or hemolysis was observed but an abnormal Hb fraction was detected using cation exchange HPLC. Molecular analysis of the β-globin gene showed heterozygosity for an AAG > ACG substitution at codon 144, resulting in a Lys→Thr amino acid replacement. We demonstrated that this is a new Hb variant with increased oxygen affinity. Its altered physiology is caused by the reduction of 2,3-diphosphoglycerate (2,3-DPG) effects, due to an amino acid substitution in the central pocket near the C-terminal of the β chain. We called this new variant Hb San Cataldo for the native city of proband.

Published
2016
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33. Co-inheritance of the rare β hemoglobin variants Hb Yaounde, Hb Görwihl and Hb City of Hope with other alterations in globin genes: impact in genetic counseling.

Author

Vinciguerra M, Passarello C, Leto F, Cassarà F, Cannata M, Maggio A, and Giambona A

Subjects
Adult, Aged, Erythrocyte Indices, Female, Heterozygote, Humans, Italy, Male, Mutation, Pedigree, Pregnancy, Sequence Analysis, DNA, Young Adult, alpha-Globins genetics, Genetic Counseling, Genetic Variation, Hemoglobins, Abnormal genetics, Inheritance Patterns, beta-Globins genetics
Abstract

Purpose: Nearly 1183 different molecular defects of the globin genes leading to hemoglobin variants have been identified (http://globin.bx.psu.edu) over the past decades. The purpose of this study was to report three cases, never described in the literature, of co-inheritance of three β hemoglobin variants with other alterations in globin genes and to evaluate the clinical significance to conduct an appropriate genetic counseling., Patients and Methods: We report the molecular study performed in three probands and their families, sampling during the screening program conducted at the Laboratory for Molecular Prenatal Diagnosis of Hemoglobinopathies at Villa Sofia-Cervello Hospital in Palermo, Italy., Results: This work allowed us to describe the co-inheritance of three rare β hemoglobin variants with other alterations in globin genes: the β hemoglobin variant Hb Yaounde [β134(H12)Val>Ala], found for the first time in combination with ααα(anti3.7) arrangement, and the β hemoglobin variants Hb Görwihl [β5(A2)Pro>Ala] and Hb City of Hope [β69(E13)Gly>Ser], found both in association with β(0) -thalassemia., Conclusion: The present work emphasizes the importance of a careful evaluation of the hematological data, especially in cases of atypical hematological parameters, to carry out an adequate and complete molecular study and to formulate an appropriate genetic counseling for couples at risk., (© 2014 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2015
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34. Identification of three new nucleotide substitutions in the β-globin gene: laboratoristic approach and impact on genetic counselling for beta-thalassaemia.

Author

Vinciguerra M, Passarello C, Leto F, Cassarà F, Cannata M, Maggio A, and Giambona A

Subjects
Adult, Databases, Genetic, Female, Genetic Counseling ethics, Genetic Counseling organization & administration, Genetic Testing, Genotype, Heterozygote, Humans, Introns, Italy, Male, Molecular Sequence Data, Pedigree, Phenotype, beta-Thalassemia diagnosis, Base Sequence, Hemoglobins, Abnormal genetics, Polymorphism, Single Nucleotide, Sequence Deletion, beta-Globins genetics, beta-Thalassemia genetics
Abstract

Purpose: Over the past two decades, a wide range of available methods for DNA analysis have allowed us to identify defects in globin genes associated with haemoglobin disorders and to correlate specific mutations with phenotypic expression. The purpose of this study was to evaluate the nature of three new nucleotide changes, mutation or single nucleotide polymorphism, found in the beta-globin gene, to conduct an appropriate genetic counselling., Patients and Methods: We report the molecular study performed in three probands and their families, sampling during the screening programme conducted at the Laboratory for Molecular Prenatal Diagnosis of Hemoglobinopathies at Villa Sofia-Cervello Hospital in Palermo, Italy., Results: This work allowed us to report three new nucleotide substitutions of the β-globin gene: a substitution of the nucleotide 16 in the CAP site area (HBB: c.-35 A>G), a substitution of the nucleotide 478 in the second intron (HBB: c.316-373) in association with β-haemoglobin variant Hb G Copenhagen (HBB:c.142G>A) and a substitution of the nucleotide 1656 within the 3' UTR (HBB: c.*+182 G>A) in association with the 1393-bp deletion (NG&#95;000007.3:g.70060&#95;71452del1393)., Conclusion: The present work emphasizes the importance of reporting the observed nucleotide changes to the Haemoglobin Variant Database, especially in the case of new or rare undefined mutations, to facilitate the determination of their phenotypic expression and the possible interactions with known molecular defects and to formulate an appropriate genetic counselling for couples at risk., (© 2014 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2014
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35. Iron chelation therapy in thalassemia major: a systematic review with meta-analyses of 1520 patients included on randomized clinical trials.

Author

Maggio A, Filosa A, Vitrano A, Aloj G, Kattamis A, Ceci A, Fucharoen S, Cianciulli P, Grady RW, Prossomariti L, Porter JB, Iacono A, Cappellini MD, Bonifazi F, Cassarà F, Harmatz P, Wood J, and Gluud C

Subjects
Chelation Therapy statistics & numerical data, Deferasirox, Deferiprone, Drug Therapy, Combination, Ferritins blood, Humans, Iron, Liver metabolism, MEDLINE, Myocardium metabolism, Randomized Controlled Trials as Topic, Treatment Outcome, Ventricular Function physiology, Benzoates administration & dosage, Deferoxamine administration & dosage, Iron Chelating Agents administration & dosage, Pyridones administration & dosage, Siderophores administration & dosage, Triazoles administration & dosage, beta-Thalassemia blood, beta-Thalassemia drug therapy
Abstract

The effectiveness of deferoxamine (DFO), deferiprone (DFP), or deferasirox (DFX) in thalassemia major was assessed. Outcomes were reported as means±SD, mean differences with 95% CI, or standardized mean differences. Statistical heterogeneity was tested using χ2 (Q) and I2. Sources of bias and Grading of Recommendations Assessment, Development and Evaluation system (GRADE) were considered. Overall, 1520 patients were included. Only 7.4% of trials were free of bias. Overall measurements suggest low trial quality (GRADE). The meta-analysis suggests lower final liver iron concentrations during associated versus monotherapy treatment (p<0.0001), increases in serum ferritin levels during DFX 5, 10, and 20 mg/kg versus DFO-treated groups (p<0.00001, p<0.00001, and p=0.002, respectively), but no statistically significant difference during DFX 30 mg/kg versus DFO (p=0.70), no statistically significant variations in heart T2* signal during associated or sequential versus mono-therapy treatment (p=0.46 and p=0.14, respectively), increases in urinary iron excretion during associated or sequential versus monotherapy treatment (p=0.008 and p=0.02, respectively), and improved ejection fraction during associated or sequential versus monotherapy treatment (p=0.01 and p<0.00001, respectively). These findings do not support any specific chelation treatment. The literature shows risks of bias, and additional larger and longer trials are needed., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published
2011
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36. The genetic heterogeneity of β-globin gene defects in Sicily reflects the historic population migrations of the island.

Author

Giambona A, Vinciguerra M, Cannata M, Cassarà F, Fiorentino G, Leto F, Gioco PL, Renda D, Passarello C, and Maggio A

Subjects
Humans, Mutation, Sicily epidemiology, beta-Thalassemia epidemiology, beta-Thalassemia genetics, Emigration and Immigration, Genetic Heterogeneity, Hemoglobins, Abnormal genetics, beta-Globins genetics
Abstract

The aim of this study is to update the incidence and the distribution of the globin gene defects causing β-thalassemia and abnormal hemoglobins in Sicily. The data derived from a total of 8875 beta-thalassemia alleles and 1330 variant hemoglobin chromosomes studied in Sicily from 1990 during a hemoglobinopathy control program. Fifty-four beta-globin gene defects were characterized, involving 30 different beta-thalassemia mutations and 24 variant hemoglobins. Eight of 30 β-thalassemia defects accounted for 95.11% of examined alleles while other beta-globin gene defects were found at lower frequencies (<1%). A consistent number (24) of variant hemoglobins were identified of whom Hb S was the most represented (72.1%). Our data underline the heterogeneity of the beta-globin gene defects in the Sicily. The enormous progress in the technique for β-globin gene analysis permitted to characterize 99.93% of mutated alleles and it has made a first trimester prenatal diagnosis program possible in our region in all cases with a great improvement in thalassemia management. The origin of the large spectrum of mutations is discussed taking in consideration the history of the island., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published
2011
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37. Management of chronic viral hepatitis in patients with thalassemia: recommendations from an international panel.

Author

Di Marco V, Capra M, Angelucci E, Borgna-Pignatti C, Telfer P, Harmatz P, Kattamis A, Prossamariti L, Filosa A, Rund D, Gamberini MR, Cianciulli P, De Montalembert M, Gagliardotto F, Foster G, Grangè JD, Cassarà F, Iacono A, Cappellini MD, Brittenham GM, Prati D, Pietrangelo A, Craxì A, and Maggio A

Subjects
Hepatitis B, Chronic complications, Hepatitis B, Chronic diagnosis, Hepatitis B, Chronic transmission, Hepatitis C, Chronic complications, Hepatitis C, Chronic diagnosis, Hepatitis C, Chronic transmission, Humans, Liver Cirrhosis complications, Liver Cirrhosis diagnosis, Thalassemia drug therapy, Thalassemia epidemiology, Antiviral Agents therapeutic use, Hepatitis B, Chronic drug therapy, Hepatitis C, Chronic drug therapy, Thalassemia complications
Abstract

Chelation therapy with new drugs prevents cardiac damage and improves the survival of thalassemia patients. Liver diseases have emerged as a critical clinical issue. Chronic liver diseases play an important role in the prognosis of thalassemia patients because of the high frequency of viral infections and important role of the liver in regulating iron metabolism. Accurate assessment of liver iron overload is required to tailor iron chelation therapy. The diagnosis of hepatitis B virus- or hepatitis C virus-related chronic hepatitis is required to detect patients who have a high risk of developing liver complications and who may benefit by antiviral therapy. Moreover, clinical management of chronic liver disease in thalassemia patients is a team management issue requiring a multidisciplinary approach. The purposes of this paper are to summarize the knowledge on the epidemiology and the risks of transmission of viral infections, to analyze invasive and noninvasive methods for the diagnosis of chronic liver disease, to report the knowledge on clinical course of chronic viral hepatitis, and to suggest the management of antiviral therapy in thalassemia patients with chronic hepatitis B or C virus or cirrhosis.

Published
2010
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38. Hepatocellular carcinoma in patients with thalassaemia syndromes: clinical characteristics and outcome in a long term single centre experience.

Author

Restivo Pantalone G, Renda D, Valenza F, D'Amato F, Vitrano A, Cassarà F, Rigano P, Di Salvo V, Giangreco A, Bevacqua E, and Maggio A

Subjects
Adult, Aged, Female, Hepatitis C, Chronic complications, Humans, Iron Overload complications, Male, Middle Aged, Prognosis, Transfusion Reaction, Carcinoma, Hepatocellular etiology, Liver Neoplasms etiology, Thalassemia therapy
Published
2010
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39. A critical review of non invasive procedures for the evaluation of body iron burden in thalassemia major patients.

Author

Maggio A, Capra M, Pepe A, Mancuso L, Cracolici E, Vitabile S, Rigano P, Cassarà F, and Midiri M

Subjects
Echocardiography methods, Humans, Iron Overload drug therapy, Magnetic Resonance Imaging methods, Iron analysis, Iron Overload metabolism, beta-Thalassemia metabolism
Abstract

It is evident that different non invasive methodologies have been implemented for the detection of organ specific iron burden in patients with thalassemia major. Among these MR relaxometry has the potential to become the method of choice for non-invasive, safe and accurate assessment of organ-specific iron load, although further theoretical research, along with studies monitoring wider age groups of patients, is needed. Moreover, the possibility of detecting organ-specific iron burden is relevant for tailoring specific chelation treatment in different patients or in the same patient during different periods of life. In fact, while heart organ-specific effect has been suggested by MR relaxometry for some chelation treatments, it is possible to suppose that another single chelator or association of other chelators may show different organ-specific effects. For these reasons, the future of our clinical research will be to understand, mainly by MR relaxometry, whether it would be possible to set up a tailored organ-specific chelation treatment, according to this supposed difference in organ efficacy of the current chelation therapies.

Published
2008

40. Hb Marineo [beta70(E14)Ala-->Val]: a silent hemoglobin variant with a mutation within the heme pocket.

Author

Giambona A, Vinciguerra M, Cassarà F, Li Muli R, Leto F, Passarello C, Wajcman H, and Maggio A

Subjects
Adult, Amino Acid Substitution, Chromatography, High Pressure Liquid, Codon genetics, DNA Mutational Analysis, Female, Globins chemistry, Haplotypes genetics, Hemoglobins, Abnormal chemistry, Humans, Male, Models, Molecular, Pedigree, Phenotype, Protein Conformation, Sequence Analysis, DNA, Sicily, Globins genetics, Hemoglobins, Abnormal genetics, Mutation, Missense, Point Mutation
Abstract

We report a new hemoglobin (Hb) variant, Hb Marineo [beta70(E14)Ala --> Val], found in three generations of a family from West Sicily. The mutation is due to a GCC --> GTC substitution at codon 70 of the beta-globin gene. To date, three mutations at codon 70 of the beta-globin gene have been described, presenting with hemolytic anemia. In our case, no anemia or other alteration of hematological indices were found. Cation exchange high performance liquid chromatography (HPLC) showed a peak in the P2 window (VARIANT I), while a peak was detected by VARIANT II HPLC in the P3 window. Reversed phase HPLC analysis showed an abnormal chain amounting to about 40% of the total beta chains.

Published
2006
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